Title of Invention	A SPIRO COMPOUND OF FORMULA (I)
Abstract	1. A spiro compound of formula a prodrug as herein described, a N-oxide as herein described, an addition salt as herein described, a quaternary amine as herein described or a stereochemically isomeric form thereof wherein R1 is hydrogen, C1-6alkyl, halo, formyl, carboxyl, C1- 6alkyloxycarbonyl, C1-6alkyl-carbonyl, N(R3R4)C(=0)-, N(R3R4)C(=0)N(R5)-, ethenyl substituted with carboxyl or C1-6alkyloxycarbonyl or C1-6alkyl substituted with hydroxy, carboxyl, C1-6alkyloxy, C1-6alkyloxycarbonyl, N(R3 R4)C(=0)-, C1-6alkylC(=0)N(R5)-, C1-6alkylS(=0) 2N(R5)-or N(R3 R4)C(=0)N(R5)-; wherein each R3 and each R4 independently are hydrogen or C1-4alkyl; R5 is hydrogen or hydroxy; R2 is hydrogen, C1-6alkyl, hydroxyC1-6alkyl, C1-6alkyloxyC1-6alkyl, N(R3 R4)C(=Q)-, aryl or halo; n is 1 or 2; -A-B- represents a bivalent radical of formula -Y-CH=CH- (a-1); -CH=CH-Y- (a-2); or -CH=CH-CH=CH- (a-3); wherein each hydrogen atom in the radicals (a-1) to (a-3) may independently be replaced by R6 wherein R6 is selected from C1-6alkyl, halo, hydroxy, C1-6alkyloxy, ethenyl substituted with carboxyl or C1-6alkyloxycarbonyl, hydroxyC1-6alkyl, formyl, carboxyl and hydroxycarbonylC1-6alkyl; each Y independently is a bivalent radical of formula -O-, -S- or -NR7-; wherein R7is hydrogen, C1-6alkyl or C1-6alkylcarbonyl; Z is a bivalent radical of formula -(CH2)p- (b-1), -CH2-C(=0)- (b-5), or -CH=CH- (b-2), -CH2-C(=NOH)- (b-6), -CH2-CHOH- (b-3), - CH2-O- (b-4), provided that the bivalent radicals (b-3), (b-4), (b-5) and (b-6) are connected to the nitrogen of the imidazole ring via their -CH2-moiety: wherein p is 1, 2, 3 or 4; L is hydrogen; C1-6alkyl; C1-6alkenyl; Ci-6alkylcarbonyl; C1-4alkyloxycarbonyl; C1-4alkyl substituted with one or more substituents each independently selected from hydroxy, carboxyl, C1-4alkylox, C1-6alkyloxycarbonyl, aryl, aryloxy, cyano or R8HN-wherein R8 is hydrogen, C1-6alkyl, C1-6alkyloxycarbonyl, C1-6alkylcarbonyl; or L represents a radical of formula -Alk-Y-Het1 (c-1), -Alk-NH-CO-Het2 (c-2) or -Alk-Het3 (c-3) wherein Alk represents C1-4 alkanediyl; Y represents O, S or NH: Het1, Het2 and Het3 each represent furanyl, tetrahydrofuranyl, thienyl, oxazolyl, thiazolyl or imidazolyl each optionally substituted with one or two C1-4 alkyl substituents, pyrrolyl or pyrazolyl optionally substituted with formyl, hydroxyC1-4alkyl, hydroxycarbonyl, C1-4alkyloxycarbonyl or with one or two C1-4alkyl substituents; thiadiazolyl or oxadiazolyl optionally substituted with amino or C1-4alkyl; pyridinyl, pyrimidinyl, pyrazinyl or pyridazinyl each optionally substituted with C1-4alkyl, C1-4 alkyloxy, amino, hydroxy or halo; and Het3 may also represent 4,5-dihydro-5-oxo-lH-tetrazolyl substituted with C1-4alkyl, 2-oxo-3-oxazolidinyl, 2-3-dihydro-2-oxo-lH-benzimidazol-l-yl or a radical of formula A-Z represents S-CH=CH, S-CH2-CH2, S-CH2-CH2-CH2, CH=CH-CH=CH, or CH2-CH2-CH2-CH2; atyl is phenyl or phenyl substituted with 1, 2 or 3 substituents each independently selected from halo, hydroxy, C1-4alky, polyhaloC1-4alkyl, cyano, aminocarbonyl, C1-4alkyloxy or polyhaloC1-4alkyloxy; provided that when L is H or benzyl; Z is a bivalent radical of formula (b-1) with p being 1 or 2, or (b-2) R1 is hydrogen, C1-6alkyl, halo, formyl, carboxyl, ethenyl substituted with carboxyl or C1-6alkyloxycarbonyl, or Ci-ealkyl substituted with hydroxyl, carboxyl or C1-6alkyloxycarbonyl; R2 is hydrogen, C1-6alkyl, hydroxy C1-6alkyl, aryl or halo; and R6 is C1-6alkyl, halo, ethenyl substituted with carboxyl or C1-6alkyloxycarbonyl, hydroxy Ciealkyl, formyl, carboxyl or hydroxycarbonylC1-6alkyl; then n is 2.

Title of Invention

A SPIRO COMPOUND OF FORMULA (I)

Abstract

1. A spiro compound of formula a prodrug as herein described, a N-oxide as herein described, an addition salt as herein described, a quaternary amine as herein described or a stereochemically isomeric form thereof wherein R1 is hydrogen, C1-6alkyl, halo, formyl, carboxyl, C1- 6alkyloxycarbonyl, C1-6alkyl-carbonyl, N(R3R4)C(=0)-, N(R3R4)C(=0)N(R5)-, ethenyl substituted with carboxyl or C1-6alkyloxycarbonyl or C1-6alkyl substituted with hydroxy, carboxyl, C1-6alkyloxy, C1-6alkyloxycarbonyl, N(R3 R4)C(=0)-, C1-6alkylC(=0)N(R5)-, C1-6alkylS(=0) 2N(R5)-or N(R3 R4)C(=0)N(R5)-; wherein each R3 and each R4 independently are hydrogen or C1-4alkyl; R5 is hydrogen or hydroxy; R2 is hydrogen, C1-6alkyl, hydroxyC1-6alkyl, C1-6alkyloxyC1-6alkyl, N(R3 R4)C(=Q)-, aryl or halo; n is 1 or 2; -A-B- represents a bivalent radical of formula -Y-CH=CH- (a-1); -CH=CH-Y- (a-2); or -CH=CH-CH=CH- (a-3); wherein each hydrogen atom in the radicals (a-1) to (a-3) may independently be replaced by R6 wherein R6 is selected from C1-6alkyl, halo, hydroxy, C1-6alkyloxy, ethenyl substituted with carboxyl or C1-6alkyloxycarbonyl, hydroxyC1-6alkyl, formyl, carboxyl and hydroxycarbonylC1-6alkyl; each Y independently is a bivalent radical of formula -O-, -S- or -NR7-; wherein R7is hydrogen, C1-6alkyl or C1-6alkylcarbonyl; Z is a bivalent radical of formula -(CH2)p- (b-1), -CH2-C(=0)- (b-5), or -CH=CH- (b-2), -CH2-C(=NOH)- (b-6), -CH2-CHOH- (b-3), - CH2-O- (b-4), provided that the bivalent radicals (b-3), (b-4), (b-5) and (b-6) are connected to the nitrogen of the imidazole ring via their -CH2-moiety: wherein p is 1, 2, 3 or 4; L is hydrogen; C1-6alkyl; C1-6alkenyl; Ci-6alkylcarbonyl; C1-4alkyloxycarbonyl; C1-4alkyl substituted with one or more substituents each independently selected from hydroxy, carboxyl, C1-4alkylox, C1-6alkyloxycarbonyl, aryl, aryloxy, cyano or R8HN-wherein R8 is hydrogen, C1-6alkyl, C1-6alkyloxycarbonyl, C1-6alkylcarbonyl; or L represents a radical of formula -Alk-Y-Het1 (c-1), -Alk-NH-CO-Het2 (c-2) or -Alk-Het3 (c-3) wherein Alk represents C1-4 alkanediyl; Y represents O, S or NH: Het1, Het2 and Het3 each represent furanyl, tetrahydrofuranyl, thienyl, oxazolyl, thiazolyl or imidazolyl each optionally substituted with one or two C1-4 alkyl substituents, pyrrolyl or pyrazolyl optionally substituted with formyl, hydroxyC1-4alkyl, hydroxycarbonyl, C1-4alkyloxycarbonyl or with one or two C1-4alkyl substituents; thiadiazolyl or oxadiazolyl optionally substituted with amino or C1-4alkyl; pyridinyl, pyrimidinyl, pyrazinyl or pyridazinyl each optionally substituted with C1-4alkyl, C1-4 alkyloxy, amino, hydroxy or halo; and Het3 may also represent 4,5-dihydro-5-oxo-lH-tetrazolyl substituted with C1-4alkyl, 2-oxo-3-oxazolidinyl, 2-3-dihydro-2-oxo-lH-benzimidazol-l-yl or a radical of formula A-Z represents S-CH=CH, S-CH2-CH2, S-CH2-CH2-CH2, CH=CH-CH=CH, or CH2-CH2-CH2-CH2; atyl is phenyl or phenyl substituted with 1, 2 or 3 substituents each independently selected from halo, hydroxy, C1-4alky, polyhaloC1-4alkyl, cyano, aminocarbonyl, C1-4alkyloxy or polyhaloC1-4alkyloxy; provided that when L is H or benzyl; Z is a bivalent radical of formula (b-1) with p being 1 or 2, or (b-2) R1 is hydrogen, C1-6alkyl, halo, formyl, carboxyl, ethenyl substituted with carboxyl or C1-6alkyloxycarbonyl, or Ci-ealkyl substituted with hydroxyl, carboxyl or C1-6alkyloxycarbonyl; R2 is hydrogen, C1-6alkyl, hydroxy C1-6alkyl, aryl or halo; and R6 is C1-6alkyl, halo, ethenyl substituted with carboxyl or C1-6alkyloxycarbonyl, hydroxy Ciealkyl, formyl, carboxyl or hydroxycarbonylC1-6alkyl; then n is 2.

Full Text	FORM 2 THE PATENTS ACT 1970 [39 OF 1970] & THE PATENTS RULES, 2003 COMPLETE SPECIFICATION [See Section 10; rule 13] "A SPIRO COMPOUND OF FORMULA (I)" JANSSEN PHARMACEUTICA N.V., of Tumhoutseweg 30, Beerse, B-2340, Belgium The following specification particularly describes the invention and the manner in which it is to be performed: 17-1-2007 12 APR 2006 The presentnvention is concernea with spiro compounds having antihistaminic activity. It further relates to their use as a medicine, their preparation as well as compositions comprising them. WO 97/24356,.published on 10 July 1997, discloses 4-(imidazo-azepine) piperidine spiro derivatives as intermediates in the preparation of l-(l,2-disubstituted piperidinyl)-4-(imidazo-azepine) piperidine spiro derivatives having tachykinin antagonistic activity. Surprisingly, the 4-(imidazo-azepine) piperidine spiro derivatives of the present invention show an interesting antihistaminic activity profile. The present invention concerns compounds of formula (I) for use as a medicine, characterized in that the compounds of formula (I) are defined as (D their prodrugs, /V-oxides, addition salts, quaternary amines and stereochemically isomeric forms wherein R is hydrogen, C1-6alkyl, halo, formyl, carboxyl, C1-6alkyloxycarbonyl, C1-6alkyl- carbonyl, N(R3R4)C(=0)-, N(R3R4)C(=0)N(R5)-. ethenyl substituted with carboxyl or C1-6aIkyloxycarbonyl, or C1-6alkyl substituted with hydroxy, carboxyl, C1-6alkyloxy, C1-6alkyloxycarbonyl, N(R3R4)C(=0)-, C1-6alkylC(=0)N(R5)-, C1-6alkylS(=0)2N(R5)- or N(R3R4)C(=0)N(R5)-; wherein each R3 and each R4 independently are hydrogen or C1-6alkyl; R5 is hydrogen or hydroxy; R2 is hydrogen, C1-6alkyl, hydroxyC1-6aIkyI, C1-6alkyloxyC1-6aIkyl, N(R3R4)C(=0):, aryl or halo; n is 1 or 2; -A-B- represents a bivalent radical of formula -Y-CH=CH- (a-1); -CH=CH-Y- (a-2); or -CH=CH-CH=CH- (a-3); wherein each hydrogen atom in the radicals (a-1) to (a-3) may independently be replaced by R6 wherein R6 is selected from C1-6alkyl, halo, hydroxy, C1-6alkyloxy, ethenyl substituted with carboxyl or C1-6alkyloxycarbonyl, hydroxyC1-6alkyl, formyl, carboxyl and hydroxycarbonylC1-6alkyl; each Y independently is a bivalent radical of formula -0-, -S- or -NR7-; wherein R7 is hydrogen, C1-6alkyi or C1-6alkylcarbonyl; Z is is a bivalent radical of formula -(CH2)P- (b-1). -CH2-0- (b-4), -CH=CH- (b-2), -CH2-C(=Q)- (b-5),or -CH2-CHOH- (b-3). -CH2-C(=NOH)- (b-6), provided that the bivalent radicals (b-3), (b-4), (b-5) and (b-6) are connected to the nitrogen of the imidazole ring via their -CH2- moiety; wherein p is 1, 2, 3 or 4; L is hydrogen; C1-6alkyl; C2-6alkenyl; C1-6alkylcarbonyI; C1-6alkyloxycarbonyl; C1-6alkyl substituted with one or more substituents each independently selected from hydroxy, carboxyl, C1-6alkyloxy, C1-6a]kyloxycarbonyl, aryl, aryloxy, cyano or R8HN- wherein R8 is hydrogen, C1-6alkyl, C1-6alkyloxycarbonyl, C1-6alkylcarbonyl; or L represents a radical of formula -Alk-Y-Hetl (c-1), -Alk-NH-CO-Het2 (c-2) or -Alk-Het3 (c-3) ; wherein Alk represents C1-4alkanediyl ; Y represents O, S or NH ; Het1, Het2 and Het3 each represent furanyl, tetrahydrofuranyl, thienyl, oxazolyl, thiazoiyl or imidazolyl each optionally substituted with one or two C1-4alkyl substituents; pyrrolyl or pyrazolyl optionally substituted with formyl, hydroxyC1-4alkyl, hydroxycarbonyl, C1-4alkyloxycarbonyl or with one or two C1-4alkyl substituents; thiadiazolyl or oxadiazolyl optionally substituted with amino orC1-4alkyl; pyridinyl, pyrimidinyl, pyrazinyl or pyridazinyl each optionally substituted with C1-4alkyl, C1-4alkyloxy, amino, hydroxy or halo; and Het3 may also represent 4,5-dihydro-5-oxo-lH-tetrazolyl substituted with C1-4alkyl, 2-oxo-3-oxazolidinyl, 2,3-dihydro-2-oxo-lH-benzimidazol-l-yl or a radical of formula wherein A-Z represents S-CH=CH, S-CH2-CH2, S-CH2-CH2-CH2. CH=CH-CH=CH, or CH2-CH2-CH2-CH2; aryl is phenyl or phenyl substituted with 1, 2 or 3 substituents each independently selected from halo, hydroxy, C1-4alkyl, polyhaloC1-4alkyl, cyano, aminocarbonyl, C1-4alkyloxy or polyhaloC1-4alkyloxy. The compounds of formula (I) are deemed novel provided that 5,6-dihydrospiro[imidazo[l,2-b][3]benzazepine-l 1[1 lH],4'-piperidine] and pharmaceuucally acceptable addition salts thereof are not included and thus the present invention also relates to the compounds of formula (I) as defined hereinabove provided that 5,6-dihydrospiro[imidazo[l,2-b][3]benzazepine-l 1[1 lH],4'-piperidine] and pharmaceutically acceptable addition salts thereof are not included. The term prodrug as used throughout this text means the pharmacologically acceptable derivatives, e.g. esters and amides, such that the resulting biotransformation product of the derivative is the active drug as defined in the compounds of formula (I). The reference by Goodman and Gilman (The Pharmacological Basis of Therapeutics, 8 ' ed., McGraw-Hill, Int. Ed. 1992, "Biotransformation of Drugs", p. 13-15) describing prodrugs generally, is hereby incorporated. As used herein C1-4alkyl as a group or part of a group defines straight or branched chain saturated hydrocarbon radicals having from 1 to 4 carbon atoms such as methyl, ethyl, propyl, 1-methylethyl, butyl and the like; C1-4alkyl as a group or part of a group defines straight or branched chain saturated hydrocarbon radicals having from 1 to 6 carbon atoms such as the groups defined for C1-4alky! and pentyl, hexyl, 2-methylpropyl, 2-methylbutyl and the like; C2-6alkenyl as a group or part of a group defines straight and branched chain hydrocarbon radicals containing one double bond and having from 2 to 6 carbon atoms such as ethenyl, 2-propenyl, 2-butenyl, 2-pentenyl, 3-pentenyl, 3-methyl-2-butenyl, 3-hexenyl and the like. As used herein before, the term (=0) forms a carbonyl moiety when attached to a carbon atom and a sulfonyl moiety when attached twice to a sulfur atom. The term (=NOH) forms a hydroxylimine moiety when attached to a carbon atom. The term halo is generic to fluoro, chloro, bromo and iodo. As used in the foregoing and hereinafter, polyhaloC1-4alkyl as a group or part of a group is defined as mono- or polyhalosubstituted C1-4alkyl, in particular methyl with one or more fluoro atoms, for example, difluoromethyl or trifluoromethyl. In case more than one halogen atoms are attached to an alkyl group within the definition of polyhaloC1-4alkyl, they may be the same or different. When any variable (e.g. R3, R4 etc.) occurs more than one time in any constituent, each definition is independent. It will be appreciated that some of the compounds of formula (I), their prodrugs, N-oxides, addition salts, quaternary amines and stereochemically isomeric forms may contain one or more centers of chirality and exist as stereochemically isomeric forms. The term "stereochemically isomeric forms" as used hereinbefore defines all the possible stereoisomeric forms which the compounds of formula (I), their prodrugs, N-oxides, addition salts, quaternary amines or physiologically functional derivatives may possess. Unless otherwise mentioned or indicated, the chemical designation of compounds denotes the mixture of all possible stereochemically isomeric forms, said mixtures containing all diastereomers and enantiomers of the basic molecular structure as well as each of the individual isomeric forms of formula (I), their prodrugs, N-oxides, addition salts or quaternary amines substantially free, i.e. associated with less than 10%, preferably less than 5%, in particular less than 2% and most preferably less than 1% of the other isomers. Stereochemically isomeric forms of the compounds of formula (I) are obviously intended to be embraced within the scope of this invention. For therapeutic use, the addition salts of the compounds of.formula (I) are those wherein the counterion is pharmaceutically acceptable. However, salts of acids and bases which are not-pharmaceutically acceptable may also find use, for example, in the preparation or purification of a pharmaceutically acceptable compound. All salts, whether pharmaceutically acceptable or not are included within the ambit of the present invention. The pharmaceutically acceptable acid and base addition salts as mentioned hereinabove are meant to comprise the therapeutically active non-toxic acid and base addition salt forms which the compounds of formula (I) are able to form. The pharmaceutically acceptable acid addition salts can conveniently be obtained by treating the base form with such appropriate acid. Appropriate acids comprise, for example, inorganic acids such as hydrohalic acids, e.g. hydrochloric or hydrobromic acid, sulfuric, nitric, phosphoric and the like acids; or organic acids such as, for example, acetic, propanoic, hydroxyacetic, lactic, pyruvic, oxalic (i.e. ethanedioic), malonic, succinic (i.e. butane-dioic acid), maleic, fumaric, malic, tartaric, citric, methanesulfonic, ethanesulforiic, benzenesulfonic, p-toluenesulfonic, cyclamic, salicylic, p-aminosalicylic, pamoic and the like acids. Conversely said salt forms can be converted by treatment with an appropriate base into the free base form. The compounds of formula (I) containing an acidic proton may also be converted into their non-toxic metal or amine addition salt forms by treatment with appropriate organic and inorganic bases. Appropriate base salt forms comprise, for example, the ammonium salts, the alkali and earth alkaline metal salts, e.g. the lithium, sodium, potassium, magnesium, calcium salts and the like, salts with organic bases, e.g. the benzathine, N-methyl-D-glucamine, hydrabamine salts, and salts with amino acids such as, for example, arginine, lysine and the like. The term addition salt as used hereinabove also comprises the solvates which the compounds of formula (I) as well as the salts thereof, are able to form. Such solvates are for example hydrates, alcoholates and the like. Some of the compounds of formula (I) may also exist in their tautomeric form. Such forms although not explicitly indicated in the above formula are intended to be included within the scope of the present invention. An interesting group of compounds consists of those compounds of formula (I) wherein L is hydrogen, C1-6alkyl, C1-6alkylcarbonyl, C1-6alkyloxycarbonyl or C1-6alkyl substituted with hydroxy, carboxyl, C1-6alkyloxy or C1-6alkyloxycarbonyl; Another interesting group of compounds consists of those compounds of formula (I) wherein -A-B- is a bivalent radical of formula -CH=CH-CH=CH- (a-3). Also interesting compounds are those compounds of formula (I) wherein -A-B- is a bivalent radical of formula -CH=CH-Y- (a-2). Further interesting compounds are those compounds of formula (I) wherein Z is -(CH2)P- (b-1), -CH=CH- (b-2), or-CH2-0- (b-4). Other interesting compounds are those compounds of formula (I) wherein L is hydrogen, C1-6alkyl, carboxyC1-6alkyl, C1-6alkyloxycarbonyl, or C1-6alkyloxycarbonylC1-6alkyl. Again other interesting compounds are those compounds of formula (I) wherein L is hydroxyC1-6alkyl or C1-6alkyl substituted with aryl and C1-6alkyloxycarbonyl. Also further interesting compounds are those compounds of formula (I) wherein R1 is hydroxyC1-6alkyl, formyl, C1-6alkyloxycarbonyl, N(R3R4)C(=0)-, halo or hydrogen. Other interesting compounds are those compounds of formula (I) wherein R1 is C1-6alkyloxyC1-6alkyl. Special compounds are those compounds of formula (I) wherein one or more of the following restrictions apply: -A-B- is a bivalent radical of formula -CH=CH-CH=CH- (a-3) wherein each hydrogen may independently be replaced by C1-6alkyl, C1-6alkyloxy, halo or hydroxy; Z is -(CH2)P- wherein p is 1,2,3 or 4, -CH2-C(=0)-, -CH2-CHOH-, -CH=CH-, -CH2-0-; L is hydrogen, C1-6alkyl or C1-6alkyloxycarbonyl; R1 is hydrogen, formyl, carboxyl, amide, halo, C1-6alkyloxycarbonyl, C1-6aiky! substituted with hydroxy, C1-6alkyloxy, -NH-C(=O)-C1-6alkyl, -NH-C(=0)-NH2, -NH-S02-C1-6alkyI; R2 is hydroxyC1-6 alkyl, C1-6alkyloxyC1-6alkyl, halo, amide. The most preferred compounds are: 5,6-dihydrospiro[llH-imida2o[2,l-b][3]benzazepine-ll,4'-piperidine]-3-carboxamide dihydrochloride (comp. 17); 1 '-butyI-5,6-dihydrospiro[imidazo[2,l-b] [3] benzazepine-l1-[1 lH],4'-piperidmej (comp. 3); 6,11 -dihydro- r-methylspiro[5H-imidazo[2,1 -b][3]benzazepine-11,4'-piperidine) cyc!ohexylsulfamate(l:2) (comp. 1); 6,Il-dihydrospiro[5-imidazo[2,l-b][3]benzazepine-ll,4'-piperidine]-3-methanolJ (E)-2-butenedioate (2:1) (comp. 18a); 3-chloro-6,ll-dihydrospiro[5H-imidazo[2,l-b][3]benzazepine-ll,4'-piperidine] (E)-2-butenedioate (1:1) (comp. 20); 6,ll-dihydro-3-(methoxymethyl)spiro[5H-imidazo[2,l-b][3]benzazepine-ll,4'- piperidine]. (E)-2-butenedioate (1:1) (comp. 58); 6,ll-dihydro-r-(2-hydroxyethyI)spiro[5H-imidazo[2,l-b][3]benzazepine-ll,4'- piperidine]-3-carboxamide (comp. 62); 6,11 -di hydro-1 '-methylspiro[5H-imidazo[2, l-b][3]benzazepine-11,4'-piperidine]-3- carboxamide monohydrate (comp. 80); ethyl 3-(aminocarbonyl)-6,ll-dihydro-a-phenylspiro[5H-imidazo[2,I-b][3]- benzazepine-1 l,4'-piperidine]-l'-propanoate monohydrochloride (comp. 64); 3-(aminocarbonyl)-6,ll-dihydrospiro[5H-imidazo[2,l-b][3]-benzazepine-ll,4'- piperidine]-r-carboxylate (comp. 79); spiro[10H-irnidazo[l,2-a]thieno[3,2-d]azepine-10,4'-piperidine] (comp. 56a); 6,11 -dihydrospiro[5H-imidazo[2,I-b][3]benzazepine-l l,4'-piperidine]-2,3- dicarboxamide dihydrochloride monohydrate (comp. 53); a prodrug, a N-oxide, an addition salt, a quaternary amine or a stereochemically isomeric form thereof. The present invention also concerns novel compounds of formula (n-a) their N-oxides, addition salts, quaternary amines and stereochemically isomeric forms, wherein R1 is hydrogen, C1-6alkyl, halo, formyl, carboxyl, C1-6alkyloxycarbonyl, C1-6alkyl- carbonyl, N(R3R4)C(=0)-, N(R3R4)C(=0)N(R5)-, ethenyl substituted with carboxyl or C1-6alkyloxycarbonyl, or C1-6alkyl substituted with hydroxy, carboxyl, amino, C1-6alkyloxy, C1-6alkyloxycarbonyl, N(R3R4)C(=0)-, C1-6alkylC(=0)N(Rs)-, C1-6alkyiS(=0)2N(R5)- or N(R3R4)C(=0)N(R5)s wherein each R3 and each R4 independently are hydrogen or C1-4alkyl; R5 is hydrogen or hydroxy; __ -A-B-, Z, R2, and n are as defined for compounds of formula (I); and P represents a protective group for example, benzyl, or those protective groups mentioned in Chapter 7 of "Protective Groups in Organic Synthesis" by T. Greene and P. Wuyts (John Wiley & Sons, Inc. 1991), provided that 6,11-dihydro r-(phenylmethyl)-5H-spiro[imidazo[l,2-b][3]benzazepine- 11,4'-piperidine] (E)-2-butenedioate(l :2) is not included . The compounds of formula (II-a) are useful for the preparation of the compounds of formula (I). Interesting compounds are those compounds of formula (Il-a) wherein P is benzyl. Also interesting compounds are those compounds of formula (H-a) wherein R1 is hydrogen, halo, formyl, N(R3R4)C(=0)-, or C1-6allkyl substituted with hydroxy, amino, C1-6alkylC(=0)N(R5)-, C1-6alkylS(=0)2N(R5)- or N(R3R4)C(=0)N(Rs)- Further interesting compounds are those compounds of formula (TI-a) wherein -A-B- is a bivalent radical of formula (a-3) wherein each hydrogen atom may independently be replaced by C1-6alky!, halo, hydroxy, or C1-6alkyloxy. Again further interesting compounds are those compounds of formula (Il-a) wherein Z is a bivalent radical of formula (b-1) and n is 1. Compounds of formula (I), can be prepared by deprotecting an intermediate of formula (II), wherein P is a protecting group, for example, benzyl, or those protective groups mentioned in Chapter 7 of "Protective Groups in Organic Synthesis" by T. Greene and P. Woyts (John Wiley & Sons, Inc. 1991). Said deprotcction reaction can be performed by, for example, catalytic hydrogenation in the presence of hydrogen and an appropriate catalyst in a reaction inert solvent. A suitable catalyst in the above reaction is, for example, platinum-on-charcoal, palladium-on-charcoal, and the like. An appropriate reaction-inert solvent for said reaction is, for example, an alcohol, e.g. methanol, ethanol, 2-propanol and the like, an ester, e.g. ethylacetate and the like, an acid, e.g. acetic acid and the like. The thus obtained deprotected compounds can optionally further be derivatized either by replacing the hydrogen on the piperidine nitrogen by a moiety belonging to L, or by introducing on the imidazole moiety a R1 group or a R2 group or a R and R group, or by derivatizing both the piperidine moiety and the imidazole moiety. An intermediate of formula II can also first be derivatized at the imidazole moiety by introducing a Rl group or a R2 group or a R1 and R2 group, resulting in an intermediate of formula (II-a), and then be deprotected, followed optionally by a derivation at the piperidine nitrogen. Alternatively, compounds of formula (I), wherein Z is a bivalent radical of formula -CH2-C(=0)- (b-5), said compounds being represented by formula (I-a), can be prepared by cyclizing an intermediate of formula (HO in the presence of an acid, e.g. trifluoromethanesulfonic acid and the like. The compounds of formula (I) may further be prepared by converting compounds of formula (I) into each other according to art-known group transformation reactions. The compounds of formula (I) may be converted to the corresponding N-oxide forms following art-known procedures for converting a trivalent nitrogen into its N-oxide form. Said N-oxidation reaction may generally be carried out by reacting the starting material of formula (I) with an appropriate organic or inorganic peroxide. Appropriate inorganic peroxides comprise, for example, hydrogen peroxide, alkali metal or earth alkaline metal peroxides, e.g. sodium peroxide, potassium peroxide; appropriate organic peroxides may comprise peroxy acids such as, for example, benzenecarboper-oxoic acid or halo substituted benzenecarboperoxoic acid, e.g. 3-chlorobenzenecarbo-peroxoic acid, peroxoalkanoic acids, e.g. peroxoacetic acid, alkylhydroperoxides, e.g. t.butyl hydro-peroxide. Suitable solvents are, for example, water, lower alcohols, e.g. ethanol and the like, hydrocarbons, e.g. toluene, ketones, e.g. 2-butanone, halogenated hydrocarbons, e.g. dichloromethane, and mixtures of such solvents. The compounds of formula (I) wherein L is other than hydrogen, said L being represented by La and said compounds being represented by formula (I-b) can be prepared by reacting the compounds of formula (I) wherein L is hydrogen, said compounds being represented by formula (I-c), with a reagent of formula La-Wt (TV),wherein W1) is a suitable leaving group, such as a halo atom, e.g.chloro, or mesylate, tosylate, trifluoromethanesulfonate. Said reaction can conveniently be conducted in a reaction-inert solvent such as, for example, an aromatic hydrocarbon, an alkanol, a ketone, an ether, a dipolar aprotic solvent, a halogenated hydrocarbon, or a mixture of such solvents. The addition of an appropriate base such as, for example, an alkali or an earth alkaline metal carbonate, hydrogen carbonate, alkoxide, hydride, amide, hydroxide or oxide, or an organic base, such as, for example, an amine, may be utilized to pick up the acid which is liberated during the course of the reaction. In some instances the addition of an iodide salt, preferably an alkali metal iodide, is appropriate. Somewhat elevated temperatures and stirring may enhance the rate of the reaction. The compounds of formula (I-b), wherein La is optionally substituted C1-6alkyl, said L, being represented by Lai and said compounds by formula (I-b-1), can be converted into the compounds of formula (I-c) by dealkylating and subsequently carbonylating the compounds of formula (I-b-1) with a reagent of formula (V), wherein W2 represents a suitable leaving group, such as a halo atom, e.g. chloro, and L,2 represents C1-6alkyloxycarbonyl, resulting in compounds of formula (I-b-2) and subsequently hydrolyzing the thus obtained compounds of formula (I-b-2). The reaction with reagent (V) is conveniently conducted by stirring and heating the starting material with the reagent in an appropriate solvent and in the presence of a suitable base. Appropriate solvents arc, for example, aromatic hydro-carbons, e.g. methylbenzene, dimethylbenzene, chlorobenzene; ethers, e.g. 1,2-dimethoxyethane; methylenechloride and the like solvents. Suitable bases are, for example, alkali or earth alkaline metal carbonates, hydrogen carbonates, hydroxides, or organic bases such as, N,N-diethyIethanamine, N-(l-methylethyI)-2-propanamine, and the like. The compounds of formula (I-b-2) are hydrolyzed in acidic or basic media following conventional methods. For example, concentrated acids such as hydrobromic, hydrochloric acid or sulfuric acid can be used, or alternatively bases such as alkali metal or earth alkaline metal hydroxides in water, an alkanol or a mixture of water-alkanol may be used. Suitable alkanols are methanol, ethanol, 2-propanol and the like. In order to enhance the rate of the reaction it is advantageous to heat the reaction mixture, in particular up to the reflux temperature. The compounds of formula (I-b-2) can also be prepared by reacting compounds of formula (I-c) with a reagent of formula (V) in the presence of a suitable base, e.g. N,N-diethylethanamine, in a reaction inert solvent, e.g. methylenechloride, or by reacting compounds of formula (I-c) with a reagent of formula (VI), e.g. t-butyloxyanhydride, in a suitable solvent, such as, e.g. methylenechloride. The compounds of formula (I-b) wherein R1 or Rl and R represent hydroxymethyl, said compounds being represented by formula (I-b-3) and (I-b-4) can be prepared by reacting the compounds of formula (I) wherein L is La and Rl and R2 are hydrogen, said compounds being represented by formula (I-b-5), with formaldehyde, optionally in the presence of an appropriate carboxylic acid - carboxylate mixture such as, for example, acetic acid - sodium acetate and the like. In order to enhance the rate of the reaction, it is advantageous to heat the reaction mixture up to the reflux temperature. The thus obtained compounds of formula (I-b-3) and (I-b-4) can be further oxidized to the corresponding aldehyde, represented by formula (I-b-6) and (I-b-7) or the corresponding carboxylic acid, represented by formula (I-b-8) and (I-b-9), by reaction with a suitable reagent such as, for example, manganese(TV)oxide, respectively, silver nitrate. The compounds of formula (I-b-8) and (I-b-9) can further be converted in the corresponding amide, said compounds being represented by formula (I-b-10) and (I-b-11), by reaction with a suitable carbodiimide, e.g. l-(3-dimethylaminopropyl)-3-ethylcarbodiimide, in the presence of ammonia and a suitable catalyst, e.g. N.N-dimethylarninopyridine, in a reaction inert solvent, e.g. methylenechloride. The compounds of formula (I) wherein L is La, and R1 or R1 and R2 are halo, said compounds being represented by formula (I-b-12) and (I-b-13), can be prepared by halogenating a compound of formula (I-b-5) with an appropriate halogenating reagent in a reaction-inert solvent. A suitable halogenating reagent in the above reaction is, for example, an Af-halogenated amide, e.g. N,N-bromosuccinimide. A suitable reaction-inert solvent for said halogena-tion reaction is, for example, N,N-dimethylformamide, N,N-dimethylacetamide, methylenechloride and the like. Another suitable halogenating reagent is, for example, tetrabutylammoniumtribromide in the presence of a suitable base, e.g. sodium carbo¬nate, in a suitable solvent, e.g. 3-methyl-2-butanone or dichloromethane/water mixture. Compounds of formula (I-b-12) can be converted in a compound of formula (I-b-10) by reaction with CuCN in the presence of a suitable solvent, e.g. N,N-dimemylfonnamide/ water mixture. The compounds of formula (I-b) wherein R1 is C1-6aIkyloxycarbonylethenyl, said compounds being represented by formula (I-b-14), can be prepared by reacting a compound of formula (I-b-6) with a reagent of formula (VH) in the presence of a base e.g. piperidine, pyridine, and the like. The compounds of formula (I-b-14) can further be hydrolyzed into a compound of formula (I-b) wherein R1 is carboxyethenyl, in the presence of an acid or a base in case La is C1-6alkyl, or in the presence of a base, in case La is C1-6alkyloxycarbonyl. Compounds of formula (I-b) wherein 1, is substituted ethyl, said La being represented by La3-CH2-CH2-, and said compounds by formula (I-b-15) can be prepared by reacting a compound of formula (I-c) with a reagent of formula (VE) in the presence of a suitable base, e.g. sodium bicarbonate or triethylamine, in a suitable reaction inert solvent, e.g. N,N-dimethylformamide or a suitable alkanol, e.g. methanol. Compounds of formula (I-c) may also be converted into compounds of formua(I-b-15) wherein La3 is hydroxy, said compounds being represented by formula (I-b-15-1) by reaction with ethylene oxide in the presence of a suitable base, e.g. triethylamine, in a suitable reaction inert solvent, such as an alkanol, e.g: methanol. Compounds of formula (I) wherein Z is a bivalent radical of formula -CH2-CHOH-(b-3), said compounds being represented by formula (I-d), can be prepared by reducing a compound of formula (I-a) in the presence of a reducing reagent, e.g. sodium borohydride, in a reaction-inert solvent, e.g. methanol and the like. Compounds of formula (I) wherein Z is a bivalent radical of formula -CH2-C(=N-OH)-(b-6), said compounds being represented by the formula (I-e), can be prepared by reacting a compound of formula (I-a) with hydroxylamine or a salt thereof, e.g. the hydrochloride salt, in a reaction inert solvent, e.g. pyridine and the like. Compounds of formula (I) wherein Z is a bivalent radical of the formula -CH=CH-(b-2), said compounds being represented by formula (I-f). can be prepared by reacting a compound of formula (I-d) in the presence of an acid, e.g. methanesulfonic acid and the like. Compounds of formula (I-b) wherein La is C1-6alkyl substituted with C1-6alkyloxy-carbonyl or C1-6alkyloxycarbonylNH-, can be converted into compounds of formula (I-b) wherein La is C1-6alkyl or aminoC1-6aIkyl by the hydrolysis reaction described above for the preparation of compounds of formula (I-c). In the foregoing and the following preparations, the reaction mixture is worked up following art-known methods and the reaction product is isolated and, if necessary, further purified. As described hereinabove, the intermediates of formula (II) can be derivatized at the imidazole moiety, said compounds being represented by formula (Il-a), before being deprotected. Introducing R1 or R1 and R2 wherein R1 and R2 represent hydroxymethyl, formyl. carboxyl or amide, in a compound of formula (II) can be performed as described herinabove for the preparation of a compound of formula (I-b-3), (I-b-4), (I-b-6), (I-b-7). (I-b-8). (I-b-9). (I-b-10), (I-b-11). Intermediates of formula (II-a), wherein Rl is aminomethyl and R is hydrogen, said intermediates being represented by formula (Il-b), can be prepared by reacting an intennediate of formula (II-c) with hydrogen and a mixture of methanol/ammonia in the presence of a suitable catalyst, for example rhodium on aluminium, in the presence of a catalyst poison, for example a thiophene solution. Intermediates of formula (II-a), wherein R1 is -CH2NHC(=0)NH2 and R2 is hydrogen, said intermediates being represented by formula (H-d) can be prepared by reacting an intermediate of formula (II-b) with potassium isocyanate in an appropriate acid, such as hydrochloric acid. Intermediates of formula (II-b) can also be converted in an intermediate of formula (Il-a), wherein R1 is -CH2NHC(=0)C1-6alkyl and R2 is hydrogen, said intermediate being represented by formula (II-e), by reaction with a reagent of formula (IX), wherein W3 represents a suitable leaving group, such as a halo atom, for example chloro, in the presence of a suitable base, e.g. N,N-diethylethanamine, in a reaction inert solvent, such as, for example methylenechloride. Intermediates of formula (II-b) can further be converted into an intermediate of formula (Il-a), wherein R1 is -CH2NHS(=O)2=C1-6alkyl and R2 is hydrogen, said intermediate being represented by formula (Of), by reaction with a reagent of formula (X) wherein W4 represents a suitable leaving group, such as a halo atom, e.g. chloro, in the presence of a suitable base, for example N,Ndiethylethanamine, in a reaction inert solvent, such as methylenechloride. Intermediates of formula (II) can also be halogenated according to the procedure described for the preparation of the compounds of formula (I-b-12) and (I-b-13), resulting in an intermediate of formula (II-g) and (II-h). Intermediates of formula (Il-g) and (H-h) can be converted in an intennediate of formula (II-i) and (II-j) by reaction under an atmosphere of ammonia and carbonmonoxide at elevated temperatures in the presence of a suitable catalyst, e.g. acetic acid, palladium salt, and a suitable ligand, e.g. l.3-bis(diphenylphosphino)-propane, in a reaction inert solvent, e.g. tetrahydrofuran. In the following paragraphs, there are described several methods of preparing the starting materials in the foregoing preparations. Intermediates of formula (II), wherein Z is a bivalent radical of formula -(CH2)P- (b-1), said Z being represented by Z1 and said intermediates being represented by formula (Il-k), can be prepared by cyclizing an alcohol of formula (XI). The intermediates of formula (Il-k) may optionally be derivatized at the imidazole moiety resulting in an intermediate of formula (II-a-1) according to the procedures described for preparing a compound of formula (I-b-3), (I-b-4), (I-b-6) to (I-b-11) and an intermediate of formula (Il-b)to(II-j). Said reaction is conveniently performed in a reaction inert solvent such as, for example tetrahydrofuran, in the presence of a suitable base such as lithium diisopropylamide and butyl lithium. Intermediates of formula (II), wherein Z represents a bivalent radical of formula -(CH2)p (b-1), or -CH2-O- (b-4), said Z being represented by Z2, and said intermediates being represented by fonnula (II-l), can also be prepared by reacting a tricyclic moiety of formula (XTV) with a reagent of formula (XV), wherein Ws represents a suitable leaving group, e.g. a halo atom, such as chloro, under an inert atmosphere in a reaction inert solvent, such as tetrahydrofuran, in the presence of a suitable base such as, for example, lithium diisopropylamide and butyl lithium. The intermediates of formula (II-1) may optionally be derivatized at the imidazole moiety resulting in an intermediate of formula (II-a-2) according to the procedures described for preparing a compound of formula (I-b-3), (I-b-4), (I-b-6) to (I-b-11) and an intermediate of fonnula (H-b) to (II-j). Intermediates of formula (XTV) can be prepared by cyclizing an intermediate of formula (XVI), according to the procedure descnbed for the preparation of intermediates of formula (II-k). Said reduction can be conducted in a suitable solvent, such as, for example methanol, in the presence of a suitable reducing agent, such as sodium borohydride. Intermediates of formula (XVI) can be prepared by reduction from the corresponding aldehydes, said intermediates being represented by formula (XVII). Intermediates of formula (XVI) can also be prepared by reacting an intermediate of formula (XVIII) with formol 38% solution under pressure. Alternatively, the tricyclic moieties of formula (XIV), wherein Z represents a bivalent radical of formula -CH2-, said Z being represented by Z3, and said tricylclic moieties being represented by formula (XlV-a), may also be prepared by first cyclizing an intermediate of formula (XVH) wherein Z2 represents Z3, said intermediate being represented by formula (XVII-a), by treating said intermediate with an appropriate acid, e.g. trifluoroacetic acid, leading to an intermediate of formula (XIX), followed by reduction in the presence of a suitable reducing agent. Said reduction reaction can be performed in the presence of hydrogen and an appropriate catalyst in a reaction inert solvent. A suitable catalyst in the above reaction is, for example, platinum-on-charcoal, palladium-on-charcoal, and the like. An appropriate reaction inert solvent for said reaction is, for example, an alcohol, e.g. methanol, ethanol, 2-propanol and the like, an ester, e.g. ethylacetate and the like, an acid, e.g. acetic acid and the like. Intermediates of formula (III) can be prepared by reacting an intermediate of formula (XX) with a reagent of formula (XXI), wherein W6 represents a suitable leaving group, such as a halo atom, e.g. chloro, in the presence of a suitable base, e.g. sodium hydride, in a reaction inert solvent, e.g. N,N-dimethylformarnide and the like. Intermediates of formula (XX), wherein R1 and R2 are hydrogen, said intermediates being represented by formula (XX-a), can be prepared by debenzylating an intermediate of formula (XXII). Said debenzylation reaction can be performed by, for example, catalytic hydrogenation in the presence of hydrogen and an appropriate catalyst in a reaction inert solvent. A suitable catalyst in the above reaction is, for example, platinum-on-charcoal, palladium-on-charcoal, and the like. An appropriate reaction inert solvent for said reaction is, for example, an alcohol, e.g. methanol, ethanol, 2-propanol and the like, an ester, e.g. ethylacetate and the like, an acid, e.g. acetic acid and the like. Intermediates of formula (XXII) can be prepared by imidazole formation out of an intermediate of formula (XXHI) in an acid, such as hydrochloric acid. (XXII) (XXIII) Intermediates of formula (XXHI) can be prepared by reacting an intermediate of formula (XXTV) with 2,2-dimethoxyethylamine in a reaction inert solvent, such as, for example N.N-dimethylformamide and the like. Intermediates of formula (XXIV) can be prepared by reacting an intermediate of formula (XXV) with thionylchloride. Intermediates of formula (XXV) can be prepared by substituting an intermediate of formula (XXVI) with benzylamine in the presence of a suitable base, e.g. //^-diethyl-ethanamine, in a reaction inert solvent, e.g. methylenechloride and the like. (XXVI) Pure stereochemically isomeric forms of the compounds of formula (I) may be obtained by the application of art-known procedures. Diastereomers may be separated by physical methods such as selective crystallization and chromatographic techniques, e.g., counter-current distribution, liquid chromatography and the like. The compounds of formula (I) as prepared in the hereinabove described processes are generally racemic mixtures of enantiomers which can be separated from one another following art-known resolution procedures. The racemic compounds of formula (I) which are sufficiently basic or acidic may be converted into the corresponding diastereomeric salt forms by reaction with a suitable chiral acid, respectively chiral base. Said diastereomeric salt forms are subsequendy separated, for example, by selective or fractional crystallization and the enantiomers are liberated therefrom by alkali or acid. An alternative manner of separating the enantiomeric forms of the compounds of formula (I) involves liquid chromatography, in particular liquid chromatography using a chiral stationary phase. Said pure stereochemically isomeric forms may also be derived from the corresponding pure stereochemically isomeric forms of the appropriate starring materials, provided that the reaction occurs stereospectfically. Preferably if a specific stereoisomer is desired, said compound will be synthesized by stereospecific methods of preparation. These methods will advantageously employ enantiomerically pure starting materials. A number of intermediates and starting materials are commercially available or are known compounds which may be prepared according to conventional reaction procedures generally known in the art. For example, the preparation of l-(l-phenyl-ethyl)-l//-imidazole is described in WO 92/22551. The compounds of formula (I), their prodrugs, N-oxides, addition salts, quaternary amines and stereochemically isomeric forms possess useful pharmacological properties. In particular they are active antihistaminic agents, which activity can be demonstrated by for instance the 'Histamine - induced Lethality in Guinea Pigs' test (Arch. Int. Pharmacodyn. Ther., 251,39-51,1981), *Protection of Rats from Compound 48/80 -induced Lethality" test (Arch. Int. Pharmacodyn. Ther., 234,164-176,1978), and 'Ascaris Allergy in Dogs' test (Arch. Int. Pharmacodyn. Ther., 251, 39-51,1981 and Drug Dev. Res., 8, 95-102, 1986). Some of the intermediates of formula (II-a) also have interesting pharmacological properties. The compounds of the present invention have a selective binding affinity for the H1 receptor, more in particular, they have a very low affinity for the 5HT2A serotonin receptor and the 5HT2C serotonin receptor. This dissociation between the H1 receptor binding affinity and the 5HT2c and 5HT2A receptor binding affinity renders it unlikely for the present compounds to cause appetite stimulation and inappropriate weight gain reported for some other H1-antagonists. An important asset of the present compounds is their lack of sedating properties at therapeutic dose levels, a troublesome side effect associated with many antihistaminic and antiallergic compounds. The non-sedating properties of the present compounds can be demonstrated, for example, by the results obtained in studying the sleep -wakefulness cycle of the rat (Psychopharmacology, 97, 436-442, (1989)) and the state of vigilance using EEG power spectra in wake rats (Sleep Research 24A, 118, (1995)). The compounds of the present invention are also characterized by the absence of relevant cardio-hemodynamic and electrophysiological effects such as QTc prolongation. An additional advantage of some of the present compounds is that they exhibit little or no metabolic transformations in animal and human liver, thus indicating a low risk for metabolic interactions. Another interesting feature of the present compounds relates to their fast onset ot action and the favorable duration of their action. The latter characteristic may enable the administration of the compound once daily. The present compounds have a favorable physicochemical profile, particularly in terms of solubility and chemical stability. In view of their physicochemical and pharmacological properties, the compounds of formula (I), their prodrugs, N-oxides, addition salts, quaternary amines and stereochemically isomeric forms thereof are very useful in the treatment of a broad range of allergic diseases such as, for example, allergic rhinitis, allergic conjunctivitis, chronic urticaria, pruritis, allergic asthma and the like. Also in view of their useful physicochemical and pharmacological properties the subject compounds may be formulated into various pharmaceutical forms for administration purposes. To prepare the antiallergic compositions of this invention, an effective amount of the particular compound, in base or acid addition salt form, as the active ingredient is combined in intimate admixture with a pharmaceutically acceptable carrier, which carrier may take a wide variety of forms depending on the form of preparation desired for administration. These pharmaceutical compositions are, desirably as unitary dosage forms, administered orally, parenterally, percutaneously, rectally or topically for systemic action, or for topical action. In case of oral liquid pharmaceutical preparations, comprising solutions, suspensions, syrups, elixirs and emulsions, any of the usual pharmaceutical media, such as, for example, water, glycols, oils, alcohols and the like, may be employed, whereas in case of oral solid pharmaceutical preparations, comprising powders, pills, capsules and tablets, excipients such as starches, sugars, kaolin, lubricants, binders, disintegrating agents and the like may be employed. Because of their ease in administration, tablets and capsules represent the most advantageous oral unit dosage forms, in which case solid pharmaceutical carriers are obviously employed. In case of injectable pharmaceutical compositions, the carrier will usually comprise sterile water, at least in large part, though other ingredients, such as semipolair solvents, may be included, for example, to aid solubility. Examples of carriers for injectable solutions comprise saline solution, glucose solution or a mixture of saline and glucose solution. Injectable solutions containing compounds of the aforementioned formulas may also be formulated in an oil for prolonged action. Appropriate oils for this purpose are, for example, peanut oil, sesame oil, cottonseed oil, com oil, soy bean oil, synthetic glycerol esters of long chain fatty acids and mixtures of these and other oils. For the preparation of injectable suspensions, appropriate liquid carriers, suspending agents and the like may be employed. In the compositions suitable for percutaneous administration, the carrier optionally comprises a penetration enhancing agent and/or a suitable wettable agent, oprionally combined with suitable additives of any nature in minor proportions, which additives do not cause any significant deleterious effects on the skin. Said additives may facilitate the administration to the skin and/or may be helpful for preparing the desired compositions. These compositions may be administered in various ways, e.g., as a transdermal patch, as a spot-on, as an ointment or as a gel. In case of pharmaceutical compositions for rectal administration, any of the usual excipients may be employed, comprising fat based and water soluble excipients, optionally combined with suitable additives, such as suspending or wetting agents. As appropriate compositions for topical application there may be cited all compositions usually employed for topically administering drugs e.g. creams, gellies, dressings, lotions, shampoos, tinctures, pastes, ointments, salves, ovules, powders, inhalations, nose sprays, eye drops and the like. Semisolid compositions such as salves, creams, gellies, ointments and the like will conveniently be used, but application of said compositions may be, for example, also by aerosol, e.g. with a propellent such as nitrogen, carbon dioxide, a freon, or without a propellent such as a pump spray or drops. It is especially advantageous to formulate the aforementioned pharmaceutical compositions in unit dosage form for ease of administration and uniformity of dosage. Unit dosage form as used in the specification and claims herein refers to physically discrete units suitable as unitary dosages, each unit containing a predetermined quantity of active ingredient calculated to produce the desired therapeutic effect in association with the required phannaceutical carrier. Examples of such unit dosage forms are tablets (including scored or coated tablets), capsules, pills, powder packets, suppositories, ovules, wafers, injectable solutions or suspensions, teaspoonfuls, tablespoonfuls and the like, and segregated multiples thereof. The present invention also relates to a method of treating warm-blooded animals suffering from allergic diseases by administering to said warm-blooded animals an effective anti-allergic amount of a compound of formula (I), a prodrug, //-oxide, addition salt, quaternary amine or stereochemically isomeric form thereof. The present invention further relates to the compounds of formula (I), their prodrugs, N-oxides, addition salts, quaternary amines and stereochemically isomeric forms thereof for use as a medicine, and hence, the use of the present compounds for the manufacture of a medicament for treating warm-blooded animals suffering from allergic diseases is also part of the present invention. In general it is contemplated that an effective antiallergic amount would be from about 0.001 mg/kg to about 2 mg/kg body weight, and more preferably from about 0.01 mg/kg to about 0.5 mg/kg body weight. In any event, an effective antiallergic amount may depend on the type and severity of the affliction to be treated and the evaluation of the physician prescribing the treatment with the subject drugs. The following examples are intended to illustrate the scope of the present invention. Experimental part Hereinafter, THF means tetrahydrofuran, DDPE means diisopropyl ether, DMF means N,N-dimethylformamide, DIPA means diisopropyl amine A. Preparation of .intermediate compounds Example Al a) A mixture of DIPA (1.4 mol) in THF (3000ml) was stirred at -70°C under N2 flow. Butyllithium 2.5 M/hexane (1.3 mol) was added portionwise at a temperature below - 40°C. The mixture was stirred at -70°C for 15 min. l-phenylethyl-lH-imidazole (1 mol) dissolved in THF was added dropwise at a temperature below -55°C. The mixture was stirred at -70°C for 1 hour. l-(phenylmethyl)-4-piperidinone (1.2 mol) dissolved in THF was added dropwise at a temperature below -55°C. The mixture was stirred at -70°C for 1 hour, then brought to room temperature, stirred at room temperature overnight and decomposed with H2O. The organic solvent was evaporated. The aqueous concentrate was extracted with CH2CI2. The organic layer was separated, dried (MgSO4), filtered and the solvent was evaporated. The residue was crystallized from DIPE (1100ml). The precipitate was Filtered off, washed with DEPE and dried, yielding 271g of 4-[l-(2-phenylethyl)-lH-imidazol-2-yl]-l-(phenylmethyl)-4-piperidinol (75%) (interm. 1). b) A mixture of intermediate (1) (0.75 mol) in trifluoromethanesulfonic acid (1500ml) was stirred at 65°C for 120 hours, then cooled, poured out on ice, alkalized with NaOH 50% and extracted with CH2CI2. The organic layer was separated, dried (MgS04). filtered and the solvent was evaporated. The residue was crystallized from DIPE/CH3CN (99/1) (1200ml). The precipitate was filtered off and dried, yielding 169.6g of 5,6-dihydro-r-(phenylmethyl)spiro[l lH-irnidazo[2,l-b][3]benzazepine- 1 l,4'-piperidine] (66%) (interm. 2). Example A2 l-(phenylmethyl)-4-[l-(phenylmethyl)1H-imidazol-2-yl]-4-piperidinol (0.124 mol) and AICI3 (0.31 mol) were stirred in a melt at 120°C for lh. The mixture was cooled, AICI3 (0.31 mol) was added and the mixture was stirred at 120°C for lh. The mixture was poured into ice, alkalized with NaOH 50% and extracted with CH2Cl2 The organic layer was dried (MgS04), filtered off and evaporated. The residue was purified by HPLC (eluent: CH2C12/(CH30H/NH3) 99/1). The pure fractions were collected and evaporated. The residue was converted into the hydrochloric acid salt (1:2) in (C2H5)2O, yielding 0.91 g of r-(phenylmethyl)spiro[imidazo[l,2-b]isoquinoline-10[5H],4'-piperidine] dihydrochloride.dihydrate (2%) (interm. 3; mp. 161.2 °C). Example A3 a) A mixture of intermediate (2) (0.09 mol) in CH2C12 (lOOOml) was cooled to 0°C. l-bromo-2,5-pyrrolidinedione (0.09 mol) was added portion wise over a 1-hour period. The organic layer was separated, washed with H2O, dried, filtered and the solvent was evaporated. The residue was purified by column chromatography over silica gel (eluent: CH2C12/CH30H 97.5/2.5 to 95/5). A pure fraction was collected and the solvent was evaporated. The residue was dissolved in ethanol and converted into the (E)-2-butenedioic acid salt (1:1). The precipitate was filtered off and dried, yielding 17.3g of 3-bromo-5,6-dihydro-1 '-(phenylmethyl)spiro[ 1 lH-imidazo[2, l-b](3]-benzazepine-ll,4'-piperidine (E)-2-butenedioate(I:l) (36%) (interm. 4). Part of this fraction (I6.5g) was taken up in H20, K2CO3 and CH2CI2. The mixture was separated into its layers. The aqueous layer was extracted with CH2CI2. The combined organic layer was dried (MgS04), filtered and the solvent was evaporated, yielding 12.9g of 3-bromo-5,6-dihydro-r-(phenylmethyl)spiro[llH-imidazo[2,l-b][3]benzazepine-l 1,4-piperidine (interm. 4a). b) A mixture of intermediate (4a) (0.21 mol), l.3-propanediylbis[diphenylphosphine] (2.5 g) and acetic acid, palladium(2+) salt (0.68 g) in THF (567 ml) was stirred in an autoclave at 150°C for 16 hours under NH3 (10 atm) and CO (30 atm). The mixture was filtered and the filtrate was evaporated. This residue was purified by column chromatography over silica gel (eluent: CH2CI2/C2H5OH 100/0 over 46 min to 70/30). The pure fractions were collected and the solvent was evaporated, yielding 36 g of 5,6-dihydro-l'-(phenylmethyl)spiro[ 1 lH-imidazo[2,l -b][3)benzazepine-l 1,4'-piperidine]-3-carboxamide (44%) (interm. 5). Example A4 a) A mixture of intermediate (2) (0.16 mol) and sodium acetate (45g) in formol 38% (300ml) and acetic acid (30ml) was stirred and refluxed for 6 hours, then cooled. poured out on ice and alkalized with a NaOH solution. The precipitate was filtered off and punftcd by column chromatography over silica gel (elucnl: CH2 Cl2/CH3OH 99/1) The desired tractions were collected and the solvent was evaporated. The residue was tnturatcd in CH3CN, filtered off and dried, yielding 13g of 5.6-dihydio-['-(phenyl-methy)spirol 11H Mmidazo[2,l-b\|(3]benzazepine-l 1,4' pipendme) 3 methanol (interm (o h) A mixture : intermediate (6) -0.032. mol) and MaO2 (65gm in chlon rrn (250ml) was stirred and refluxed for 2 hours, then cooled, filtered over dicaiite and the filtrate was evaporated, yielding 11g of 5,6-dihydro-r-(phenylmethyl)spiro( IIH-imidazo¬[2,1-b][3]benzazepine-l l,4'-pipendine]-3-carboxaldehyde (interm. 7). c) A mixture of intermediate (7) (0.0296 mol) in CH3OH/NH3 (500ml) was hydrogenated at 50°C with Rh/Al2O3 5% (2g) as a catalyst in the presence of a thiophene solution (2ml). After uptake of H2 (I equiv), the catalyst was filtered off and the filtrate was evaporated, yielding 1 Ig of 5,6-dihydro-l'-(phenylmethyI)spiro[ 1 [H-imidazo[2,l-b][3]benzazepine-ll,4'-piperidine]-3-methananvine (interm. 8). Pan of this fraction (lg) was purified by column chromatography over silica gel (eluenf. CH2Cl2/CH3OH/NH3)95/5). The pure fractions were collected and the solvent was evaporated The residue was dissolved m 2-propanol and converted into the hydro chloric acid ,alt (1:3) with 2-propanol/HCl The mixture was crystallized from DIPF The precipitate was filtered off and dried, yielding 0.8g of 5.6 dihydro l'-(phenvl-meth\! 1 //-imidazof 2.1 -hj[3)ben/azepine i ! .4' -pip-.-r idme} ■ .^ methanamine livdro, blonde i 1:3) hvdrate (IT) (interm Sai d) A mixture of intermediate (8) (0.0198 mol; HI li('i IN [ 1 1// imida/o(2,l b\|[3]benza7.epin]-3-yl\|methyl\|methyl\|urea (interm. 9) hxample A 5 A mixture of intermediate (8) (0.0295 mol) and tnethylamme (0035 mol) in CH2CJ2 (140ml) was stined at room temperature A solution ot acetyl chloride (0.03 mol) in CH2C12 (10ml) was added dropwise. The mixture was stined at room temperature for I hour and poured out into H2O. K2CO3 (2g) was added. The mixture was extracted with CH2Cl2 The organic layer was separated, washed with H2O2, dried, filtered and A mixture of intermediate 14 , (0.47 mol) in MCI 6N (1500ml) was stirred until a cloudy solution, then washed with CH2Cl2 (900ml). stirred at 80°C lor I hour, cooled. alkalized with a NaOH 50% solution and extracted with CH2CI2. The organic Iaver was separated, dried (MgS04), filtered and the solvent was evaporated The residue was crystallized from CH3CN. The precipitate was filtered off and dried, yielding 38.3g of l-rnethy!-4-phenyl-4-[l-pheny ethyl)-lH-imideatly1-2-yl\|piperidme (in term. 15). e) A mixture of intermediate (15) (0.195 mol) in methanol (350ml) was hydtogenated at room temperature for 18 hours with palladium on charcoal 10% (3g) as a catalyst. After uptake of H2 (1 equiv), the catalyst was filtered off and the filtrate was evaporated. The residue was crystallized from CH3CN. The precipitate was filtered off and dried, yielding 42.3g of 4-( 1 /Y-imidazol-2-yl)- 1-methyM-phenylpiperidine (90%) (interna. 16). 0 A mixture of sodium hydride 60% (0.232 mol) in DMF (150ml) was stirred at room temperature. Intermediate (16) (0.145 mol) dissolved in DMF (400ml) was added dropwise, The mixture was stirred at room temperature for 1 hour. Methyl 2-chloro- acetate (0.232 mol) dissolved in DMF (400ml) was added dropwise. The mixture was stirred at room temperature for 20 mm. poured out into a solution of NaHCO) (20g) in H2O (2000ml) and extracted with CH2Cl2 The organic Iaver was separated, dried (MgS04), filtered and the solvenf was evaporated. The residue was pun tied by column chromatograplu over silica gel ieiuem nCH2Cl3- 95/5). The pure. fractions uere collected and the solvent v.as evaporated, sickling 40 lg of metfnl 2-(!-metvT4-phenv!-4-pipend:nv!)-l// imidazole-1-acetate (88%) (interm I7' Example AS a) Reaction tinder N2 atmosphere A mixture of DIPA (0 455 mol) in THF (500 ml) was stirred at 78 '(.' Butylhtfnum, 2 5 Mhcxane (0 390 mol) was added dropwise at -4()°C. The mixture was stirred tor 15 min. then re-cooled to -78V A solution of 1 -(4-phcnylbutyl) T//-imidazole, prepared according to the procedure described m J. Chcm. Soe. Perkin Trans . 1 (1975), 17, 1670-1671, (0.325 mol) in THP (350 :nh was added dropwise at -60°C The mixture was stirred for one hour, then re-cooled to 78°C This mixture was added dropwise to a mixture of ;V,/V-dimethylfonnamide (0.390 mol, dry, pa) in THT: (500 nil), stined at -78°C The reaction mixture was stirred for one hour at -78°C, then allowed to warm to room temperature while stining overnight. A saturated aqueous NH4Cl solution (400 ml) was added and this mixture was extracted with THF. The separated organic layer was dned, filtered and the solvent evaporated, yielding 74.2 g of l-(4-phenylbutyl)-1 H-imidazole- 2-carboxamide (lntenm. 18). b) A mixture of intermediate (18) (0.325 mol) in methanol (1400 ml) was stirred at room temperature. NaBH4 (0.650 mol) was added portionwise and the reaction mixture was stirred for 2 hours at room temperature. The solvent was evaporated. The residue was taken up into water and this mixture was extracted with CH2C12. The separates organic layer was dried, filtered and the solvent evaporated. The residue was purified by column chromatography over silica gel (eluent: CH2CI2/CH3OH 100/0, 99/1, 97/3, 96/4, 95/5 and 93/7). The desired fractions were collected and the solvent was evaporated, yielding 49.5 gof l-(4-phenylbutyl)-lH-imidazole-2-methanol (66%) (interm. 19). c) A mixture of intermediate (19) (0.417 mol) in methajiesulfonic acid (960ml) was stirred at 120°C for 40 hours, then cooled, poured out on ice and alkalized with NH4OH. The organic layer was separated, dried, filtered and the solvent evaporated. This fraction was purified by HPLC over silica gel (eluent: CH2C12/CH30H 97/3). A pure fraction was collected and the solvent was evaporated. The residue was crystallized from DEPE. The precipitate was filtered off and dried, yielding 15.7g of 6,7,8,13-tetrahydro-5H-imidazo[2,l-b][3]benzazonine (18%) (interm. 20). d) A mixture of DIPA (0.151 mol) in THF (650ml) was stirred at -78°C under N2 flow. Butyllithium 2,5M in hexane (0.144 mol) was added dropwise at a temperature below -40°C. The mixture was stirred at -78°C for 15 min. Intermediate (20) (0.072 mol) in a small amount of THF was added dropwise at a temperature below -55oC The mixture was stirred at -78°C for 1 hour. N,N-bis(2-chloroethyl)benzenernethanamine hydrochloride in a small amount of THF was added dropwise at a temperature below -SOX. The mixture was stirred at 78°C for 1 hour, allowed to warm to room temperature overnight and decomposed with H20. The organic solvent was evaporated. The aqueous concentrate was extracted with CH2C12. The organic layer was separated, dried, filtered and the solvent was evaporated. This fraction was purified by column chromatography over silica gel (eluent: CH2CI2/CH,OH 100/0, 99/1. 98/2, 96/4, 94/6 and 92/8). A fraction was collected and the solvent was evaporated, yielding 5,6,7,8-tetrahydro-1 '-(phenylmethyl)spiro[13H-imidazo[2,1 -b] [3 Jbenzazonine-13,4'-pipendine] (interm. 21), Example A9 A mixture of 5,10-dihydro-imidazo[l,2-blisoquinoIine-7.8-diol, obtained according to the procedure described in Ex.No. A8 c, (0.155 mol), phenyltrimethylammonium chloride (0.31 mol) and K2C03 (0.68 mol) in DMF (400ml) was stirred at 90°C for 20 hours, cooled, poured out into H2O and filtered over dicalite. The filtrate was separated into its layers. The organic layer was washed with H2O, dried (MgS04), filtered and the solvent was evaporated. The residue was purified over silica gel on a glass filter (eluent: CH2C12/CH30H 100/0 to 97/3). The pure fractions were collected and the solvent was evaporated, yielding 3g of 5,10-dihydro-7,8-dimethoxyimidazo[l,2-b]iso-quinoline (8.4%) (interm. 22). Example A10 A mixture of intermediate (31) (see Table 1), prepared according to the procedure described in Ex.No. A8d, (0.01 mol) in HBr 48 % solution (60ml) was stirred and refluxed for 2 hours. The solvent was evaporated The residue was taken up in a small amount of H20. The mixture was alkalized with K2CO3 and extracted with CH2CI2/CH3OH. The organic layer was separated, dried, filtered and the solvent was evaporated, yielding 4.3g of 5,6-dihydro-r-(phenylmethyl)spiro[l lH-imidazo-[2,l-bJ[3]benzazepine-ll,4'-piperidine]-8,9-diol (100%) (interm. 23). Example All A mixture of compound (22) (0.0117 mol) and triethyl amine (0.0421 mol) in toluene (100ml) was stirred and refluxed. Ethyl carbonochloridate (0.0702 mol) was added dropwise at reflux temperature. The mixture was stirred and refluxed for I hour, cooled, poured out into H2O and K2CO3 (15g) and separated into its layers. The aqueous layer was extracted with CH2CI2. The combined organic layer was dried (MgS04), filtered and the solvent was evaporated. The residue was punfied over silica gel on a glass filter (eluent: CH2Cl2/ethanol 96/4). The pure fractions were collected and the solvent was evaporated. The residue was boiled in DIPE. The precipitate was filtered off and dried, yielding 2.4g of [l'-(ethoxycarbonyl)spiro[ 1 l H-imidazo[2,l-b]-[3)benzazepme-ll.4'-piperidine)-6-yl] ethyl carbonate (33%) (interm. 24). Table 1 lists intermediates which were prepared according to one of the above mentioned examples. Table 1 B. Preparation of final compounds Example Bl (preparative example) A mixture of intermediate (2) (0.02 mol) in methanol (150ml) was hydrogenated with palladium on charcoal 10% (2g) as a catalyst at 50°C for 18hours. After uptake of H2 (leq), the catalyst was filtered and the filtrate was evaporated, yielding 5,6-dihydro-spiro[ 1 lH-imidazo[2,1 -b][3]benzazepine-1 l,4'-piperidine] (comp. 6; not claimed). This fraction was converted into the hydrochloric acid salt (1:1) in CH3CN, yielding 5g of 5.6-dihydrospiro(imidazo[l,2-b][3)benzazepine-l1[1 lHl,4'-piperidine] monohydrochloride (86%) (comp. 6a; not claimed). A fraction obtained in said way, can also be converted into the (E)-2-butenedioic acid salt. Example B2 a) A mixture of compound (6) (0.1 mol) and N,N-diethylethanamine (0.13 mol) in CH2C12 (300ml) was stirred at a temperature below 10°C. Ethyl carbonochloridate (0.12 mol) was added dropwise at this temperature. The mixture was allowed to warm to room temperature and then stirred at room temperature for 1 hour. Water and K2C03 (10g) were added. The mixture was separated into its layers. The aqueous layer was extracted with CH2C12. The combined organic layer was dried (MgSO4), filtered and the solvent was evaporated, yielding 35.4g of ethyl 5,6-hydrospiro[llH-imidazo-[2, l-b][3]benzazepine-U,4'-piperidine]-l-carboxylate (100%) (comp. 4). b) A mixture of compound (4) (0.1 mol), sodium acetate (0.3 mol) and acetic acid (0.258 mol) in formaldehyde 38% solution (165ml) was stirred and refluxed for 10 hours. The mixture was poured out into ice and a NaOH solution and extracted with CH2CI2. The organic layer was separated, dried (MgSO4), filtered and the solvent was evaporated. The residue was purified by column chromatography over silica gel (eluent: CH2Cl2/ethanol 95/5 to 90/10). The pure fractions were collected and the solvent was evaporated, yielding 16.5g of ethyl 5,6 dihydko-3(ydroxyrnethyi)spiro-[1 lH-irnida2o[2,l-b][3]-ben2azepine-ll14'-piperidine]-r-carboxylate (46%)(comp. 5). c) A mixture of compound (5) (0.046 mol) and potassium hydroxide (0.46 mol) in 2-propanol (130ml) was stirred and refluxed for 7 hours. The solvent was evaporated. The residue was taken up in water and extracted with CH2CI2. The organic layer was separated, dried (MgS04), filtered and the solvent was evaporated, yielding 11.5g of 5,6-dihydrospiro[llH-irrudazo[2,l-b][3]ber^azepine-ll,4'-piperidine]-3-methanol (88%) (comp. 18). Pan of this fraction (lg) was dissolved in CH3OH and converted into the (E)-2-butenedioic acid salt (2:1). The precipitate was filtered off and dried, yielding 0.6g of 5,6-dihydrospiro[l lH-irrudazo[2.1-b][3]benzazepine-ll,4'-piperidine]-3~methanol (E)-2-butenedioic acid salt (2:1) (comp. 18a). Example B3 A mixture of compound (6) (0.01 mol) and (CH20)n (0.066 mol) in methanol (150ml) and thiophene 4% solution (1ml) was hydrogenated with palladium on charcoal 10% (lg) as a catalyst at 50°C. After uptake of H2 (Ieq), the catalyst was filtered and the filtrate was evaporated. The residue was taken up in H2O/K2CO3/NH4OH and stirred. The mixture was extracted with CH2C12, dried, filtered and evaporated. The residue was converted into the cyclohexanesulfamic acid salt (1:2) in 2-propanone and recrystallized twice from 2-propanol, yielding 2.44g of 6,1 l-dihydro-l'-methyl-spiro[5H-imidazo[2,l-b][3]benzazepine-ll,4'-piperidine] cyclohexylsulfamate(l:2) (40%) (comp. I). Example B4 a) A mixture of 1-bromobutane (0.012 mol), compound (6) (0.01 mol), Na2C03 (0.02 mol) and potassium iodide (few crystals) in 2-butanone (200ml) was stirred and refluxed overnight. The mixture was evaporated, the residue was taken up in water and extracted with CH2C12. The organic layer was dried, filtered off and evaporated. The residue was purified by column chromatography over silica gel (eluent: CH2C12/ (CH3OH/NH3) 95/5). The pure fractions were collected and evaporated. The residue was converted into the hydrochloric acid salt (1:2) in 2-propanol. The precipitate was filtered and dried, yielding 0.7g of r-butyl-5,6-dihydrospiro[imidazo[2,l-b][3]-benzazepine-ll-[l lH],4'-piperidine] dihydrochloride.hemihydrate (18%) (comp. 3). b) A mixture of l-(3-chloropropoxy)-4-fluorobenzene (0.018 mol), 5,6-dihydro- spiro[llH-imidazo[2,l-b][3]benzazepine-ll,4'-piperidine] (0.015 mol), Na2C03 (0.015 mol) and Kl (10 mg) in 4-methyl-2-pentanone (200ml) was stirred and refluxed for 18 hours. The mixture was poured into water, separated and the aqueous layer was extracted with CH2C12. The organic layer was dried (MgS04), filtered off and evaporated. The residue was purified on a glass filter over silica gel (eluent: CH2C12/CH30H 90/10). The pure fractions were collected and evaporated. The residue was converted into the cyclohexylsulfamic acid salt (1:2) in 2-propanone. Yielding : 4.26gof l'-[3-(4-fluorophenoxy)propyl]-5,6Kiihydrospiro[irnidazo[2,l-b][3]benza- epine-11-[1 lH],4'-piperidine] cyclohexylsulfamate(l:2) (37%); mp. 180°C (comp. 71). c) A mixture of l-chloro-3-methyl-2-butene (0.02 mol), 5,6-dihydrospiro[ 11H-imidazo(2,l-b][3]benzazepine-ll,4'-piperidine] (0.015 mol), Na2C03 (0.015 mol) and Kl (0.015 mol) in N.N-dimethylaceetamide (150ml) was stirred at room temperature overnight. The mixture was filtered over dicalite and evaporated. The residue was taken up in CH2Cl2/water 95/5. The precipitate was filtered off and dried. Yielding : 0.86g of 5,6-dihydro-r-(3-methyl-2-butenyl)spiro[imidazo(2,l-b][3]benzazepine-ll-[11H],4'-piperidine] monohydroiodide (12.7%): mp. 255.4°C (comp. 74). d) A mixture of l-(2-bromoethyl)-4-ethyl-1.4-dihydro-5H-tetrazol-5-one (0.012 mol), 5,6-dihydrospiro[llH-imidazo[2,l-b][3]benzazepine-H,4'-piperidine] (0.01 mol), Na2C03 (0.01 mol) and Kl (10 mg) in 4-methyl-2-pentanone (200ml) was stirred and refluxed for 18 hours. The mixture was poured into water. The mixture was separated and the aqueous layer was extracted with 3-methyl-2-butanone, dried (MgSO4), filtered and evaporated. The residue was purified on a glass filter over silica gel (eluent: CH2Cl2/CH3OH 95/5 to 93/7). The pure fractions were collected and evaporated. The residue was converted into the hydrochloric acid salt (1:2) in C2H5OH. Yielding : 2.63g of l-[2-(5,6-dihydrospiro[llH-imidazo[2,l-b][3]benzazepin-ll,4'-piperidin]-r-yl)ethylH-ethyl-1,4-dihydro-5H-tetrazol-5-one dihydrochloride (56%); mp. 230°C (comp. 75). e) A mixture of chloroacetonitrile (0.11 mol), 5.6-dihydrospiro[llH-imidazo[2,l-b]-[3]benzazepine-l l,4'-piperidine] (0.1 mol) and MN-diethylethanamine (0.12 mol) in DMF (400ml) was stirred at room temperature for 48 hours . The mixture was poured into water and extracted with CH2C12. The organic layer was dried (MgS04), filtered off and evaporated. The residue was purified on a glass filter over silica gel (eluent: CH2CI2/CH3OH 96/4). The pure fractions were collected and evaporated. The residue was crystallized from CH3CN. Yielding: 18.5g5,6-dihydrospiro[irmdazo[2,l-b][3]-benzazepine-1 l-[l lH],4'piperidine]-r-acetonitrile (63%); mp. 152.6°C (comp. 76). Example B5 Bis(l,l-dimethylethyl) dicarbonate (0.095 mol) dissolved in a small amount of CH2Cl2 was added dropwise to a stirring mixture of compound (6) (0.079 mol) in CH2C12 (250ml). The mixture was stirred at room temperature for the weekend, then washed with H20, dried, filtered and the solvent was evaporated. Toluene was added and evaporated again. The residue was stirred in DIPE. The precipitate was filtered off and the filtrate was evaporated. This fraction was purified over silica gel on a glass filter (eluent: CH2C12/CH30H 100/0,99/1,98/2 and 9674). The pure fractions were collected and the solvent was evaporated. The residue was stirred in hexane. The precipitate was filtered off and dried, yielding 15.05g of 1,1-dimethylethyl 5,6-dihydrospiro[llH-imidazo[2,l-b][3]benzazepine-l l,4'-piperidine]-r-carboxylate (54%) (comp. 7). Example B6 a) A mixture of tetrahydro-2-furanmethanol methanesulfonate (0.0lmol), compound 6 (0.0lmol) and Na2C03 (002mol) in 4-methyl-2-pentanone (150ml) was stirred and refluxed overnight. The reaction mixture was filtered over dicalite. The filtrate was evaporated. The residue was purified by column chromatography over silica gel (eluent: CH2C12/(CH30H/NH3) 95/5). The pure fractions were collected and the solvent was evaporated. The residue was dissolved in 2-propanone and converted into the cyclohexane sulfamic acid salt (1:2). The precipitate was filtered off and dried. Yielding: 1.48g of 5,6-dihydro-r-[(tetrahydro-2-furanyl)methyI]spiro[imidazo[2,l-b] [3]benzazepine-l 1(1 lH],4'-piperidine] cyclohexylsulfamate(l:2) monohydrate (20.7%); mp. 120.2°C (comp. 72). b) A mixture of compound 6 (0.02 mol) and 2-thiophenecarboxaldehyde (0.053 mol) in methanol (300ml) was hydrogenated with Raney Nickel (2g) as a catalyst. After uptake of H2 (leq), the catalyst was filtered off and the filtrate was evaporated. The residue was purified by column chromatography over silica gel (eluent: CH2C12/ CH3OH 95/5). The pure fractions were collected and evaporated. The residue was converted into the cyclohexanesulfamic acid salt (1:1) in 2-propanone. The precipitate was filtered off and dried. The residue was recrystallized from 2-propanol. The precipitate was filtered off and dried. Yielding : 0.72g of 5,6-dihydro-l'-(2-thienyl- methyl)spiro[imidazo[2,l-b][3]benza2epine-l 1(1 lH],4'-piperidine] cyclohexyl-sulfamate(l:l) (6.6%); mp. 211.1°C (comp. 73). Example B7 a) A mixture of compound (9) (0.155 mol), prepared according to the procedure described in Ex. No. B2 b, and Mn02 (300g) in chloroform (1200ml) was stirred and refluxed for 90 min. The mixture was filtered over dicalite and the filtrate was evaporated. Part of this fraction (lg) was crystallized from CH3CN. The precipitate was filtered off and dried, yielding 0.5g of 1,1-dimethylethyl 3-formyl-5,6-dihydro-spirotinudazo[ 2,1-b][3] berizazepine-ll4'-piperidinel-l-carboxylate (comp. 12). b) A mixture of compound (12) (0.134 mol), NaCN (0.705 mol) and Mn02 (233g) in methanol (2500ml) was stirred at room temperature. Acetic acid (45.5ml) was added dropwxse. The mixture was stirred and refluxed for 20 hours and filtered over dicalite. The filtrate was evaporated. The residue was taken up in H20, CH2CI2 and K2C03. The mixture was separated into its layers. The aqueous layer was extracted with CH2CI2. The combined organic layer was dried (MgSCU), filtered and the solvent was evaporated. The residue was purified by column chromatography over silica gel (eluent: CH2Cl2/CH3OH 97/3). A pure fraction was collected and the solvent was evaporated, yielding 47.7g of methyl (1,1-dimethylethyl) 5,6-dihydrospiro[11H irnidazo[2,l-b][3]benzazepine-l l,4'-piperidine]-3,1'-dicarboxylate (87%) (comp. 13). c) A mixture of compound (13) (0.056 mol) in NaOH IN (100ml), H20 (250ml) and THF (250mJ) was stirred at room temperature for 18 hours. The organic solvent was evaporated. The aqueous concentrate was neutralized with HCI IN (100ml) and extracted with CH2C12. The organic layer was separated, dried (MgSO4), filtered and the solvent was evaporated. Part of this fraction (2g) was crystallized from CH3CN. The precipitate was filtered off and dried, yielding l.l6g of l'-[(l,l-dirnethylethoxy)-carbonyll-5,6-6jhydrospiro[llH-imidazo[2,l-b][3]benza2epine-ll,4'-piperidine]-3-carboxylic acid (comp. 14). d) A mixture of compound (14) (0.04 mol) and N,N-dimethyl-4-pyridinamine (0.04 mol) in CH2C12 (300ml) was stirred until complete dissolution. N.N-diethyl-ethanamine (0.05 mol) was added. Then Ar-(ethylcarbonirnidoyl)-N,N-dimethyl-l,3-propanediamine monohydrochloride (0.05 mol) was added portionwise. The mixture was stirred at room temperature for 30 min! N,N-diethylethanamine (0.06 mol) was added and then NH4Cl (0.05 mol) was added portionwise. The mixture was stirred at room temperature overnight, poured out into H2O and separated into its layers. The aqueous layer was extracted with CH2CI2. The combined organic layer was dried (MgSO4), filtered and the solvent was evaporated. The residue was purified by column chromatography over silica gel (eluent: CH2CI2/CH3OH 97.5/2.5). The pure fractions were collected and the solvent was evaporated. The residue was crystallized from CH3CN. The precipitate was filtered off and dried, yielding 9.5g of 1,1-dimethyIediyl 3 -(arru nocarbon yl )-5,6-dihydrospi ro[ 11 H midazo[2,1 -b] [3 ] benzazepine- 11 ,4'-piperidine]-r-carboxylate(60%)(comp. 16). e) A mixture of compound (16) (0.023 mol) in HCI/2-propanol (25ml) and methanol (100ml) was stirred and refluxed for 90 min and then cooled. The precipitate was filtered off and dried, yielding 8g of 5,6-dihydrospiro[l lH3 -imidazo[2,l-b][3]-tenzazepine-ll,4'-piperidine]-3-carboxamide dihydrochloride(94%)(comp. 17). The precipitate can also be converted into the (E)-2-butenedioic acid salt. 0 Preparation of compound 61 A mixture of compound (17) (0.0135 mol) and NaHC03 (0.0271 mol) in THF (100ml) and ethanol (50ml) was stirred and refluxed for 10 min. Methyl 2-propenoate (0.0149 mol) was added. The mixture was stirred and refluxed for 3 hours and then cooled. The solvent was evaporated under reduced pressure. The residue was partitioned between H20 and CH2C12. The organic layer was separated, dried (MgS04), filtered and the solvent evaporated. The residue was purified by column chromatography over silica gel (eluent: CH2C12/(CH30H/NH3) 95/5 to 90/10). The pure fractions were collected and the solvent was evaporated. The residue was purified again by column chromatography over silica gel (eluent: CH2CI2/(CH3OH/NH3) 99/1 to 97/3). The pure fractions were collected and the solvent was evaporated. The residue was refluxed in CH3OH/diethyl ether 2:8 (precipitation resulted). The precipitate was filtered off, washed with diethyl ether and dried in vacuo at 40°C overnight. Yielding: 2.27g of compound 61. g) /V,/V-diethylethanamine (0.0081 mol) was added at room temperature to a suspension of compound 17 (0.004 mol) in methanol (100ml). The mixture was cooled to 0°C. Oxirane was bubbled through the rruxture for 45 min. The mixture was allowed to warm to room temperature and then stirred at room temperature for 30 min. The solvent was evaporated under reduced pressure. The residue was purified by column chromatography over silica gel (eluent: CH2Cl2/(CH3OH/NH3) 97/3 to 95/5). The pure fractions were collected and the solvent was evaporated. The residue was crystallized from CH3OH/CH2C12 1:4. The precipitate was filtered off and dried. Yielding: 0.25g of 6,ll-dihydro-r-(2-hydroxyetehyl)spiro[5H-imidazo[2,l-b][3]-benzazepine-1 l,4'-pipendine]-3-carboxamide (18%) (compound 62). MN-diethylethanamine (0.0113 mol) was added at room temperature to a suspension of compound 17 (0.0054 mol) in methanol (100ml). After 5 min, oxirane was bubbled through the mixture at 0°C for 1 hour. The solvent was evaporated. The residue was suspended in t-butanol (200ml). Methyl chloroacetate (0.007 mol) andJV./V-diethyl-ethanamine (0.0054 mol) were added. The mixture was stirred and refluxed for 48 hours. The solvent was evaporated. The residue was purified by column chromato¬graphy over silica gel (eluent: CH2Cl2/(CH3OH/NH3) 98/2 to 95/5). Two fractions were collected and the solvent was evaporated. Fraction 1 was crystallized from CH3OH/CH3CN 1:3. The precipitate was filtered off and dried. The residue was purified by column chromatography over silica gel (eluent: CH2Cl2/(CH3OH/NH3) 97/3 to 95/5). The pure fractions were collected and the solvent was evaporated. Yielding: 0.46g of compound 63. i) N,N-diethylethanamine (0.0271 mol) was added at room temperature to a suspension of compound 17 (0.0129 mol) and ethyl a-methylenebenzeneacetate (0.0140 mol) in DMF (100ml). The mixture was stirred at room temperature over the weekend. The solvent was evaporated. The residue was extracted with CH2Cl2/H2O. The mixture was separated into its layers. The precipitate in the organic layer was filtered off. Yielding: 2.6g of ethyl 3-(aminocarbonyl)-6,l l-dihydro-a-phenylspiro[5H-irnidazo-[2,l-b][3]benzazepine-ll.4'-piperidinel-l'-propanoate monohydrochloride (compound 64). A mixture of compound 17 (0.0027 mol), l-(3-chloropropyl)-l,3-dihydro-2H-benzimidazol-2-one (0.003 mol). Na2CO3 (0.0027 mol) and Kl (few crystals) in CH3CN (100ml) was stirred and refluxed for 48 hours. The solvent was evaporated. The residue was purified by column chromatography over silica gel (eluent: CH2CI2/ (CH3OH/NH3) 99/1 to 95/5). Two fractions were collected and their solvents were evaporated. The desired fraction was purified again by column chromatography over silica gel (eluent: CH2Cl2/(CH3OH/NH3) 97/3 to 95/5). The pure fractions were collected and the solvent was evaporated. Yielding: 0.18g of compound 65. A mixture of isobutyl (2-chloroethyl)carbamoate (0.008 mol), 5,6-dihydrospiro[11H-imidazo[2,l-b][3]benzazepine-l l,4'-piperidine]-3-carboxamide dihydrochloride (0.004 mol). 4-methyl-2-pentanone (50 ml), Na2C03 (0.020 mol) and KI (catalytic quantity) was stirred and refluxed (oil bath: 130°C) overnight. The solvent was evaporated (vacuum, 60°C). Water was added. CH2CI2/CH3OH 90/10 was added. The organic layer was separated, dried (MgS04), filtered and the solvent was evaporated. The residue was purified by column chromatography over silica gel (eluent: CH2C12/ (CH3OH/NH3) 95/5). The desired fractions were collected and the solvent was evaporated. Yield: 1.5 g of compound 66 (85.4%). A mixture of compound 66 (0.00227 mol) and HCl/2-propanol (3 ml) in 2-propanol (30 ml) was stirred at 80°C (oil bath). The solvent was evaporated (vacuum, 40°C). 2-Propanol was added, then evaporated (2 x). Ethanol was added, then evaporated. The residue was stirred in boiling ethanol (50 ml), then filtered off over a P4 glass filter and the product was dried under a stream of N2. Yield: 0.254 g (24.0%). The filtrate was stirred for 3 hours while cooling on an ice-bath. The precipitate was filtered off over a P3 glass filter and dried (vacuum, 60°C, 3 hours). Yield: 0.304 g (28.7%). The filtrate was evaporated. The residue was dried (over the weekend under N2 flow). Total yield: 70.4% of compound 67. m) Methyl chloroformate (0.0036 mol) was added at room temperature to a suspension of compound (17) (0.0032 mol) in CH2C12 (100ml). A mixture of N,N-diethylethan-arrune (0.0097 mol) in CH2CI2 (20ml) was added dropwise. The mixture was stirred at room temperature for the weekend. The solvent was evaporated. The residue was purified by column chromatography over silica gel (eluent: CH2CI2/CH3OH 99/1 to 98/2). The pure fractions were collected and the solvent was evaporated. The residue was crystallized from CH3CN. The precipitate was filtered off and dried. Yield: 0.68g of 3-(aminocarbonyl)-6,l l-dihydrospiro(5H-imidazo[2,l-b][3]-benzazepine-l 1,4'-piperidine]-r-carboxylate (60%) (comp. 79). n) A mixture of compound (17) (0.005 mol), KOAc (2g) and paraformaldehyd (0.5g) in methanol (100ml) was hydrogenated with palladium on charcoal 10% (0.5g) as a catalyst in the presence of a thiophene solution (1ml). After uptake of H2 (1 equiv), the catalyst was filtered off and the filtrate was evaporated. The residue was purified by column chromatography over silica gel (eluent: CH2Cl2/(CH3OH/NH3) 97/3). The pure fractions were collected and the solvent was evaporated. This fraction was purified again by column chromatography over silica gel (eluent: CH2C12/(CH30H/NH3) 97/3 to 95/5). The pure fractions were collected and the solvent was evaporated. Yield: 0.43g of 6'11-Kiihydro-r-memylspiro[5H-imida2o[2,l-b][3]benzazepine-ll,4,-piperidine]-3-carboxamide monohydrate (28%) (comp. 80). Example B8 a) A solution of compound (7) (1.63 mol) in CH2C12 (7500ml) was cooled to 0°C under N2 flow. l-Bromo-2,5-pyrrolidinedione (1.63 mol) was added portionwise (29g each). H20 (3000ml) was added. The mixture was stirred overnight. The organic layer was separated, dried, filtered and the solvent was evaporated. This fraction was purified by HPLC over silica gel (eluent: CH2Cl2/CH3OH 100/0, 98/2, 90/10 and 100/0). A pure fraction was collected and the solvent was evaporated, yielding 189g of 1,1-dimethyl-ethyl 2.3-dib^omo-5,6-dihydrosp^ro[ll//-lmidazo[2,l-b][3]benzazepine-ll,4,-piperidine]-l'-carboxylate (27%) (comp 48). The 3-monobromo analogue (comp. 60; Ex. No. B 10a) can be prepared in a similar way. b) A mixture of compound (48) (0.02 mol), acetic acid, palladium(2+) salt (0.15g) and l,3-propanediylbis[diphenylphosphinej (0.55g) in THF (150ml) was stirred in an autoclave at 150°C for 16 hours under pressure of CO gas (30 bar) and NH3 gas (10 atm). The mixture was cooled, filtered and the filtrate was evaporated. This fraction was purified over silica gel on a glass filter (eluent: CH2Cl2/CH3OH 95/5). The pure fractions were collected and the solvent was evaporated. The residue was crystallized from CH3CN. The precipitate was filtered off and dried, yielding 1,1-dimethylethyl 2,3-bis(aminocarbonyl)-5,6-dihydrospiro[l lH-imidazo[2,l-b][3]benzazepme-ll,4'-piperidine] 1-1'-carboxylate (comp. 49) Example B9 Dibenzoyl peroxide (0.5g) was added to a stirring mixture of compound (7) (0.039 mol) in CH2CI2 (210ml). l-Chloro-2,5-pyrrolidinedione (0.078 mol) in a small amount of CH2C12 was added dropwise. The mixture was stirred at room temperature overnight. The solvent was evaporated. H20 was added and the mixture was extracted with CH2C12. The organic layer was separated, dried, filtered and the solvent was evaporated. The residue was purified over silica gel on a glass filter (eluent: CH2CI2/ CH3OH 100/0,99/1, 98/2,96/4 and 94/6). The pure fractions were collected and the solvent was evaporated. Some starting material (7.5g; 0.02 mol) was recuperated. The reaction was carried out again. Dibenzoyl peroxide (0.5g) was added to a stirring mixture of compound (7) (0.02 mol) in CH2CI2 (210ml). 1 -Chloro-2,5-pyrroIidinedione (0.078 mol) in a small amount of CH2Cl2 was added dropwise. The mixture was stirred at room temperature overnight. The solvent was evaporated. H20 was added and the mixture was extracted with CH2C12. The organic layer was separated, dried, filtered and the solvent was evaporated. The residue was purified over silica gel on a glass filter (eluent: CH2Cl2/CH3OH 100/0,99/1 and 98.5/1.5). The pure fractions were collected and the solvent was evaporated. The residue was combined with the one obtained from the first reaction, yielding 14g of 1,1-dimethylethyl 3-chloro-5,6-dihydrospiro[llH-imidazo[2,l-b][3]ben2azepine-ll,4,-piperidine]-r-carboxylate (93%) (comp. 19). Example B10 a) CH2C12 (87 ml) was added to 1,1-dimethylethyl 5,6-dihydrospiro[llH-imidazo[2,l- b][3]benzazepine-l l,4'-piperidinel-l'-carboxylate (comp. 7) in methanol (0,0582 mol). Water (58 ml) was added. Water (58 ml) and Na2CO3 (0.0582 mol) were added to the separated organic layer and the mixture was cooled to 0-5°C (solution I). Br2 (0.0565 mol) was added to a solution of tetrabutylammoniumbromide (0.0565 mol) and CH2C12 (29 ml). This mixture was stirred for 25 minutes at 15-25°C and added to solution 1 during I hour. After stirring for I hour at 20°C, water (58 ml) was added. The separated organic layer was evaporated. 3-Methyl-2-butanone (87 ml) and water (29 ml) were added to the oily residue and this mixture was heated to 80°C. The separated organic layer was wased with water (29ml) at 80°C. The organic layer was azeotroped till 116°C. 3-Methyl-2-butanone (40.7 ml) was distilled off and the product was crystallized during 2 hours at 50°C. The crystallized product was filtered off, washed with 3-methyl-2-butanone and dned (vacuum. 50°C). Yield : 13.03g of 1,1-dimethylethyl 3-bromo-5,6-dihydrospiro[l lH-imidazo[2,l-b][3]benzazepine-l 1,4'-piperidineH'-carboxylate (51.8%) (comp. 60). b) A mixture of compound (60) (0.257 mol), DMF (515 ml), H20 (26 ml) and CuGN (1,287 mol) were heated till 132°C, stirred for 17 hours and then cooled to room temperature. The mixture was poured into 2056 ml of H20 and stirred for 2 hours. The precipitate was filtered off, washed twice with H2O (149 ml) and dried (vacuum, 100°C). The resulting precipitate was refluxed in 3-methyl-2-butanone (772 ml) for 30 min, followed by cooling the reaction mixture to 50°C and filtering. NH4OH (129 ml) was added to the filtrate at 50°C and stirred for 30 min. The 3-methyl-2-butanone layer was separated and washed with NH4OH (129 ml) as described above. This procedure was repeated for another 5 times. The 3-methyl-2-butanone layer was separated again, azeotroped for 30 min and partially evaporated. The resulting mixture was crystallized and the precipitate was filtered, washed with 3-methyl-2-butanone (7.7 ml) and dried (vacuum, 50°C). Yield : 52.4 g of l,l-dimethylethyl 3-(aminocarbonyl)-5,6-dihydro-spiro[llH-imidazo[2,l-b][3]benzazepine-ll,4'-piperidine]-r-carboxylate (53%) (comp. 16). Example Bll a) A mixture of intermediate (18) (0.152 mol) in trifluoromethanesulfonic acid (500ml) was stirred at 158°C for 90 hours. The mixture was cooled, poured out on ice and K2C03 (800g) and extracted with CH2C12. The organic layer was separated, dried (MgSO4), filtered and the solvent was evaporated partially until 100ml while the temperature was kept below 40°C. The concentrate was purified immediately by column chromatography over silica gel (eluent: CH2Cl2/(CH30H/NH3) 95/5). The pure fractions were collected and the solvent was evaporated, yielding 18.lg of 1-methyl-spiro[llH-imidazo[2,l-b][3]benzazepine-l l,4'-piperidin]-6(5H)-one (42%) (comp. 22). Part of this fraction (1.5g) was dissolved in ethanol and converted into the (E)-2-butenedioic acid salt (2:3). The precipitate was filtered off and dned, yielding 1.92g of l-methylspiro[11H-imidazo[2,l b][3]benzazepine-ll,4'-piperidin]-6(5H)-one (E)-2-butenedioic acid salt (2:3) (comp. 22a). b) A mixture of intermediate (24) (0.041 mol) in HBr 48% solution (250ml) was stirred and refluxed for 4 hours. The mixture was poured out on ice and K2CO3 and extracted with CH2CI2. The organic layer was separated, dried (MgSO4), filtered and the solvent was evaporated, yielding 10.4gof spiro[llH-imidazo[2,l-b][3]benzazepine-ll,4'-piperidin]-6(5H)-one (95%) (comp. 23). Part of this fraction (0.9g) was dissolved in ethanol and converted into the (E)-2-butenedioic acid salt (2:3). The precipitate was filtered off and dried, yielding 0.78g of spiro[ 1 lH-imidazo[2,l-b][3]benzazepine-ll,4'-piperidin]-6(5H)-one (E)-2-butenedioic acid salt (2:3) (comp. 23a). c) A mixture of compound (23) (0.01 mol) in methanol (300ml) was stirred on an ice bath. NaBH4 (0.02 mol) was added portionwise over a 15-min period. The mixture was stirred on an ice bath for 1 hour. The solvent was evaporated at a temperature below 40°C. The residue was taken up in H2O and the mixture was extracted with CH2CI2/ CH3OH 90/10. The organic layer was separated, dried (MgS04), filtered and the solvent was evaporated, yielding 2g of 5,6-dihydrospiro[11H-imidazo[2,l-b][3]-benzazepine-ll,4'-piperidine]-6-ol (75%) (comp. 26). d) A mixture of compound (26) (0.0075 mol) in methanesulfonic acid (50ml) was stirred at room temperature for 40 min. The mixture was poured out on ice, alkalized with a NaOH 50% solution and extracted with CH2CI2- The organic layer was separated, dried (MgS04), filtered and the solvent was evaporated, yielding 2g of spiro[ll H-imidazo[2,l-b][3]benzazepine-l l,4'-piperidine] (100%) (comp.27). Part of this fraction (0.3g) was dissolved in ethanol and converted into the (E)-2-butenedioic acid salt (1:1). The precipitate was filtered off and dried, yielding 0.26g spiro[llH-imidazo[2,l-b](3]benzazepine-l l,4'-piperidine] (E)-2-butenedioic acid salt (1:1) (comp. 27a). Example B12 A mixture of compound (24) (0.0128 mol) in H2S04(5ml) and methanol (100ml) was stirred and refluxed for the weekend. The solvent was evaporated. The residue was taken up in H2O. The mixture was alkalized with a NaOH solution and extracted with CH2CI2. The organic layer was separated, dried, filtered and the solvent was evaporated, yielding 4.4g of 5,6-dihydro-2,3-bis(methoxymethyl)spiro[l1 H-imidazo¬[2,1,-b][3]benzazepine-11,4'-pipendine] (100%) (comp. 31). Example B13 a) A mixture of 5,6-dihydrospiro[imidazo(2,l-bl[3]benzazepine-l 1-[11H],4'-pipendine)-r-acetonitrile (comp. 76) (0 055 mol) in NH3/CH3OH (500ml) was hydrogenated with Raney Nickel (2g) as a catalyst at room temperature. After uptake of H2 (2eq), the catalyst was filtered off and the filtrate was evaporated. Yielding : 20.9gof 5,6-dihydrospiro(imidazo(2,l-bl[31benza2epine-ll-[llH],4'-piperidine]-r-ethanamine 2-propanolate(2:l). tnhydrochlonde. sesquihydrate; mp. 245.9°C (comp. 77). b) A mixture of 2-chloropyrimidme (0.012mol), 5,6-dihydro-spiro[imidazo[2,l-b][3]-benzazepine-1 l-[11H],4'-piperidine]l'-ethanamine (O.Olmol) and Na2C03 (0.02mol) in 4-methyl-2-pentanone (200ml) was stirred and refluxed for 48 hours. The reaction mixture was filtered over dicalite. The filtrate was evaporated. The residue was purified by column chromatography over silica gel (eluent: CH2C12/(CH30H/NH3) 95/5). The pure fractions were collected and the solvent was evaporated. The residue was dissolved in 2-propanol and converted into the hydrochloric acid salt (1:3). The precipitate was filtered off and dried. Yielding: 0.94g of 5.6-dihydro-N-2-pyrimidinyl-spiro[imidazo[2,l-b][3]benzazepine-11 -[ 11H]1,4'-piperidine]-l'-ethanamine trihydrochloride. monohydrate.2-propanolate(l:l) (16.7%) (comp. 78). c) 3-Chloro-6-(3-methyl4,2,4-th«adiazol-5-yl)pyridazine (0.01 mol) and 5,6-dihydro-spiro[imidazo[2,l-b][3]benzazepine-U-(l lH],4'-piperidinc]-r-ethananune (0.01 mol) were stirred at 140°C for 2h. The mixture was cooled and purified by column chromatography over silica ge! (eluent: CH2Cl2/(CH3OH/NH3) 95/5). The pure fractions were collected and evaporated. The residue was converted into the hydro¬chloric acid salt (1:4) in 2-piopanol and dned. Yielding : 2.22g of 2-[[2-(5,6-dihydro-spiro[imidazo[24-b][3]benza2epine-11-[11H],4'-piperidin]-1-yl)ethyl]amjno]-4(lH) pyrimidinone trihydrochloride.2-propanolate(l.T). sesquihydrate (36.6%) (comp. 68). The following Tables list compounds of formula (I) as prepared according to one of the above examples (Ex. No.). (1) cyclohexylsulfamate (1:2); (2) hydrochloric acid (1:2); (3) (E)-2-butenedioate (1:1); (4) (E)-2-butenedioate(2:l) Table 3 Co No. Ex. No. R1 -A-B- Salt/Melting point 57 58 B2c B12 H -CH2-0-CH3 -S-CH=CH--CH=CH-CH=CH- - (3) (E)-2-butenedioate (1:1); (5) hydrochloric acid (I: I); (6) (E)-2-butenedioate (2:3) Table 4 (E)-2-butenedioate (1:1); (5) hydrochloric acid (1:1); (6) (E)-2-butenedioate (2:3) (2) hydrochloric acid (1.2), (5) hydrochloric acid (1:1); (7) monohydrate; (8) hydrochloric acid (1:3) monohydrate Table 6 (1) cyclohexylsulfanute (1:2); (2) hydrochloric acid (1:2); (9) hydrochloric acid (13) hydrate (21) ethanolate (2:1); (10) cyclohexylsulfamate (1:2) hydrate (1:2); (11) cyclohexylsulfamate (1:1); (12) hydroiodic acid (I: I); (13) hydrochloric acid (1:3) hydrate (2:3) 2-propanolate (2:1); (14) hydrochloric acid (1:3) hydrate (1:1) 2-propanolate (1:1); (15) hydrochloric acid (1:3) hydrate (2:3) 2-propanolate (1:1) Table 7 (3) (E)-2-butenedioate (1:1) C. Pharmacological Example The ED50 values (mg/kg) in the test "Protection of Rats from Compound 48/80 induced Lethality" for the compounds of formula (I) are listed in the Table below. Compound No. ED50 (mg/kg) 1 2.5 3 2.5 17 0.04 18a 0.08 20 0.31 53 0.31 56a 2.5 58 2.5 62 0.63 64 0.31 79 0.04 80 0.63 D. Composition Examples The following formulations exemplify typical pharmaceutical compositions suitable for systemic or topical administration to warm-blooded animals in accordance with the present invention. "Active ingredient" (A.I.) as used throughout these examples relates to a compound of formula (I), a prodrug, an addition salt, a N-oxide, a quaternary amine or a stereochemically isomeric form thereof Example D1 : Oral drops 500 g of the A.I. is dissolved in 0.5 1 of 2-hydroxypropanoic acid and 1.5 1 of the polyethylene glycol at 60~80°C. After cooling to 30~40°C there are added 35 1 of polyethylene glycol and the mixture is stirred well. Then there is added a solution of 1750 g of sodium saccharin in 2.5 I of purified water and while stirring there are added 2.5 1 of cocoa flavor and polyethylene glycol q.s. to a volume of 50 I, providing an oral drop solution comprising 10 mg/ml of the A.I. The resulting solution is filled into suitable containers. Example D2: Oral solutions 9 g of methyl 4-hydroxybenzoate and 1 g of propyl 4-hydroxybenzoate are dissolved in 4 I of boiling purified water. In 3 1 of this solution are dissolved first 10 g of 2,3-dihydroxybutanedioic acid and thereafter 20 g of the A.I. The latter solution is combined with the remaining part of the former solution and 12 1 of 1,2,3-propanetriol and 3 1 of sorbitol 70% solution are added thereto. 40 g of sodium saccharin are dissolved in 0.5 1 of water and 2 ml of raspberry and 2 ml of gooseberry essence are added. The latter solution is combined with the former, water is added q.s. to a volume of 20 1 providing an oral solution comprising 5 mg of the A.I. per teaspoonful (5 ml). The resulting solution is filled in suitable containers. Example D3 : Capsules 20 g of the A.I., 6 g sodium lauryl sulfate, 56 g starch, 56 g lactose, 0.8 g colloidal silicon dioxide, and 12 g magnesium stearate are vigorously stirred together. The resulting mixture is subsequently filled into 1000 suitable hardened gelatin capsules, each comprising 20 mg of the A.I.. Example P4 : Film-coated tablets Preparation of tablet core A mixture of 100 g of the A.I., 570 g lactose and 200 g starch is mixed well and thereafter humidified with a solution of 5 g sodium dodecyl sulfate and 10 g polyvinyl¬pyrrolidone (Kollidon-K 90®) in about 200 ml of water. The wet powder mixture is sieved, dried and sieved again. Then there are added 100 g microcrystalline cellulose (Avicel®) and 15 g hydrogenated vegetable oil (Sterotex ®). The whole is mixed well and compressed into tablets, giving 10.000 tablets, each comprising 10 mg of the active ingredient. Coating To a solution of 10 g methyl cellulose (Methocel 60 HG®) in 75 ml of denaturated ethanol there is added a solution of 5 g of ethyl cellulose (Ethocel 22 cps ®) in 150 ml of dichloromethane Then there are added 75 ml of dichloromethane and 2.5 ml 1,2,3-propanetriol. 10 g of polyethylene glycol is molten and dissolved in 75 ml of dichloromethane. The latter solution is added to the former and then there are added 2.5 g of magnesium octadecanoate, 5 g of polyvinylpyrrolidone and 30 ml of concen¬trated colour suspension (Opaspray K-1-2109®) and the whole is homogcnated. The tablet cores are coated with the thus obtained mixture in a coating apparatus. WE CLAIM: 1. A spiro compound of formula a prodrug as herein described, a N-oxide as herein described, an addition salt as herein described, a quaternary amine as herein described or a stereochemically isomeric form thereof wherein R1 is hydrogen, C1-6alkyl, halo, formyl, carboxyl, C1- 6alkyloxycarbonyl, C1-6alkyl-carbonyl, N(R3R4)C(=0)-, N(R3R4)C(=0)N(R5)-, ethenyl substituted with carboxyl or C1-6alkyloxycarbonyl or C1-6alkyl substituted with hydroxy, carboxyl, C1-6alkyloxy, C1-6alkyloxycarbonyl, N(R3 R4)C(=0)-, C1-6alkylC(=0)N(R5)-, C1-6alkylS(=0) 2N(R5)-or N(R3 R4)C(=0)N(R5)-; wherein each R3 and each R4 independently are hydrogen or C1-4alkyl; R5 is hydrogen or hydroxy; R2 is hydrogen, C1-6alkyl, hydroxyC1-6alkyl, C1-6alkyloxyC1-6alkyl, N(R3 R4)C(=Q)-, aryl or halo; n is 1 or 2; -A-B- represents a bivalent radical of formula -Y-CH=CH- (a-1); -CH=CH-Y- (a-2); or -CH=CH-CH=CH- (a-3); wherein each hydrogen atom in the radicals (a-1) to (a-3) may independently be replaced by R6 wherein R6 is selected from C1-6alkyl, halo, hydroxy, C1-6alkyloxy, ethenyl substituted with carboxyl or C1-6alkyloxycarbonyl, hydroxyC1-6alkyl, formyl, carboxyl and hydroxycarbonylC1-6alkyl; each Y independently is a bivalent radical of formula -O-, -S- or -NR7-; wherein R7is hydrogen, C1-6alkyl or C1-6alkylcarbonyl; Z is a bivalent radical of formula -(CH2)p- (b-1), -CH2-C(=0)- (b-5), or -CH=CH- (b-2), -CH2-C(=NOH)- (b-6), -CH2-CHOH- (b-3), - CH2-O- (b-4), provided that the bivalent radicals (b-3), (b-4), (b-5) and (b-6) are connected to the nitrogen of the imidazole ring via their -CH2-moiety: wherein p is 1, 2, 3 or 4; L is hydrogen; C1-6alkyl; C1-6alkenyl; Ci-6alkylcarbonyl; C1-4alkyloxycarbonyl; C1-4alkyl substituted with one or more substituents each independently selected from hydroxy, carboxyl, C1-4alkylox, C1-6alkyloxycarbonyl, aryl, aryloxy, cyano or R8HN-wherein R8 is hydrogen, C1-6alkyl, C1-6alkyloxycarbonyl, C1-6alkylcarbonyl; or L represents a radical of formula -Alk-Y-Het1 (c-1), -Alk-NH-CO-Het2 (c-2) or -Alk-Het3 (c-3) wherein Alk represents C1-4 alkanediyl; Y represents O, S or NH: Het1, Het2 and Het3 each represent furanyl, tetrahydrofuranyl, thienyl, oxazolyl, thiazolyl or imidazolyl each optionally substituted with one or two C1-4 alkyl substituents, pyrrolyl or pyrazolyl optionally substituted with formyl, hydroxyC1-4alkyl, hydroxycarbonyl, C1-4alkyloxycarbonyl or with one or two C1-4alkyl substituents; thiadiazolyl or oxadiazolyl optionally substituted with amino or C1-4alkyl; pyridinyl, pyrimidinyl, pyrazinyl or pyridazinyl each optionally substituted with C1-4alkyl, C1-4 alkyloxy, amino, hydroxy or halo; and Het3 may also represent 4,5-dihydro-5-oxo-lH-tetrazolyl substituted with C1-4alkyl, 2-oxo-3-oxazolidinyl, 2-3-dihydro-2-oxo-lH-benzimidazol-l-yl or a radical of formula A-Z represents S-CH=CH, S-CH2-CH2, S-CH2-CH2-CH2, CH=CH-CH=CH, or CH2-CH2-CH2-CH2; atyl is phenyl or phenyl substituted with 1, 2 or 3 substituents each independently selected from halo, hydroxy, C1-4alky, polyhaloC1-4alkyl, cyano, aminocarbonyl, C1-4alkyloxy or polyhaloC1-4alkyloxy; provided that when L is H or benzyl; Z is a bivalent radical of formula (b-1) with p being 1 or 2, or (b-2) R1 is hydrogen, C1-6alkyl, halo, formyl, carboxyl, ethenyl substituted with carboxyl or C1-6alkyloxycarbonyl, or Ci-ealkyl substituted with hydroxyl, carboxyl or C1-6alkyloxycarbonyl; R2 is hydrogen, C1-6alkyl, hydroxy C1-6alkyl, aryl or halo; and R6 is C1-6alkyl, halo, ethenyl substituted with carboxyl or C1-6alkyloxycarbonyl, hydroxy Ciealkyl, formyl, carboxyl or hydroxycarbonylC1-6alkyl; then n is 2. 2. A compound as claimed in claim 1 wherein L is hydrogen, C1-6alkyl, C1-6alkylcarbonyl, C1-6alkycoxycarbonyl or C1-6alkyl substituted with hydroxy, carboxyl, C1-6alkyloxy or C1-6alkyloxycarbonyl. 3. A compound as claimed in claim 1 wherein L is C1-6alkyl substituted with aryl and C1-6alkyloxycarbonyl. 4. A compound as claimed in any one of the preceding claims wherein -A-B- is a bivalent radical of formula -CH=CH-CH=CH-(a-3) or -CH=CH-Y-(a-2). 5. A compound as claimed in any one of the preceding claims wherein Z is -(CH2) P- (b-1), -CH=CH- (b-2), or -CH2-O- (b-4). 6. A compound as claimed in claims 1, 2, 4 or 5 wherein L is hydrogen, Ciealkyl, hydroxyCi-ealkyl, carboxyCi-6alkyl, C1-6 alkyloxycarbonyl, or Ci-6alkyloxycarbonylCi-6alkyl. 7. A compound as claimed in any one of the preceding claims wherein R1 is hydroxyC1-6alkyl, formyl, C1-6alkyloxycarbonyl, C1-6alkyloxyC1-6alkyl, N(R3R4)C(=0)-, halo or hydrogen. 8. A compound as claimed in claim 1 wherein the compound is 5,6-dihydrospiro [11 H-imidazo [2, l-b][3]benzazepine-ll,4'-piperidine]-3-carboxamide dihydrochloride; l'-butyl-5,6-dihydrospiro[imidazo[2, l-b][3]benzazepine-11-[ 11H] ,4'-piperidine]; 6,1 l-dihydro-l'-methylspiro[5-H-imidazo[2, l-b][3]benzazepine-11,4'-pipendine]cyclohexylsulfamate(l :2); 6,ll-dihydrospiro[5-imidazo[2) l-b][3]benzazepine- 11, 4'-piperidine]-3-methanol) (E) -2-butenedioate (2:1); 3-chloro-6, 1 l-dihydrospir[5H-imidazo[2, l-b][3]benzazepine-11, 4>-piperidine] (E)-2-butenedioate (1:1); 6,1 l-dihydro-3-(methoxymethyl)spiro[5H-imidazo[2,1 -b][3]benzazepine- 11 ,4'- piperidine]. (E)-2-butenedioate (1:1); 6,11 -dihydro-1 '-(2-hydroxyethyl) spiro[5H-imidazo[2, 1 -b] [3]benzazepine-11 ^'-piperidinej-S-carboxamide; 6,11-dihydro-l'-methylspiro[5H-imidazo[2, l-b][3]benzazepine-1 l,4'-piperidine]-3-carboxamide monohydrate; ethyl 3-(aminocarbonyl)-6, 11 -dihydro-a-phenylspiro[5-imidazo[2, l-b][3)-benzazepine-ll, 4'-piperidine]-l'-prapanoate monohydrochloride; 3-(aminocarbonyl)-6, ll-dihydrospiro[5H-imidazo[2, l-b][3]benzazepine-ll, 4'-piperidine]-r-carboxylate; spiro[ 1 OH-irnidazo[l ,2-a]thieno[3,2-d]azepine-10,4'-piperidine]; 6, ll-dihydrospiro[5H-imidazo[2,l-b] [3]benzazepine- 11, 4'-piperidine]-2,3-dicarboxamide dihydrochloride monohydrate; a prodrug, a N-oxide, an addition salt, a quaternary amine or a stereochemically isomeric form thereof. A pharmaceutical composition comprising a pharmaceutically acceptable carrier, and as active ingredient a therapeutically effective amount of a compound as claimed in any one of claims 1 to 8. A spiro compound of formula a N-oxide, an addition salt, a quaternary amine or a stereochemically isomeric form thereof wherein P is a protective group and n, -A-B-, Z, R1 and R2 are claimed as in claim 1. provided that 6,11 -dihydro-1 '-(phenylmethyl)-5H-spiro[imidazo[ l,2-b)[3]benzazepine-ll ,4-piperidine] and pharmaceutically acceptable addition salts thereof are not included. 11. A compound as claimed in claim 10 wherein P is benzyl. 12. A process of preparing a compound as claimed in claim 1, wherein it comprises a) deprotecting an intermediate of formula (II), followed optionally by derivatizing either the piperidine moiety, or the imidazole moiety, or both the piperidine moiety and the imidazole moiety with -A-B-, Z, L, R1 and R2, and n defined as in claim 1 and P being a protective group; b) derivatizing an intermediate of formula (II) at the imidazole moiety, leading to the formation of an intermediate of formula (Il-a), followed by deprotecting the piperidine moiety, and followed optionally by derivatizing the piperidine moiety c) by cyclizing an intermediate of formula (III) in the presence of an appropriate acid, resulting in a compound of formula (I-a) with -A-B-, L, R1 and R2, and a defined as in claim 1; and, if desired, converting compounds of formula (I) and (I-a) into each other following art-known transformations, and further, if desired, converting the compounds of formula (I), into a therapeutically active non-toxic acid addition salt by treatment with an acid, or into a therapeutically active non-toxic base addition salt by treatment with a base, or conversely, converting the acid addition salt form into the free base by treatment with alkali, or converting the base addition salt into the free acid by treatment with acid; and, if desired, preparing stereochemically isomeric forms or N-oxide forms thereof. 13. A process of preparing a compound as claimed in claim 10, wherein it comprises a) cyclizing a compound of formula (XI) with an appropriate acid, leading to a compound of formula (II-k), followed optionally by derivatizing the imidazole moiety, leading to a compound of formula (II-a-I) with -A-B-, R', R2, n and P defined as in claim 13, and Zi being a bivalent radical of formula -(CH2)p-, wherein p is 1,2,3 or 4. b) by reacting a tricyclic moiety of formula (XIV) with a reagent of formula (XV) under an inert atmosphere in a reaction inert solvent in the presence of a suitable base, leading the a compound of formula (II-1), followed optionally by derivatizing the imidazole moiety leading to a compound of formula (II-a-2) with -A-B-, R1, R2, n and P defined as in claim 13, Ws being a suitable leaving group, e.g. a halo, and Z2 being a bivalent radical of formula or -(CH2) p-, or CH2-O-, wherein p is 1, 2, 3 or 4. Dated this 23rd day of April, 2001 (SHUKADEV KHURAIJAM) OF REMFRY & SAGAR ATTORNEY FOR THE APPLICANTS

Full Text

FORM 2
THE PATENTS ACT 1970
[39 OF 1970]
&
THE PATENTS RULES, 2003
COMPLETE SPECIFICATION
[See Section 10; rule 13]
"A SPIRO COMPOUND OF FORMULA (I)"
JANSSEN PHARMACEUTICA N.V., of Tumhoutseweg 30, Beerse, B-2340, Belgium
The following specification particularly describes the invention and the manner in which it is to be performed:
17-1-2007
12 APR 2006

The presentnvention is concernea with spiro compounds having antihistaminic activity. It further relates to their use as a medicine, their preparation as well as compositions comprising them.
WO 97/24356,.published on 10 July 1997, discloses 4-(imidazo-azepine) piperidine spiro derivatives as intermediates in the preparation of l-(l,2-disubstituted piperidinyl)-4-(imidazo-azepine) piperidine spiro derivatives having tachykinin antagonistic activity.
Surprisingly, the 4-(imidazo-azepine) piperidine spiro derivatives of the present invention show an interesting antihistaminic activity profile.
The present invention concerns compounds of formula (I) for use as a medicine, characterized in that the compounds of formula (I) are defined as

(D

their prodrugs, /V-oxides, addition salts, quaternary amines and stereochemically
isomeric forms wherein
R is hydrogen, C1-6alkyl, halo, formyl, carboxyl, C1-6alkyloxycarbonyl, C1-6alkyl-
carbonyl, N(R3R4)C(=0)-, N(R3R4)C(=0)N(R5)-. ethenyl substituted with carboxyl or
C1-6aIkyloxycarbonyl, or C1-6alkyl substituted with hydroxy, carboxyl, C1-6alkyloxy,
C1-6alkyloxycarbonyl, N(R3R4)C(=0)-, C1-6alkylC(=0)N(R5)-, C1-6alkylS(=0)2N(R5)-
or N(R3R4)C(=0)N(R5)-;
wherein each R3 and each R4 independently are hydrogen or C1-6alkyl;
R5 is hydrogen or hydroxy; R2 is hydrogen, C1-6alkyl, hydroxyC1-6aIkyI, C1-6alkyloxyC1-6aIkyl, N(R3R4)C(=0):, aryl or halo; n is 1 or 2;
-A-B- represents a bivalent radical of formula
-Y-CH=CH- (a-1);

-CH=CH-Y- (a-2); or
-CH=CH-CH=CH- (a-3);
wherein each hydrogen atom in the radicals (a-1) to (a-3) may independently be
replaced by R6 wherein R6 is selected from C1-6alkyl, halo, hydroxy,
C1-6alkyloxy, ethenyl substituted with carboxyl or C1-6alkyloxycarbonyl,
hydroxyC1-6alkyl, formyl, carboxyl and hydroxycarbonylC1-6alkyl;
each Y independently is a bivalent radical of formula -0-, -S- or -NR7-;
wherein R7 is hydrogen, C1-6alkyi or C1-6alkylcarbonyl;
Z is is a bivalent radical of formula
-(CH2)P- (b-1). -CH2-0- (b-4),
-CH=CH- (b-2), -CH2-C(=Q)- (b-5),or
-CH2-CHOH- (b-3). -CH2-C(=NOH)- (b-6),
provided that the bivalent radicals (b-3), (b-4), (b-5) and (b-6) are connected to the nitrogen of the imidazole ring via their -CH2- moiety; wherein p is 1, 2, 3 or 4;
L is hydrogen; C1-6alkyl; C2-6alkenyl; C1-6alkylcarbonyI; C1-6alkyloxycarbonyl;
C1-6alkyl substituted with one or more substituents each independently selected from
hydroxy, carboxyl, C1-6alkyloxy, C1-6a]kyloxycarbonyl, aryl, aryloxy, cyano or R8HN-
wherein R8 is hydrogen, C1-6alkyl, C1-6alkyloxycarbonyl, C1-6alkylcarbonyl; or
L represents a radical of formula
-Alk-Y-Hetl (c-1),
-Alk-NH-CO-Het2 (c-2) or
-Alk-Het3 (c-3) ; wherein
Alk represents C1-4alkanediyl ;
Y represents O, S or NH ;
Het1, Het2 and Het3 each represent furanyl, tetrahydrofuranyl, thienyl, oxazolyl,
thiazoiyl or imidazolyl each optionally substituted with one or two C1-4alkyl
substituents; pyrrolyl or pyrazolyl optionally substituted with formyl, hydroxyC1-4alkyl,
hydroxycarbonyl, C1-4alkyloxycarbonyl or with one or two C1-4alkyl substituents;
thiadiazolyl or oxadiazolyl optionally substituted with amino orC1-4alkyl; pyridinyl,
pyrimidinyl, pyrazinyl or pyridazinyl each optionally substituted with C1-4alkyl,
C1-4alkyloxy, amino, hydroxy or halo; and
Het3 may also represent 4,5-dihydro-5-oxo-lH-tetrazolyl substituted with C1-4alkyl,
2-oxo-3-oxazolidinyl, 2,3-dihydro-2-oxo-lH-benzimidazol-l-yl or a radical of formula

wherein

A-Z represents S-CH=CH, S-CH2-CH2, S-CH2-CH2-CH2. CH=CH-CH=CH, or
CH2-CH2-CH2-CH2;
aryl is phenyl or phenyl substituted with 1, 2 or 3 substituents each independently selected from halo, hydroxy, C1-4alkyl, polyhaloC1-4alkyl, cyano, aminocarbonyl, C1-4alkyloxy or polyhaloC1-4alkyloxy.
The compounds of formula (I) are deemed novel provided that 5,6-dihydrospiro[imidazo[l,2-b][3]benzazepine-l 1[1 lH],4'-piperidine] and pharmaceuucally acceptable addition salts thereof are not included and thus the present invention also relates to the compounds of formula (I) as defined hereinabove provided that 5,6-dihydrospiro[imidazo[l,2-b][3]benzazepine-l 1[1 lH],4'-piperidine] and pharmaceutically acceptable addition salts thereof are not included.
The term prodrug as used throughout this text means the pharmacologically acceptable
derivatives, e.g. esters and amides, such that the resulting biotransformation product of
the derivative is the active drug as defined in the compounds of formula (I). The
reference by Goodman and Gilman (The Pharmacological Basis of Therapeutics, 8 '
ed., McGraw-Hill, Int. Ed. 1992, "Biotransformation of Drugs", p. 13-15) describing
prodrugs generally, is hereby incorporated.
As used herein C1-4alkyl as a group or part of a group defines straight or branched chain saturated hydrocarbon radicals having from 1 to 4 carbon atoms such as methyl, ethyl, propyl, 1-methylethyl, butyl and the like; C1-4alkyl as a group or part of a group defines straight or branched chain saturated hydrocarbon radicals having from 1 to 6 carbon atoms such as the groups defined for C1-4alky! and pentyl, hexyl, 2-methylpropyl, 2-methylbutyl and the like; C2-6alkenyl as a group or part of a group defines straight and branched chain hydrocarbon radicals containing one double bond and having from 2 to 6 carbon atoms such as ethenyl, 2-propenyl, 2-butenyl, 2-pentenyl, 3-pentenyl, 3-methyl-2-butenyl, 3-hexenyl and the like.
As used herein before, the term (=0) forms a carbonyl moiety when attached to a carbon atom and a sulfonyl moiety when attached twice to a sulfur atom. The term (=NOH) forms a hydroxylimine moiety when attached to a carbon atom.

The term halo is generic to fluoro, chloro, bromo and iodo. As used in the foregoing and hereinafter, polyhaloC1-4alkyl as a group or part of a group is defined as mono- or polyhalosubstituted C1-4alkyl, in particular methyl with one or more fluoro atoms, for example, difluoromethyl or trifluoromethyl. In case more than one halogen atoms are attached to an alkyl group within the definition of polyhaloC1-4alkyl, they may be the same or different.

When any variable (e.g. R3, R4 etc.) occurs more than one time in any constituent, each definition is independent.
It will be appreciated that some of the compounds of formula (I), their prodrugs, N-oxides, addition salts, quaternary amines and stereochemically isomeric forms may contain one or more centers of chirality and exist as stereochemically isomeric forms.
The term "stereochemically isomeric forms" as used hereinbefore defines all the possible stereoisomeric forms which the compounds of formula (I), their prodrugs, N-oxides, addition salts, quaternary amines or physiologically functional derivatives may possess. Unless otherwise mentioned or indicated, the chemical designation of compounds denotes the mixture of all possible stereochemically isomeric forms, said mixtures containing all diastereomers and enantiomers of the basic molecular structure as well as each of the individual isomeric forms of formula (I), their prodrugs, N-oxides, addition salts or quaternary amines substantially free, i.e. associated with less than 10%, preferably less than 5%, in particular less than 2% and most preferably less than 1% of the other isomers. Stereochemically isomeric forms of the compounds of formula (I) are obviously intended to be embraced within the scope of this invention.
For therapeutic use, the addition salts of the compounds of.formula (I) are those wherein the counterion is pharmaceutically acceptable. However, salts of acids and bases which are not-pharmaceutically acceptable may also find use, for example, in the preparation or purification of a pharmaceutically acceptable compound. All salts, whether pharmaceutically acceptable or not are included within the ambit of the present invention.
The pharmaceutically acceptable acid and base addition salts as mentioned hereinabove are meant to comprise the therapeutically active non-toxic acid and base addition salt forms which the compounds of formula (I) are able to form. The pharmaceutically acceptable acid addition salts can conveniently be obtained by treating the base form with such appropriate acid. Appropriate acids comprise, for example, inorganic acids

such as hydrohalic acids, e.g. hydrochloric or hydrobromic acid, sulfuric, nitric, phosphoric and the like acids; or organic acids such as, for example, acetic, propanoic, hydroxyacetic, lactic, pyruvic, oxalic (i.e. ethanedioic), malonic, succinic (i.e. butane-dioic acid), maleic, fumaric, malic, tartaric, citric, methanesulfonic, ethanesulforiic, benzenesulfonic, p-toluenesulfonic, cyclamic, salicylic, p-aminosalicylic, pamoic and the like acids.

Conversely said salt forms can be converted by treatment with an appropriate base into the free base form.
The compounds of formula (I) containing an acidic proton may also be converted into their non-toxic metal or amine addition salt forms by treatment with appropriate organic and inorganic bases. Appropriate base salt forms comprise, for example, the ammonium salts, the alkali and earth alkaline metal salts, e.g. the lithium, sodium, potassium, magnesium, calcium salts and the like, salts with organic bases, e.g. the benzathine, N-methyl-D-glucamine, hydrabamine salts, and salts with amino acids such as, for example, arginine, lysine and the like.
The term addition salt as used hereinabove also comprises the solvates which the compounds of formula (I) as well as the salts thereof, are able to form. Such solvates are for example hydrates, alcoholates and the like.
Some of the compounds of formula (I) may also exist in their tautomeric form. Such forms although not explicitly indicated in the above formula are intended to be included within the scope of the present invention.
An interesting group of compounds consists of those compounds of formula (I) wherein L is hydrogen, C1-6alkyl, C1-6alkylcarbonyl, C1-6alkyloxycarbonyl or C1-6alkyl substituted with hydroxy, carboxyl, C1-6alkyloxy or C1-6alkyloxycarbonyl;
Another interesting group of compounds consists of those compounds of formula (I) wherein -A-B- is a bivalent radical of formula -CH=CH-CH=CH- (a-3).
Also interesting compounds are those compounds of formula (I) wherein -A-B- is a bivalent radical of formula -CH=CH-Y- (a-2).
Further interesting compounds are those compounds of formula (I) wherein Z is -(CH2)P- (b-1), -CH=CH- (b-2), or-CH2-0- (b-4).

Other interesting compounds are those compounds of formula (I) wherein L is hydrogen, C1-6alkyl, carboxyC1-6alkyl, C1-6alkyloxycarbonyl, or C1-6alkyloxycarbonylC1-6alkyl.
Again other interesting compounds are those compounds of formula (I) wherein L is hydroxyC1-6alkyl or C1-6alkyl substituted with aryl and C1-6alkyloxycarbonyl.
Also further interesting compounds are those compounds of formula (I) wherein R1 is hydroxyC1-6alkyl, formyl, C1-6alkyloxycarbonyl, N(R3R4)C(=0)-, halo or hydrogen.
Other interesting compounds are those compounds of formula (I) wherein R1 is C1-6alkyloxyC1-6alkyl.
Special compounds are those compounds of formula (I) wherein one or more of the
following restrictions apply:
-A-B- is a bivalent radical of formula -CH=CH-CH=CH- (a-3) wherein each hydrogen
may independently be replaced by C1-6alkyl, C1-6alkyloxy, halo or hydroxy;
Z is -(CH2)P- wherein p is 1,2,3 or 4, -CH2-C(=0)-, -CH2-CHOH-, -CH=CH-, -CH2-0-;
L is hydrogen, C1-6alkyl or C1-6alkyloxycarbonyl;
R1 is hydrogen, formyl, carboxyl, amide, halo, C1-6alkyloxycarbonyl, C1-6aiky!
substituted with hydroxy, C1-6alkyloxy, -NH-C(=O)-C1-6alkyl, -NH-C(=0)-NH2,
-NH-S02-C1-6alkyI;
R2 is hydroxyC1-6 alkyl, C1-6alkyloxyC1-6alkyl, halo, amide.
The most preferred compounds are:
5,6-dihydrospiro[llH-imida2o[2,l-b][3]benzazepine-ll,4'-piperidine]-3-carboxamide
dihydrochloride (comp. 17);
1 '-butyI-5,6-dihydrospiro[imidazo[2,l-b] [3] benzazepine-l1-[1 lH],4'-piperidmej
(comp. 3);
6,11 -dihydro- r-methylspiro[5H-imidazo[2,1 -b][3]benzazepine-11,4'-piperidine)
cyc!ohexylsulfamate(l:2) (comp. 1);
6,Il-dihydrospiro[5-imidazo[2,l-b][3]benzazepine-ll,4'-piperidine]-3-methanolJ
(E)-2-butenedioate (2:1) (comp. 18a);
3-chloro-6,ll-dihydrospiro[5H-imidazo[2,l-b][3]benzazepine-ll,4'-piperidine]
(E)-2-butenedioate (1:1) (comp. 20);
6,ll-dihydro-3-(methoxymethyl)spiro[5H-imidazo[2,l-b][3]benzazepine-ll,4'-
piperidine]. (E)-2-butenedioate (1:1) (comp. 58);

6,ll-dihydro-r-(2-hydroxyethyI)spiro[5H-imidazo[2,l-b][3]benzazepine-ll,4'-
piperidine]-3-carboxamide (comp. 62);
6,11 -di hydro-1 '-methylspiro[5H-imidazo[2, l-b][3]benzazepine-11,4'-piperidine]-3-
carboxamide monohydrate (comp. 80);
ethyl 3-(aminocarbonyl)-6,ll-dihydro-a-phenylspiro[5H-imidazo[2,I-b][3]-
benzazepine-1 l,4'-piperidine]-l'-propanoate monohydrochloride (comp. 64);
3-(aminocarbonyl)-6,ll-dihydrospiro[5H-imidazo[2,l-b][3]-benzazepine-ll,4'-
piperidine]-r-carboxylate (comp. 79);
spiro[10H-irnidazo[l,2-a]thieno[3,2-d]azepine-10,4'-piperidine] (comp. 56a);
6,11 -dihydrospiro[5H-imidazo[2,I-b][3]benzazepine-l l,4'-piperidine]-2,3-
dicarboxamide dihydrochloride monohydrate (comp. 53);
a prodrug, a N-oxide, an addition salt, a quaternary amine or a stereochemically
isomeric form thereof.
The present invention also concerns novel compounds of formula

(n-a)

their N-oxides, addition salts, quaternary amines and stereochemically isomeric forms, wherein
R1 is hydrogen, C1-6alkyl, halo, formyl, carboxyl, C1-6alkyloxycarbonyl, C1-6alkyl-
carbonyl, N(R3R4)C(=0)-, N(R3R4)C(=0)N(R5)-, ethenyl substituted with carboxyl or
C1-6alkyloxycarbonyl, or C1-6alkyl substituted with hydroxy, carboxyl, amino,
C1-6alkyloxy, C1-6alkyloxycarbonyl, N(R3R4)C(=0)-, C1-6alkylC(=0)N(Rs)-,
C1-6alkyiS(=0)2N(R5)- or N(R3R4)C(=0)N(R5)s
wherein each R3 and each R4 independently are hydrogen or C1-4alkyl;
R5 is hydrogen or hydroxy; __
-A-B-, Z, R2, and n are as defined for compounds of formula (I); and
P represents a protective group for example, benzyl, or those protective groups
mentioned in Chapter 7 of "Protective Groups in Organic Synthesis" by T. Greene and
P. Wuyts (John Wiley & Sons, Inc. 1991),
provided that 6,11-dihydro r-(phenylmethyl)-5H-spiro[imidazo[l,2-b][3]benzazepine-
11,4'-piperidine] (E)-2-butenedioate(l :2) is not included .

The compounds of formula (II-a) are useful for the preparation of the compounds of formula (I).
Interesting compounds are those compounds of formula (Il-a) wherein P is benzyl.
Also interesting compounds are those compounds of formula (H-a) wherein R1 is hydrogen, halo, formyl, N(R3R4)C(=0)-, or C1-6allkyl substituted with hydroxy, amino, C1-6alkylC(=0)N(R5)-, C1-6alkylS(=0)2N(R5)- or N(R3R4)C(=0)N(Rs)-
Further interesting compounds are those compounds of formula (TI-a) wherein -A-B- is a bivalent radical of formula (a-3) wherein each hydrogen atom may independently be replaced by C1-6alky!, halo, hydroxy, or C1-6alkyloxy.
Again further interesting compounds are those compounds of formula (Il-a) wherein Z is a bivalent radical of formula (b-1) and n is 1.
Compounds of formula (I), can be prepared by deprotecting an intermediate of formula (II), wherein P is a protecting group, for example, benzyl, or those protective groups mentioned in Chapter 7 of "Protective Groups in Organic Synthesis" by T. Greene and P. Woyts (John Wiley & Sons, Inc. 1991). Said deprotcction reaction can be performed by, for example, catalytic hydrogenation in the presence of hydrogen and an appropriate catalyst in a reaction inert solvent. A suitable catalyst in the above reaction is, for example, platinum-on-charcoal, palladium-on-charcoal, and the like. An appropriate reaction-inert solvent for said reaction is, for example, an alcohol, e.g. methanol, ethanol, 2-propanol and the like, an ester, e.g. ethylacetate and the like, an acid, e.g. acetic acid and the like. The thus obtained deprotected compounds can optionally further be derivatized either by replacing the hydrogen on the piperidine nitrogen by a moiety belonging to L, or by introducing on the imidazole moiety a R1 group or a R2 group or a R and R group, or by derivatizing both the piperidine moiety and the imidazole moiety.
An intermediate of formula II can also first be derivatized at the imidazole moiety by introducing a Rl group or a R2 group or a R1 and R2 group, resulting in an intermediate of formula (II-a), and then be deprotected, followed optionally by a derivation at the piperidine nitrogen.

Alternatively, compounds of formula (I), wherein Z is a bivalent radical of formula -CH2-C(=0)- (b-5), said compounds being represented by formula (I-a), can be prepared by cyclizing an intermediate of formula (HO in the presence of an acid, e.g. trifluoromethanesulfonic acid and the like.

The compounds of formula (I) may further be prepared by converting compounds of formula (I) into each other according to art-known group transformation reactions.
The compounds of formula (I) may be converted to the corresponding N-oxide forms following art-known procedures for converting a trivalent nitrogen into its N-oxide form. Said N-oxidation reaction may generally be carried out by reacting the starting material of formula (I) with an appropriate organic or inorganic peroxide. Appropriate inorganic peroxides comprise, for example, hydrogen peroxide, alkali metal or earth alkaline metal peroxides, e.g. sodium peroxide, potassium peroxide; appropriate organic peroxides may comprise peroxy acids such as, for example, benzenecarboper-oxoic acid or halo substituted benzenecarboperoxoic acid, e.g. 3-chlorobenzenecarbo-peroxoic acid, peroxoalkanoic acids, e.g. peroxoacetic acid, alkylhydroperoxides, e.g.

t.butyl hydro-peroxide. Suitable solvents are, for example, water, lower alcohols, e.g. ethanol and the like, hydrocarbons, e.g. toluene, ketones, e.g. 2-butanone, halogenated hydrocarbons, e.g. dichloromethane, and mixtures of such solvents.
The compounds of formula (I) wherein L is other than hydrogen, said L being represented by La and said compounds being represented by formula (I-b) can be prepared by reacting the compounds of formula (I) wherein L is hydrogen, said compounds being represented by formula (I-c), with a reagent of formula La-Wt (TV),wherein W1) is a suitable leaving group, such as a halo atom, e.g.chloro, or mesylate, tosylate, trifluoromethanesulfonate.

Said reaction can conveniently be conducted in a reaction-inert solvent such as, for example, an aromatic hydrocarbon, an alkanol, a ketone, an ether, a dipolar aprotic solvent, a halogenated hydrocarbon, or a mixture of such solvents. The addition of an appropriate base such as, for example, an alkali or an earth alkaline metal carbonate, hydrogen carbonate, alkoxide, hydride, amide, hydroxide or oxide, or an organic base, such as, for example, an amine, may be utilized to pick up the acid which is liberated during the course of the reaction. In some instances the addition of an iodide salt, preferably an alkali metal iodide, is appropriate. Somewhat elevated temperatures and stirring may enhance the rate of the reaction.
The compounds of formula (I-b), wherein La is optionally substituted C1-6alkyl, said L, being represented by Lai and said compounds by formula (I-b-1), can be converted into the compounds of formula (I-c) by dealkylating and subsequently carbonylating the compounds of formula (I-b-1) with a reagent of formula (V), wherein W2 represents a suitable leaving group, such as a halo atom, e.g. chloro, and L,2 represents C1-6alkyloxycarbonyl, resulting in compounds of formula (I-b-2) and subsequently hydrolyzing the thus obtained compounds of formula (I-b-2).

The reaction with reagent (V) is conveniently conducted by stirring and heating the starting material with the reagent in an appropriate solvent and in the presence of a suitable base. Appropriate solvents arc, for example, aromatic hydro-carbons, e.g. methylbenzene, dimethylbenzene, chlorobenzene; ethers, e.g. 1,2-dimethoxyethane; methylenechloride and the like solvents. Suitable bases are, for example, alkali or earth alkaline metal carbonates, hydrogen carbonates, hydroxides, or organic bases such as, N,N-diethyIethanamine, N-(l-methylethyI)-2-propanamine, and the like. The compounds of formula (I-b-2) are hydrolyzed in acidic or basic media following conventional methods. For example, concentrated acids such as hydrobromic, hydrochloric acid or sulfuric acid can be used, or alternatively bases such as alkali metal or earth alkaline metal hydroxides in water, an alkanol or a mixture of water-alkanol may be used. Suitable alkanols are methanol, ethanol, 2-propanol and the like. In order to enhance the rate of the reaction it is advantageous to heat the reaction mixture, in particular up to the reflux temperature.
The compounds of formula (I-b-2) can also be prepared by reacting compounds of formula (I-c) with a reagent of formula (V) in the presence of a suitable base, e.g. N,N-diethylethanamine, in a reaction inert solvent, e.g. methylenechloride, or by reacting compounds of formula (I-c) with a reagent of formula (VI), e.g. t-butyloxyanhydride, in a suitable solvent, such as, e.g. methylenechloride.

The compounds of formula (I-b) wherein R1 or Rl and R represent hydroxymethyl, said compounds being represented by formula (I-b-3) and (I-b-4) can be prepared by

reacting the compounds of formula (I) wherein L is La and Rl and R2 are hydrogen, said compounds being represented by formula (I-b-5), with formaldehyde, optionally in the presence of an appropriate carboxylic acid - carboxylate mixture such as, for example, acetic acid - sodium acetate and the like. In order to enhance the rate of the reaction, it is advantageous to heat the reaction mixture up to the reflux temperature.
The thus obtained compounds of formula (I-b-3) and (I-b-4) can be further oxidized to the corresponding aldehyde, represented by formula (I-b-6) and (I-b-7) or the corresponding carboxylic acid, represented by formula (I-b-8) and (I-b-9), by reaction with a suitable reagent such as, for example, manganese(TV)oxide, respectively, silver nitrate.
The compounds of formula (I-b-8) and (I-b-9) can further be converted in the corresponding amide, said compounds being represented by formula (I-b-10) and (I-b-11), by reaction with a suitable carbodiimide, e.g. l-(3-dimethylaminopropyl)-3-ethylcarbodiimide, in the presence of ammonia and a suitable catalyst, e.g. N.N-dimethylarninopyridine, in a reaction inert solvent, e.g. methylenechloride.

The compounds of formula (I) wherein L is La, and R1 or R1 and R2 are halo, said compounds being represented by formula (I-b-12) and (I-b-13), can be prepared by

halogenating a compound of formula (I-b-5) with an appropriate halogenating reagent in a reaction-inert solvent.

A suitable halogenating reagent in the above reaction is, for example, an Af-halogenated amide, e.g. N,N-bromosuccinimide. A suitable reaction-inert solvent for said halogena-tion reaction is, for example, N,N-dimethylformamide, N,N-dimethylacetamide, methylenechloride and the like. Another suitable halogenating reagent is, for example, tetrabutylammoniumtribromide in the presence of a suitable base, e.g. sodium carbo¬nate, in a suitable solvent, e.g. 3-methyl-2-butanone or dichloromethane/water mixture.
Compounds of formula (I-b-12) can be converted in a compound of formula (I-b-10) by reaction with CuCN in the presence of a suitable solvent, e.g. N,N-dimemylfonnamide/ water mixture.

The compounds of formula (I-b) wherein R1 is C1-6aIkyloxycarbonylethenyl, said compounds being represented by formula (I-b-14), can be prepared by reacting a compound of formula (I-b-6) with a reagent of formula (VH) in the presence of a base e.g. piperidine, pyridine, and the like.
The compounds of formula (I-b-14) can further be hydrolyzed into a compound of formula (I-b) wherein R1 is carboxyethenyl, in the presence of an acid or a base in case La is C1-6alkyl, or in the presence of a base, in case La is C1-6alkyloxycarbonyl.
Compounds of formula (I-b) wherein 1, is substituted ethyl, said La being represented

by La3-CH2-CH2-, and said compounds by formula (I-b-15) can be prepared by reacting a compound of formula (I-c) with a reagent of formula (VE) in the presence of a suitable base, e.g. sodium bicarbonate or triethylamine, in a suitable reaction inert solvent, e.g. N,N-dimethylformamide or a suitable alkanol, e.g. methanol.

Compounds of formula (I-c) may also be converted into compounds of formua(I-b-15) wherein La3 is hydroxy, said compounds being represented by formula (I-b-15-1) by reaction with ethylene oxide in the presence of a suitable base, e.g. triethylamine, in a suitable reaction inert solvent, such as an alkanol, e.g: methanol.

Compounds of formula (I) wherein Z is a bivalent radical of formula -CH2-CHOH-(b-3), said compounds being represented by formula (I-d), can be prepared by reducing a compound of formula (I-a) in the presence of a reducing reagent, e.g. sodium borohydride, in a reaction-inert solvent, e.g. methanol and the like.

Compounds of formula (I) wherein Z is a bivalent radical of formula -CH2-C(=N-OH)-(b-6), said compounds being represented by the formula (I-e), can be prepared by

reacting a compound of formula (I-a) with hydroxylamine or a salt thereof, e.g. the hydrochloride salt, in a reaction inert solvent, e.g. pyridine and the like.

Compounds of formula (I) wherein Z is a bivalent radical of the formula -CH=CH-(b-2), said compounds being represented by formula (I-f). can be prepared by reacting a compound of formula (I-d) in the presence of an acid, e.g. methanesulfonic acid and the like.

Compounds of formula (I-b) wherein La is C1-6alkyl substituted with C1-6alkyloxy-carbonyl or C1-6alkyloxycarbonylNH-, can be converted into compounds of formula (I-b) wherein La is C1-6alkyl or aminoC1-6aIkyl by the hydrolysis reaction described above for the preparation of compounds of formula (I-c).
In the foregoing and the following preparations, the reaction mixture is worked up following art-known methods and the reaction product is isolated and, if necessary, further purified.
As described hereinabove, the intermediates of formula (II) can be derivatized at the
imidazole moiety, said compounds being represented by formula (Il-a), before being
deprotected.
Introducing R1 or R1 and R2 wherein R1 and R2 represent hydroxymethyl, formyl.
carboxyl or amide, in a compound of formula (II) can be performed as described
herinabove for the preparation of a compound of formula (I-b-3), (I-b-4), (I-b-6),
(I-b-7). (I-b-8). (I-b-9). (I-b-10), (I-b-11).

Intermediates of formula (II-a), wherein Rl is aminomethyl and R is hydrogen, said intermediates being represented by formula (Il-b), can be prepared by reacting an intennediate of formula (II-c) with hydrogen and a mixture of methanol/ammonia in the presence of a suitable catalyst, for example rhodium on aluminium, in the presence of a catalyst poison, for example a thiophene solution.

Intermediates of formula (II-a), wherein R1 is -CH2NHC(=0)NH2 and R2 is hydrogen, said intermediates being represented by formula (H-d) can be prepared by reacting an intermediate of formula (II-b) with potassium isocyanate in an appropriate acid, such as hydrochloric acid.

Intermediates of formula (II-b) can also be converted in an intermediate of formula (Il-a), wherein R1 is -CH2NHC(=0)C1-6alkyl and R2 is hydrogen, said intermediate being represented by formula (II-e), by reaction with a reagent of formula (IX), wherein W3 represents a suitable leaving group, such as a halo atom, for example chloro, in the presence of a suitable base, e.g. N,N-diethylethanamine, in a reaction inert solvent, such as, for example methylenechloride.

Intermediates of formula (II-b) can further be converted into an intermediate of formula (Il-a), wherein R1 is -CH2NHS(=O)2=C1-6alkyl and R2 is hydrogen, said intermediate being represented by formula (Of), by reaction with a reagent of formula (X) wherein W4 represents a suitable leaving group, such as a halo atom, e.g. chloro, in the presence of a suitable base, for example N,Ndiethylethanamine, in a reaction inert solvent, such as methylenechloride.

Intermediates of formula (II) can also be halogenated according to the procedure described for the preparation of the compounds of formula (I-b-12) and (I-b-13), resulting in an intermediate of formula (II-g) and (II-h).

Intermediates of formula (Il-g) and (H-h) can be converted in an intennediate of formula (II-i) and (II-j) by reaction under an atmosphere of ammonia and carbonmonoxide at elevated temperatures in the presence of a suitable catalyst, e.g.

acetic acid, palladium salt, and a suitable ligand, e.g. l.3-bis(diphenylphosphino)-propane, in a reaction inert solvent, e.g. tetrahydrofuran.
In the following paragraphs, there are described several methods of preparing the starting materials in the foregoing preparations.

Intermediates of formula (II), wherein Z is a bivalent radical of formula -(CH2)P- (b-1), said Z being represented by Z1 and said intermediates being represented by formula (Il-k), can be prepared by cyclizing an alcohol of formula (XI). The intermediates of formula (Il-k) may optionally be derivatized at the imidazole moiety resulting in an intermediate of formula (II-a-1) according to the procedures described for preparing a compound of formula (I-b-3), (I-b-4), (I-b-6) to (I-b-11) and an intermediate of formula (Il-b)to(II-j).
Said reaction is conveniently performed in a reaction inert solvent such as, for example tetrahydrofuran, in the presence of a suitable base such as lithium diisopropylamide and butyl lithium.

Intermediates of formula (II), wherein Z represents a bivalent radical of formula -(CH2)p (b-1), or -CH2-O- (b-4), said Z being represented by Z2, and said intermediates being represented by fonnula (II-l), can also be prepared by reacting a tricyclic moiety of formula (XTV) with a reagent of formula (XV), wherein Ws represents a suitable leaving group, e.g. a halo atom, such as chloro, under an inert atmosphere in a reaction inert solvent, such as tetrahydrofuran, in the presence of a suitable base such as, for example, lithium diisopropylamide and butyl lithium. The intermediates of formula (II-1) may optionally be derivatized at the imidazole moiety resulting in an intermediate of formula (II-a-2) according to the procedures described for preparing a compound of formula (I-b-3), (I-b-4), (I-b-6) to (I-b-11) and an intermediate of fonnula (H-b) to (II-j).

Intermediates of formula (XTV) can be prepared by cyclizing an intermediate of formula (XVI), according to the procedure descnbed for the preparation of intermediates of formula (II-k).

Said reduction can be conducted in a suitable solvent, such as, for example methanol, in the presence of a suitable reducing agent, such as sodium borohydride.
Intermediates of formula (XVI) can be prepared by reduction from the corresponding aldehydes, said intermediates being represented by formula (XVII).

Intermediates of formula (XVI) can also be prepared by reacting an intermediate of formula (XVIII) with formol 38% solution under pressure.

Alternatively, the tricyclic moieties of formula (XIV), wherein Z represents a bivalent radical of formula -CH2-, said Z being represented by Z3, and said tricylclic moieties being represented by formula (XlV-a), may also be prepared by first cyclizing an intermediate of formula (XVH) wherein Z2 represents Z3, said intermediate being represented by formula (XVII-a), by treating said intermediate with an appropriate acid, e.g. trifluoroacetic acid, leading to an intermediate of formula (XIX), followed by reduction in the presence of a suitable reducing agent.

Said reduction reaction can be performed in the presence of hydrogen and an appropriate catalyst in a reaction inert solvent. A suitable catalyst in the above reaction is, for example, platinum-on-charcoal, palladium-on-charcoal, and the like. An appropriate reaction inert solvent for said reaction is, for example, an alcohol, e.g. methanol, ethanol, 2-propanol and the like, an ester, e.g. ethylacetate and the like, an acid, e.g. acetic acid and the like.
Intermediates of formula (III) can be prepared by reacting an intermediate of formula (XX) with a reagent of formula (XXI), wherein W6 represents a suitable leaving group, such as a halo atom, e.g. chloro, in the presence of a suitable base, e.g. sodium hydride, in a reaction inert solvent, e.g. N,N-dimethylformarnide and the like.

Intermediates of formula (XX), wherein R1 and R2 are hydrogen, said intermediates being represented by formula (XX-a), can be prepared by debenzylating an intermediate of formula (XXII).

Said debenzylation reaction can be performed by, for example, catalytic hydrogenation in the presence of hydrogen and an appropriate catalyst in a reaction inert solvent. A suitable catalyst in the above reaction is, for example, platinum-on-charcoal, palladium-on-charcoal, and the like. An appropriate reaction inert solvent for said reaction is, for example, an alcohol, e.g. methanol, ethanol, 2-propanol and the like, an ester, e.g. ethylacetate and the like, an acid, e.g. acetic acid and the like.
Intermediates of formula (XXII) can be prepared by imidazole formation out of an
intermediate of formula (XXHI) in an acid, such as hydrochloric acid.

(XXII)

(XXIII)
Intermediates of formula (XXHI) can be prepared by reacting an intermediate of formula (XXTV) with 2,2-dimethoxyethylamine in a reaction inert solvent, such as, for example N.N-dimethylformamide and the like.

Intermediates of formula (XXIV) can be prepared by reacting an intermediate of

formula (XXV) with thionylchloride.
Intermediates of formula (XXV) can be prepared by substituting an intermediate of formula (XXVI) with benzylamine in the presence of a suitable base, e.g. //^-diethyl-ethanamine, in a reaction inert solvent, e.g. methylenechloride and the like.

(XXVI)
Pure stereochemically isomeric forms of the compounds of formula (I) may be obtained by the application of art-known procedures. Diastereomers may be separated by physical
methods such as selective crystallization and chromatographic techniques, e.g., counter-current distribution, liquid chromatography and the like.
The compounds of formula (I) as prepared in the hereinabove described processes are generally racemic mixtures of enantiomers which can be separated from one another following art-known resolution procedures. The racemic compounds of formula (I) which are sufficiently basic or acidic may be converted into the corresponding diastereomeric salt forms by reaction with a suitable chiral acid, respectively chiral base. Said diastereomeric salt forms are subsequendy separated, for example, by selective or fractional crystallization and the enantiomers are liberated therefrom by alkali or acid. An alternative manner of separating the enantiomeric forms of the compounds of formula (I) involves liquid chromatography, in particular liquid chromatography using a chiral stationary phase. Said pure stereochemically isomeric forms may also be derived from the corresponding pure stereochemically isomeric forms of the appropriate starring materials, provided that the reaction occurs stereospectfically. Preferably if a specific stereoisomer is desired, said compound will be synthesized by stereospecific methods of preparation. These methods will advantageously employ enantiomerically pure starting materials.

A number of intermediates and starting materials are commercially available or are known compounds which may be prepared according to conventional reaction procedures generally known in the art. For example, the preparation of l-(l-phenyl-ethyl)-l//-imidazole is described in WO 92/22551.
The compounds of formula (I), their prodrugs, N-oxides, addition salts, quaternary amines and stereochemically isomeric forms possess useful pharmacological properties. In particular they are active antihistaminic agents, which activity can be demonstrated by for instance the 'Histamine - induced Lethality in Guinea Pigs' test (Arch. Int. Pharmacodyn. Ther., 251,39-51,1981), *Protection of Rats from Compound 48/80 -induced Lethality" test (Arch. Int. Pharmacodyn. Ther., 234,164-176,1978), and 'Ascaris Allergy in Dogs' test (Arch. Int. Pharmacodyn. Ther., 251, 39-51,1981 and Drug Dev. Res., 8, 95-102, 1986).
Some of the intermediates of formula (II-a) also have interesting pharmacological properties.
The compounds of the present invention have a selective binding affinity for the H1 receptor, more in particular, they have a very low affinity for the 5HT2A serotonin receptor and the 5HT2C serotonin receptor. This dissociation between the H1 receptor binding affinity and the 5HT2c and 5HT2A receptor binding affinity renders it unlikely for the present compounds to cause appetite stimulation and inappropriate weight gain reported for some other H1-antagonists.
An important asset of the present compounds is their lack of sedating properties at therapeutic dose levels, a troublesome side effect associated with many antihistaminic and antiallergic compounds. The non-sedating properties of the present compounds can be demonstrated, for example, by the results obtained in studying the sleep -wakefulness cycle of the rat (Psychopharmacology, 97, 436-442, (1989)) and the state of vigilance using EEG power spectra in wake rats (Sleep Research 24A, 118, (1995)).
The compounds of the present invention are also characterized by the absence of relevant cardio-hemodynamic and electrophysiological effects such as QTc prolongation.
An additional advantage of some of the present compounds is that they exhibit little or no metabolic transformations in animal and human liver, thus indicating a low risk for metabolic interactions.

Another interesting feature of the present compounds relates to their fast onset ot action and the favorable duration of their action. The latter characteristic may enable the administration of the compound once daily.
The present compounds have a favorable physicochemical profile, particularly in terms of solubility and chemical stability.
In view of their physicochemical and pharmacological properties, the compounds of formula (I), their prodrugs, N-oxides, addition salts, quaternary amines and stereochemically isomeric forms thereof are very useful in the treatment of a broad range of allergic diseases such as, for example, allergic rhinitis, allergic conjunctivitis, chronic urticaria, pruritis, allergic asthma and the like.
Also in view of their useful physicochemical and pharmacological properties the subject compounds may be formulated into various pharmaceutical forms for administration purposes. To prepare the antiallergic compositions of this invention, an effective amount of the particular compound, in base or acid addition salt form, as the active ingredient is combined in intimate admixture with a pharmaceutically acceptable carrier, which carrier may take a wide variety of forms depending on the form of preparation desired for administration. These pharmaceutical compositions are, desirably as unitary dosage forms, administered orally, parenterally, percutaneously, rectally or topically for systemic action, or for topical action. In case of oral liquid pharmaceutical preparations, comprising solutions, suspensions, syrups, elixirs and emulsions, any of the usual pharmaceutical media, such as, for example, water, glycols, oils, alcohols and the like, may be employed, whereas in case of oral solid pharmaceutical preparations, comprising powders, pills, capsules and tablets, excipients such as starches, sugars, kaolin, lubricants, binders, disintegrating agents and the like may be employed. Because of their ease in administration, tablets and capsules represent the most advantageous oral unit dosage forms, in which case solid pharmaceutical carriers are obviously employed. In case of injectable pharmaceutical compositions, the carrier will usually comprise sterile water, at least in large part, though other ingredients, such as semipolair solvents, may be included, for example, to aid solubility. Examples of carriers for injectable solutions comprise saline solution, glucose solution or a mixture of saline and glucose solution. Injectable solutions containing compounds of the aforementioned formulas may also be formulated in an oil for prolonged action. Appropriate oils for this purpose are, for example, peanut oil, sesame oil, cottonseed oil, com oil, soy bean oil, synthetic glycerol esters of long chain

fatty acids and mixtures of these and other oils. For the preparation of injectable suspensions, appropriate liquid carriers, suspending agents and the like may be employed. In the compositions suitable for percutaneous administration, the carrier optionally comprises a penetration enhancing agent and/or a suitable wettable agent, oprionally combined with suitable additives of any nature in minor proportions, which additives do not cause any significant deleterious effects on the skin. Said additives may facilitate the administration to the skin and/or may be helpful for preparing the desired compositions. These compositions may be administered in various ways, e.g., as a transdermal patch, as a spot-on, as an ointment or as a gel. In case of pharmaceutical compositions for rectal administration, any of the usual excipients may be employed, comprising fat based and water soluble excipients, optionally combined with suitable additives, such as suspending or wetting agents. As appropriate compositions for topical application there may be cited all compositions usually employed for topically administering drugs e.g. creams, gellies, dressings, lotions, shampoos, tinctures, pastes, ointments, salves, ovules, powders, inhalations, nose sprays, eye drops and the like. Semisolid compositions such as salves, creams, gellies, ointments and the like will conveniently be used, but application of said compositions may be, for example, also by aerosol, e.g. with a propellent such as nitrogen, carbon dioxide, a freon, or without a propellent such as a pump spray or drops.
It is especially advantageous to formulate the aforementioned pharmaceutical compositions in unit dosage form for ease of administration and uniformity of dosage. Unit dosage form as used in the specification and claims herein refers to physically discrete units suitable as unitary dosages, each unit containing a predetermined quantity of active ingredient calculated to produce the desired therapeutic effect in association with the required phannaceutical carrier. Examples of such unit dosage forms are tablets (including scored or coated tablets), capsules, pills, powder packets, suppositories, ovules, wafers, injectable solutions or suspensions, teaspoonfuls, tablespoonfuls and the like, and segregated multiples thereof.
The present invention also relates to a method of treating warm-blooded animals suffering from allergic diseases by administering to said warm-blooded animals an effective anti-allergic amount of a compound of formula (I), a prodrug, //-oxide, addition salt, quaternary amine or stereochemically isomeric form thereof.
The present invention further relates to the compounds of formula (I), their prodrugs, N-oxides, addition salts, quaternary amines and stereochemically isomeric forms

thereof for use as a medicine, and hence, the use of the present compounds for the manufacture of a medicament for treating warm-blooded animals suffering from allergic diseases is also part of the present invention.
In general it is contemplated that an effective antiallergic amount would be from about 0.001 mg/kg to about 2 mg/kg body weight, and more preferably from about 0.01 mg/kg to about 0.5 mg/kg body weight. In any event, an effective antiallergic amount may depend on the type and severity of the affliction to be treated and the evaluation of the physician prescribing the treatment with the subject drugs.
The following examples are intended to illustrate the scope of the present invention.
Experimental part
Hereinafter, THF means tetrahydrofuran, DDPE means diisopropyl ether, DMF means
N,N-dimethylformamide, DIPA means diisopropyl amine
A. Preparation of .intermediate compounds
Example Al
a) A mixture of DIPA (1.4 mol) in THF (3000ml) was stirred at -70°C under N2 flow.
Butyllithium 2.5 M/hexane (1.3 mol) was added portionwise at a temperature below -
40°C. The mixture was stirred at -70°C for 15 min. l-phenylethyl-lH-imidazole
(1 mol) dissolved in THF was added dropwise at a temperature below -55°C. The mixture was stirred at -70°C for 1 hour. l-(phenylmethyl)-4-piperidinone (1.2 mol) dissolved in THF was added dropwise at a temperature below -55°C. The mixture was stirred at -70°C for 1 hour, then brought to room temperature, stirred at room temperature overnight and decomposed with H2O. The organic solvent was evaporated. The aqueous concentrate was extracted with CH2CI2. The organic layer was separated, dried (MgSO4), filtered and the solvent was evaporated. The residue was crystallized from DIPE (1100ml). The precipitate was Filtered off, washed with DEPE and dried, yielding 271g of 4-[l-(2-phenylethyl)-lH-imidazol-2-yl]-l-(phenylmethyl)-4-piperidinol (75%) (interm. 1).
b) A mixture of intermediate (1) (0.75 mol) in trifluoromethanesulfonic acid (1500ml)
was stirred at 65°C for 120 hours, then cooled, poured out on ice, alkalized with NaOH
50% and extracted with CH2CI2. The organic layer was separated, dried (MgS04).
filtered and the solvent was evaporated. The residue was crystallized from
DIPE/CH3CN (99/1) (1200ml). The precipitate was filtered off and dried, yielding
169.6g of 5,6-dihydro-r-(phenylmethyl)spiro[l lH-irnidazo[2,l-b][3]benzazepine-
1 l,4'-piperidine] (66%) (interm. 2).

Example A2
l-(phenylmethyl)-4-[l-(phenylmethyl)1H-imidazol-2-yl]-4-piperidinol (0.124 mol) and AICI3 (0.31 mol) were stirred in a melt at 120°C for lh. The mixture was cooled, AICI3 (0.31 mol) was added and the mixture was stirred at 120°C for lh. The mixture was poured into ice, alkalized with NaOH 50% and extracted with CH2Cl2 The organic layer was dried (MgS04), filtered off and evaporated. The residue was purified by HPLC (eluent: CH2C12/(CH30H/NH3) 99/1). The pure fractions were collected and evaporated. The residue was converted into the hydrochloric acid salt (1:2) in (C2H5)2O, yielding 0.91 g of r-(phenylmethyl)spiro[imidazo[l,2-b]isoquinoline-10[5H],4'-piperidine] dihydrochloride.dihydrate (2%) (interm. 3; mp. 161.2 °C).
Example A3
a) A mixture of intermediate (2) (0.09 mol) in CH2C12 (lOOOml) was cooled to 0°C. l-bromo-2,5-pyrrolidinedione (0.09 mol) was added portion wise over a 1-hour period. The organic layer was separated, washed with H2O, dried, filtered and the solvent was evaporated. The residue was purified by column chromatography over silica gel (eluent: CH2C12/CH30H 97.5/2.5 to 95/5). A pure fraction was collected and the solvent was evaporated. The residue was dissolved in ethanol and converted into the (E)-2-butenedioic acid salt (1:1). The precipitate was filtered off and dried, yielding 17.3g of 3-bromo-5,6-dihydro-1 '-(phenylmethyl)spiro[ 1 lH-imidazo[2, l-b](3]-benzazepine-ll,4'-piperidine (E)-2-butenedioate(I:l) (36%) (interm. 4). Part of this fraction (I6.5g) was taken up in H20, K2CO3 and CH2CI2. The mixture was separated into its layers. The aqueous layer was extracted with CH2CI2. The combined organic layer was dried (MgS04), filtered and the solvent was evaporated, yielding 12.9g of 3-bromo-5,6-dihydro-r-(phenylmethyl)spiro[llH-imidazo[2,l-b][3]benzazepine-l 1,4-piperidine (interm. 4a).
b) A mixture of intermediate (4a) (0.21 mol), l.3-propanediylbis[diphenylphosphine] (2.5 g) and acetic acid, palladium(2+) salt (0.68 g) in THF (567 ml) was stirred in an autoclave at 150°C for 16 hours under NH3 (10 atm) and CO (30 atm). The mixture was filtered and the filtrate was evaporated. This residue was purified by column chromatography over silica gel (eluent: CH2CI2/C2H5OH 100/0 over 46 min to 70/30). The pure fractions were collected and the solvent was evaporated, yielding 36 g of 5,6-dihydro-l'-(phenylmethyl)spiro[ 1 lH-imidazo[2,l -b][3)benzazepine-l 1,4'-piperidine]-3-carboxamide (44%) (interm. 5).
Example A4
a) A mixture of intermediate (2) (0.16 mol) and sodium acetate (45g) in formol 38%
(300ml) and acetic acid (30ml) was stirred and refluxed for 6 hours, then cooled.

poured out on ice and alkalized with a NaOH solution. The precipitate was filtered off and punftcd by column chromatography over silica gel (elucnl: CH2 Cl2/CH3OH 99/1) The desired tractions were collected and the solvent was evaporated. The residue was tnturatcd in CH3CN, filtered off and dried, yielding 13g of 5.6-dihydio-['-(phenyl-methy)spirol 11H Mmidazo[2,l-b|(3]benzazepine-l 1,4' pipendme) 3 methanol (interm (o
h) A mixture : intermediate (6) -0.032. mol) and MaO2 (65gm in chlon rrn (250ml) was stirred and refluxed for 2 hours, then cooled, filtered over dicaiite and the filtrate was evaporated, yielding 11g of 5,6-dihydro-r-(phenylmethyl)spiro( IIH-imidazo¬[2,1-b][3]benzazepine-l l,4'-pipendine]-3-carboxaldehyde (interm. 7).
c) A mixture of intermediate (7) (0.0296 mol) in CH3OH/NH3 (500ml) was hydrogenated at 50°C with Rh/Al2O3 5% (2g) as a catalyst in the presence of a thiophene solution (2ml). After uptake of H2 (I equiv), the catalyst was filtered off and the filtrate was evaporated, yielding 1 Ig of 5,6-dihydro-l'-(phenylmethyI)spiro[ 1 [H-imidazo[2,l-b][3]benzazepine-ll,4'-piperidine]-3-methananvine (interm. 8). Pan of this fraction (lg) was purified by column chromatography over silica gel (eluenf. CH2Cl2/CH3OH/NH3)95/5). The pure fractions were collected and the solvent was evaporated The residue was dissolved m 2-propanol and converted into the hydro chloric acid ,alt (1:3) with 2-propanol/HCl The mixture was crystallized from DIPF The precipitate was filtered off and dried, yielding 0.8g of 5.6 dihydro l'-(phenvl-meth\! 1 //-imidazof 2.1 -hj[3)ben/azepine i ! .4' -pip-.-r idme} ■ .^ methanamine livdro, blonde i 1:3) hvdrate (IT) (interm Sai
d) A mixture of intermediate (8) (0.0198 mol; HI li('i IN [ 1 1// imida/o(2,l b|[3]benza7.epin]-3-yl|methyl|methyl|urea (interm. 9)
hxample A 5
A mixture of intermediate (8) (0.0295 mol) and tnethylamme (0035 mol) in CH2CJ2 (140ml) was stined at room temperature A solution ot acetyl chloride (0.03 mol) in CH2C12 (10ml) was added dropwise. The mixture was stined at room temperature for I hour and poured out into H2O. K2CO3 (2g) was added. The mixture was extracted with CH2Cl2 The organic layer was separated, washed with H2O2, dried, filtered and

A mixture of intermediate 14 , (0.47 mol) in MCI 6N (1500ml) was stirred until a cloudy solution, then washed with CH2Cl2 (900ml). stirred at 80°C lor I hour, cooled. alkalized with a NaOH 50% solution and extracted with CH2CI2. The organic Iaver was separated, dried (MgS04), filtered and the solvent was evaporated The residue was crystallized from CH3CN. The precipitate was filtered off and dried, yielding 38.3g of l-rnethy!-4-phenyl-4-[l-pheny ethyl)-lH-imideatly1-2-yl|piperidme (in term. 15).
e) A mixture of intermediate (15) (0.195 mol) in methanol (350ml) was hydtogenated at room temperature for 18 hours with palladium on charcoal 10% (3g) as a catalyst. After uptake of H2 (1 equiv), the catalyst was filtered off and the filtrate was evaporated. The residue was crystallized from CH3CN. The precipitate was filtered off and dried, yielding 42.3g of 4-( 1 /Y-imidazol-2-yl)- 1-methyM-phenylpiperidine (90%) (interna. 16).
0 A mixture of sodium hydride 60% (0.232 mol) in DMF (150ml) was stirred at room
temperature. Intermediate (16) (0.145 mol) dissolved in DMF (400ml) was added
dropwise, The mixture was stirred at room temperature for 1 hour. Methyl 2-chloro-
acetate (0.232 mol) dissolved in DMF (400ml) was added dropwise. The mixture was
stirred at room temperature for 20 mm. poured out into a solution of NaHCO) (20g) in
H2O (2000ml) and extracted with CH2Cl2 The organic Iaver was separated, dried
(MgS04), filtered and the solvenf was evaporated. The residue was pun tied by column
chromatograplu over silica gel ieiuem nCH2Cl3- 95/5). The pure.
fractions uere collected and the solvent v.as evaporated, sickling 40 lg of metfnl
2-(!-metvT4-phenv!-4-pipend:nv!)-l// imidazole-1-acetate (88%) (interm I7'
Example AS
a) Reaction tinder N2 atmosphere A mixture of DIPA (0 455 mol) in THF (500 ml) was stirred at 78 '(.' Butylhtfnum, 2 5 Mhcxane (0 390 mol) was added dropwise at -4()°C. The mixture was stirred tor 15 min. then re-cooled to -78V A solution of
1 -(4-phcnylbutyl) T//-imidazole, prepared according to the procedure described m
J. Chcm. Soe. Perkin Trans . 1 (1975), 17, 1670-1671, (0.325 mol) in THP (350 :nh was added dropwise at -60°C The mixture was stirred for one hour, then re-cooled to 78°C This mixture was added dropwise to a mixture of ;V,/V-dimethylfonnamide (0.390 mol, dry, pa) in THT: (500 nil), stined at -78°C The reaction mixture was stirred for one hour at -78°C, then allowed to warm to room temperature while stining overnight. A saturated aqueous NH4Cl solution (400 ml) was added and this mixture was extracted with THF. The separated organic layer was dned, filtered and the solvent

evaporated, yielding 74.2 g of l-(4-phenylbutyl)-1 H-imidazole- 2-carboxamide (lntenm. 18).
b) A mixture of intermediate (18) (0.325 mol) in methanol (1400 ml) was stirred at room temperature. NaBH4 (0.650 mol) was added portionwise and the reaction mixture was stirred for 2 hours at room temperature. The solvent was evaporated. The residue was taken up into water and this mixture was extracted with CH2C12. The separates organic layer was dried, filtered and the solvent evaporated. The residue was purified by column chromatography over silica gel (eluent: CH2CI2/CH3OH 100/0, 99/1, 97/3, 96/4, 95/5 and 93/7). The desired fractions were collected and the solvent was evaporated, yielding 49.5 gof l-(4-phenylbutyl)-lH-imidazole-2-methanol (66%) (interm. 19).
c) A mixture of intermediate (19) (0.417 mol) in methajiesulfonic acid (960ml) was stirred at 120°C for 40 hours, then cooled, poured out on ice and alkalized with NH4OH. The organic layer was separated, dried, filtered and the solvent evaporated. This fraction was purified by HPLC over silica gel (eluent: CH2C12/CH30H 97/3). A pure fraction was collected and the solvent was evaporated. The residue was crystallized from DEPE. The precipitate was filtered off and dried, yielding 15.7g of 6,7,8,13-tetrahydro-5H-imidazo[2,l-b][3]benzazonine (18%) (interm. 20).
d) A mixture of DIPA (0.151 mol) in THF (650ml) was stirred at -78°C under N2 flow. Butyllithium 2,5M in hexane (0.144 mol) was added dropwise at a temperature below -40°C. The mixture was stirred at -78°C for 15 min. Intermediate (20) (0.072 mol) in a small amount of THF was added dropwise at a temperature below -55oC The mixture was stirred at -78°C for 1 hour. N,N-bis(2-chloroethyl)benzenernethanamine hydrochloride in a small amount of THF was added dropwise at a temperature below -SOX. The mixture was stirred at 78°C for 1 hour, allowed to warm to room temperature overnight and decomposed with H20. The organic solvent was evaporated. The aqueous concentrate was extracted with CH2C12. The organic layer was separated, dried, filtered and the solvent was evaporated. This fraction was purified by column chromatography over silica gel (eluent: CH2CI2/CH,OH 100/0, 99/1. 98/2, 96/4, 94/6 and 92/8). A fraction was collected and the solvent was evaporated, yielding 5,6,7,8-tetrahydro-1 '-(phenylmethyl)spiro[13H-imidazo[2,1 -b] [3 Jbenzazonine-13,4'-pipendine] (interm. 21),
Example A9
A mixture of 5,10-dihydro-imidazo[l,2-blisoquinoIine-7.8-diol, obtained according to the procedure described in Ex.No. A8 c, (0.155 mol), phenyltrimethylammonium chloride (0.31 mol) and K2C03 (0.68 mol) in DMF (400ml) was stirred at 90°C for 20

hours, cooled, poured out into H2O and filtered over dicalite. The filtrate was separated into its layers. The organic layer was washed with H2O, dried (MgS04), filtered and the solvent was evaporated. The residue was purified over silica gel on a glass filter (eluent: CH2C12/CH30H 100/0 to 97/3). The pure fractions were collected and the solvent was evaporated, yielding 3g of 5,10-dihydro-7,8-dimethoxyimidazo[l,2-b]iso-quinoline (8.4%) (interm. 22).
Example A10
A mixture of intermediate (31) (see Table 1), prepared according to the procedure described in Ex.No. A8d, (0.01 mol) in HBr 48 % solution (60ml) was stirred and refluxed for 2 hours. The solvent was evaporated The residue was taken up in a small amount of H20. The mixture was alkalized with K2CO3 and extracted with CH2CI2/CH3OH. The organic layer was separated, dried, filtered and the solvent was evaporated, yielding 4.3g of 5,6-dihydro-r-(phenylmethyl)spiro[l lH-imidazo-[2,l-bJ[3]benzazepine-ll,4'-piperidine]-8,9-diol (100%) (interm. 23).
Example All
A mixture of compound (22) (0.0117 mol) and triethyl amine (0.0421 mol) in toluene (100ml) was stirred and refluxed. Ethyl carbonochloridate (0.0702 mol) was added dropwise at reflux temperature. The mixture was stirred and refluxed for I hour, cooled, poured out into H2O and K2CO3 (15g) and separated into its layers. The aqueous layer was extracted with CH2CI2. The combined organic layer was dried (MgS04), filtered and the solvent was evaporated. The residue was punfied over silica gel on a glass filter (eluent: CH2Cl2/ethanol 96/4). The pure fractions were collected and the solvent was evaporated. The residue was boiled in DIPE. The precipitate was filtered off and dried, yielding 2.4g of [l'-(ethoxycarbonyl)spiro[ 1 l H-imidazo[2,l-b]-[3)benzazepme-ll.4'-piperidine)-6-yl] ethyl carbonate (33%) (interm. 24).
Table 1 lists intermediates which were prepared according to one of the above mentioned examples.
Table 1

B. Preparation of final compounds Example Bl (preparative example)
A mixture of intermediate (2) (0.02 mol) in methanol (150ml) was hydrogenated with palladium on charcoal 10% (2g) as a catalyst at 50°C for 18hours. After uptake of H2 (leq), the catalyst was filtered and the filtrate was evaporated, yielding 5,6-dihydro-spiro[ 1 lH-imidazo[2,1 -b][3]benzazepine-1 l,4'-piperidine] (comp. 6; not claimed). This fraction was converted into the hydrochloric acid salt (1:1) in CH3CN, yielding 5g of 5.6-dihydrospiro(imidazo[l,2-b][3)benzazepine-l1[1 lHl,4'-piperidine] monohydrochloride (86%) (comp. 6a; not claimed). A fraction obtained in said way, can also be converted into the (E)-2-butenedioic acid salt.
Example B2
a) A mixture of compound (6) (0.1 mol) and N,N-diethylethanamine (0.13 mol) in CH2C12 (300ml) was stirred at a temperature below 10°C. Ethyl carbonochloridate (0.12 mol) was added dropwise at this temperature. The mixture was allowed to warm

to room temperature and then stirred at room temperature for 1 hour. Water and K2C03 (10g) were added. The mixture was separated into its layers. The aqueous layer was extracted with CH2C12. The combined organic layer was dried (MgSO4), filtered and the solvent was evaporated, yielding 35.4g of ethyl 5,6-hydrospiro[llH-imidazo-[2, l-b][3]benzazepine-U,4'-piperidine]-l-carboxylate (100%) (comp. 4).
b) A mixture of compound (4) (0.1 mol), sodium acetate (0.3 mol) and acetic acid (0.258 mol) in formaldehyde 38% solution (165ml) was stirred and refluxed for 10 hours. The mixture was poured out into ice and a NaOH solution and extracted with CH2CI2. The organic layer was separated, dried (MgSO4), filtered and the solvent was evaporated. The residue was purified by column chromatography over silica gel (eluent: CH2Cl2/ethanol 95/5 to 90/10). The pure fractions were collected and the solvent was evaporated, yielding 16.5g of ethyl 5,6 dihydko-3(ydroxyrnethyi)spiro-[1 lH-irnida2o[2,l-b][3]-ben2azepine-ll14'-piperidine]-r-carboxylate (46%)(comp. 5).
c) A mixture of compound (5) (0.046 mol) and potassium hydroxide (0.46 mol) in 2-propanol (130ml) was stirred and refluxed for 7 hours. The solvent was evaporated. The residue was taken up in water and extracted with CH2CI2. The organic layer was separated, dried (MgS04), filtered and the solvent was evaporated, yielding 11.5g of 5,6-dihydrospiro[llH-irrudazo[2,l-b][3]ber^azepine-ll,4'-piperidine]-3-methanol (88%) (comp. 18). Pan of this fraction (lg) was dissolved in CH3OH and converted into the (E)-2-butenedioic acid salt (2:1). The precipitate was filtered off and dried, yielding 0.6g of 5,6-dihydrospiro[l lH-irrudazo[2.1-b][3]benzazepine-ll,4'-piperidine]-3~methanol (E)-2-butenedioic acid salt (2:1) (comp. 18a).
Example B3
A mixture of compound (6) (0.01 mol) and (CH20)n (0.066 mol) in methanol (150ml) and thiophene 4% solution (1ml) was hydrogenated with palladium on charcoal 10% (lg) as a catalyst at 50°C. After uptake of H2 (Ieq), the catalyst was filtered and the filtrate was evaporated. The residue was taken up in H2O/K2CO3/NH4OH and stirred. The mixture was extracted with CH2C12, dried, filtered and evaporated. The residue was converted into the cyclohexanesulfamic acid salt (1:2) in 2-propanone and recrystallized twice from 2-propanol, yielding 2.44g of 6,1 l-dihydro-l'-methyl-spiro[5H-imidazo[2,l-b][3]benzazepine-ll,4'-piperidine] cyclohexylsulfamate(l:2) (40%) (comp. I).
Example B4
a) A mixture of 1-bromobutane (0.012 mol), compound (6) (0.01 mol), Na2C03 (0.02 mol) and potassium iodide (few crystals) in 2-butanone (200ml) was stirred and refluxed overnight. The mixture was evaporated, the residue was taken up in water and

extracted with CH2C12. The organic layer was dried, filtered off and evaporated. The residue was purified by column chromatography over silica gel (eluent: CH2C12/ (CH3OH/NH3) 95/5). The pure fractions were collected and evaporated. The residue was converted into the hydrochloric acid salt (1:2) in 2-propanol. The precipitate was filtered and dried, yielding 0.7g of r-butyl-5,6-dihydrospiro[imidazo[2,l-b][3]-benzazepine-ll-[l lH],4'-piperidine] dihydrochloride.hemihydrate (18%) (comp. 3).
b) A mixture of l-(3-chloropropoxy)-4-fluorobenzene (0.018 mol), 5,6-dihydro-
spiro[llH-imidazo[2,l-b][3]benzazepine-ll,4'-piperidine] (0.015 mol), Na2C03
(0.015 mol) and Kl (10 mg) in 4-methyl-2-pentanone (200ml) was stirred and refluxed
for 18 hours. The mixture was poured into water, separated and the aqueous layer was
extracted with CH2C12. The organic layer was dried (MgS04), filtered off and
evaporated. The residue was purified on a glass filter over silica gel (eluent:
CH2C12/CH30H 90/10). The pure fractions were collected and evaporated. The residue
was converted into the cyclohexylsulfamic acid salt (1:2) in 2-propanone. Yielding :
4.26gof l'-[3-(4-fluorophenoxy)propyl]-5,6Kiihydrospiro[irnidazo[2,l-b][3]benza-
epine-11-[1 lH],4'-piperidine] cyclohexylsulfamate(l:2) (37%); mp. 180°C
(comp. 71).
c) A mixture of l-chloro-3-methyl-2-butene (0.02 mol), 5,6-dihydrospiro[ 11H-imidazo(2,l-b][3]benzazepine-ll,4'-piperidine] (0.015 mol), Na2C03 (0.015 mol) and Kl (0.015 mol) in N.N-dimethylaceetamide (150ml) was stirred at room temperature overnight. The mixture was filtered over dicalite and evaporated. The residue was taken up in CH2Cl2/water 95/5. The precipitate was filtered off and dried. Yielding : 0.86g of 5,6-dihydro-r-(3-methyl-2-butenyl)spiro[imidazo(2,l-b][3]benzazepine-ll-[11H],4'-piperidine] monohydroiodide (12.7%): mp. 255.4°C (comp. 74).
d) A mixture of l-(2-bromoethyl)-4-ethyl-1.4-dihydro-5H-tetrazol-5-one (0.012 mol), 5,6-dihydrospiro[llH-imidazo[2,l-b][3]benzazepine-H,4'-piperidine] (0.01 mol), Na2C03 (0.01 mol) and Kl (10 mg) in 4-methyl-2-pentanone (200ml) was stirred and refluxed for 18 hours. The mixture was poured into water. The mixture was separated and the aqueous layer was extracted with 3-methyl-2-butanone, dried (MgSO4), filtered and evaporated. The residue was purified on a glass filter over silica gel (eluent: CH2Cl2/CH3OH 95/5 to 93/7). The pure fractions were collected and evaporated. The residue was converted into the hydrochloric acid salt (1:2) in C2H5OH. Yielding : 2.63g of l-[2-(5,6-dihydrospiro[llH-imidazo[2,l-b][3]benzazepin-ll,4'-piperidin]-r-yl)ethylH-ethyl-1,4-dihydro-5H-tetrazol-5-one dihydrochloride (56%); mp. 230°C (comp. 75).
e) A mixture of chloroacetonitrile (0.11 mol), 5.6-dihydrospiro[llH-imidazo[2,l-b]-[3]benzazepine-l l,4'-piperidine] (0.1 mol) and MN-diethylethanamine (0.12 mol) in

DMF (400ml) was stirred at room temperature for 48 hours . The mixture was poured into water and extracted with CH2C12. The organic layer was dried (MgS04), filtered off and evaporated. The residue was purified on a glass filter over silica gel (eluent: CH2CI2/CH3OH 96/4). The pure fractions were collected and evaporated. The residue was crystallized from CH3CN. Yielding: 18.5g5,6-dihydrospiro[irmdazo[2,l-b][3]-benzazepine-1 l-[l lH],4'piperidine]-r-acetonitrile (63%); mp. 152.6°C (comp. 76).
Example B5
Bis(l,l-dimethylethyl) dicarbonate (0.095 mol) dissolved in a small amount of CH2Cl2 was added dropwise to a stirring mixture of compound (6) (0.079 mol) in CH2C12 (250ml). The mixture was stirred at room temperature for the weekend, then washed with H20, dried, filtered and the solvent was evaporated. Toluene was added and evaporated again. The residue was stirred in DIPE. The precipitate was filtered off and the filtrate was evaporated. This fraction was purified over silica gel on a glass filter (eluent: CH2C12/CH30H 100/0,99/1,98/2 and 9674). The pure fractions were collected and the solvent was evaporated. The residue was stirred in hexane. The precipitate was filtered off and dried, yielding 15.05g of 1,1-dimethylethyl 5,6-dihydrospiro[llH-imidazo[2,l-b][3]benzazepine-l l,4'-piperidine]-r-carboxylate (54%) (comp. 7).
Example B6
a) A mixture of tetrahydro-2-furanmethanol methanesulfonate (0.0lmol), compound 6 (0.0lmol) and Na2C03 (002mol) in 4-methyl-2-pentanone (150ml) was stirred and refluxed overnight. The reaction mixture was filtered over dicalite. The filtrate was evaporated. The residue was purified by column chromatography over silica gel (eluent: CH2C12/(CH30H/NH3) 95/5). The pure fractions were collected and the solvent was evaporated. The residue was dissolved in 2-propanone and converted into the cyclohexane sulfamic acid salt (1:2). The precipitate was filtered off and dried. Yielding: 1.48g of 5,6-dihydro-r-[(tetrahydro-2-furanyl)methyI]spiro[imidazo[2,l-b] [3]benzazepine-l 1(1 lH],4'-piperidine] cyclohexylsulfamate(l:2) monohydrate (20.7%); mp. 120.2°C (comp. 72).
b) A mixture of compound 6 (0.02 mol) and 2-thiophenecarboxaldehyde (0.053 mol) in methanol (300ml) was hydrogenated with Raney Nickel (2g) as a catalyst. After uptake of H2 (leq), the catalyst was filtered off and the filtrate was evaporated. The residue was purified by column chromatography over silica gel (eluent: CH2C12/ CH3OH 95/5). The pure fractions were collected and evaporated. The residue was converted into the cyclohexanesulfamic acid salt (1:1) in 2-propanone. The precipitate was filtered off and dried. The residue was recrystallized from 2-propanol. The precipitate was filtered off and dried. Yielding : 0.72g of 5,6-dihydro-l'-(2-thienyl-

methyl)spiro[imidazo[2,l-b][3]benza2epine-l 1(1 lH],4'-piperidine] cyclohexyl-sulfamate(l:l) (6.6%); mp. 211.1°C (comp. 73).
Example B7
a) A mixture of compound (9) (0.155 mol), prepared according to the procedure described in Ex. No. B2 b, and Mn02 (300g) in chloroform (1200ml) was stirred and refluxed for 90 min. The mixture was filtered over dicalite and the filtrate was evaporated. Part of this fraction (lg) was crystallized from CH3CN. The precipitate was filtered off and dried, yielding 0.5g of 1,1-dimethylethyl 3-formyl-5,6-dihydro-spirotinudazo[ 2,1-b][3] berizazepine-ll4'-piperidinel-l-carboxylate (comp. 12).
b) A mixture of compound (12) (0.134 mol), NaCN (0.705 mol) and Mn02 (233g) in methanol (2500ml) was stirred at room temperature. Acetic acid (45.5ml) was added dropwxse. The mixture was stirred and refluxed for 20 hours and filtered over dicalite. The filtrate was evaporated. The residue was taken up in H20, CH2CI2 and K2C03. The mixture was separated into its layers. The aqueous layer was extracted with CH2CI2. The combined organic layer was dried (MgSCU), filtered and the solvent was evaporated. The residue was purified by column chromatography over silica gel (eluent: CH2Cl2/CH3OH 97/3). A pure fraction was collected and the solvent was evaporated, yielding 47.7g of methyl (1,1-dimethylethyl) 5,6-dihydrospiro[11H irnidazo[2,l-b][3]benzazepine-l l,4'-piperidine]-3,1'-dicarboxylate (87%) (comp. 13).
c) A mixture of compound (13) (0.056 mol) in NaOH IN (100ml), H20 (250ml) and THF (250mJ) was stirred at room temperature for 18 hours. The organic solvent was evaporated. The aqueous concentrate was neutralized with HCI IN (100ml) and extracted with CH2C12. The organic layer was separated, dried (MgSO4), filtered and the solvent was evaporated. Part of this fraction (2g) was crystallized from CH3CN. The precipitate was filtered off and dried, yielding l.l6g of l'-[(l,l-dirnethylethoxy)-carbonyll-5,6-6jhydrospiro[llH-imidazo[2,l-b][3]benza2epine-ll,4'-piperidine]-3-carboxylic acid (comp. 14).
d) A mixture of compound (14) (0.04 mol) and N,N-dimethyl-4-pyridinamine (0.04 mol) in CH2C12 (300ml) was stirred until complete dissolution. N.N-diethyl-ethanamine (0.05 mol) was added. Then Ar-(ethylcarbonirnidoyl)-N,N-dimethyl-l,3-propanediamine monohydrochloride (0.05 mol) was added portionwise. The mixture was stirred at room temperature for 30 min! N,N-diethylethanamine (0.06 mol) was added and then NH4Cl (0.05 mol) was added portionwise. The mixture was stirred at room temperature overnight, poured out into H2O and separated into its layers. The aqueous layer was extracted with CH2CI2. The combined organic layer was dried (MgSO4), filtered and the solvent was evaporated. The residue was purified by column

chromatography over silica gel (eluent: CH2CI2/CH3OH 97.5/2.5). The pure fractions were collected and the solvent was evaporated. The residue was crystallized from CH3CN. The precipitate was filtered off and dried, yielding 9.5g of 1,1-dimethyIediyl 3 -(arru nocarbon yl )-5,6-dihydrospi ro[ 11 H midazo[2,1 -b] [3 ] benzazepine- 11 ,4'-piperidine]-r-carboxylate(60%)(comp. 16).
e) A mixture of compound (16) (0.023 mol) in HCI/2-propanol (25ml) and methanol (100ml) was stirred and refluxed for 90 min and then cooled. The precipitate was filtered off and dried, yielding 8g of 5,6-dihydrospiro[l lH3 -imidazo[2,l-b][3]-tenzazepine-ll,4'-piperidine]-3-carboxamide dihydrochloride(94%)(comp. 17). The precipitate can also be converted into the (E)-2-butenedioic acid salt.
0 Preparation of compound 61
A mixture of compound (17) (0.0135 mol) and NaHC03 (0.0271 mol) in THF (100ml) and ethanol (50ml) was stirred and refluxed for 10 min. Methyl 2-propenoate (0.0149 mol) was added. The mixture was stirred and refluxed for 3 hours and then cooled. The solvent was evaporated under reduced pressure. The residue was partitioned between H20 and CH2C12. The organic layer was separated, dried (MgS04), filtered and the solvent evaporated. The residue was purified by column chromatography over silica gel (eluent: CH2C12/(CH30H/NH3) 95/5 to 90/10). The pure fractions were collected and the solvent was evaporated. The residue was purified again by column chromatography over silica gel (eluent: CH2CI2/(CH3OH/NH3) 99/1 to 97/3). The pure fractions were collected and the solvent was evaporated. The residue was refluxed in CH3OH/diethyl ether 2:8 (precipitation resulted). The precipitate was filtered off, washed with diethyl ether and dried in vacuo at 40°C overnight. Yielding: 2.27g of compound 61.
g) /V,/V-diethylethanamine (0.0081 mol) was added at room temperature to a suspension of compound 17 (0.004 mol) in methanol (100ml). The mixture was cooled to 0°C. Oxirane was bubbled through the rruxture for 45 min. The mixture was allowed to warm to room temperature and then stirred at room temperature for 30 min. The solvent was evaporated under reduced pressure. The residue was purified by column chromatography over silica gel (eluent: CH2Cl2/(CH3OH/NH3) 97/3 to 95/5). The pure fractions were collected and the solvent was evaporated. The residue was crystallized from CH3OH/CH2C12 1:4. The precipitate was filtered off and dried. Yielding: 0.25g of 6,ll-dihydro-r-(2-hydroxyetehyl)spiro[5H-imidazo[2,l-b][3]-benzazepine-1 l,4'-pipendine]-3-carboxamide (18%) (compound 62).

MN-diethylethanamine (0.0113 mol) was added at room temperature to a suspension of compound 17 (0.0054 mol) in methanol (100ml). After 5 min, oxirane was bubbled through the mixture at 0°C for 1 hour. The solvent was evaporated. The residue was suspended in t-butanol (200ml). Methyl chloroacetate (0.007 mol) andJV./V-diethyl-ethanamine (0.0054 mol) were added. The mixture was stirred and refluxed for 48 hours. The solvent was evaporated. The residue was purified by column chromato¬graphy over silica gel (eluent: CH2Cl2/(CH3OH/NH3) 98/2 to 95/5). Two fractions were collected and the solvent was evaporated. Fraction 1 was crystallized from CH3OH/CH3CN 1:3. The precipitate was filtered off and dried. The residue was purified by column chromatography over silica gel (eluent: CH2Cl2/(CH3OH/NH3) 97/3 to 95/5). The pure fractions were collected and the solvent was evaporated. Yielding: 0.46g of compound 63.
i) N,N-diethylethanamine (0.0271 mol) was added at room temperature to a suspension of compound 17 (0.0129 mol) and ethyl a-methylenebenzeneacetate (0.0140 mol) in DMF (100ml). The mixture was stirred at room temperature over the weekend. The solvent was evaporated. The residue was extracted with CH2Cl2/H2O. The mixture was separated into its layers. The precipitate in the organic layer was filtered off. Yielding: 2.6g of ethyl 3-(aminocarbonyl)-6,l l-dihydro-a-phenylspiro[5H-irnidazo-[2,l-b][3]benzazepine-ll.4'-piperidinel-l'-propanoate monohydrochloride (compound 64).

A mixture of compound 17 (0.0027 mol), l-(3-chloropropyl)-l,3-dihydro-2H-benzimidazol-2-one (0.003 mol). Na2CO3 (0.0027 mol) and Kl (few crystals) in CH3CN (100ml) was stirred and refluxed for 48 hours. The solvent was evaporated. The residue was purified by column chromatography over silica gel (eluent: CH2CI2/ (CH3OH/NH3) 99/1 to 95/5). Two fractions were collected and their solvents were evaporated. The desired fraction was purified again by column chromatography over

silica gel (eluent: CH2Cl2/(CH3OH/NH3) 97/3 to 95/5). The pure fractions were collected and the solvent was evaporated. Yielding: 0.18g of compound 65.
A mixture of isobutyl (2-chloroethyl)carbamoate (0.008 mol), 5,6-dihydrospiro[11H-imidazo[2,l-b][3]benzazepine-l l,4'-piperidine]-3-carboxamide dihydrochloride (0.004 mol). 4-methyl-2-pentanone (50 ml), Na2C03 (0.020 mol) and KI (catalytic quantity) was stirred and refluxed (oil bath: 130°C) overnight. The solvent was evaporated (vacuum, 60°C). Water was added. CH2CI2/CH3OH 90/10 was added. The organic layer was separated, dried (MgS04), filtered and the solvent was evaporated. The residue was purified by column chromatography over silica gel (eluent: CH2C12/ (CH3OH/NH3) 95/5). The desired fractions were collected and the solvent was evaporated. Yield: 1.5 g of compound 66 (85.4%).

A mixture of compound 66 (0.00227 mol) and HCl/2-propanol (3 ml) in 2-propanol (30 ml) was stirred at 80°C (oil bath). The solvent was evaporated (vacuum, 40°C). 2-Propanol was added, then evaporated (2 x). Ethanol was added, then evaporated. The residue was stirred in boiling ethanol (50 ml), then filtered off over a P4 glass filter and the product was dried under a stream of N2. Yield: 0.254 g (24.0%). The filtrate was stirred for 3 hours while cooling on an ice-bath. The precipitate was filtered off over a P3 glass filter and dried (vacuum, 60°C, 3 hours). Yield: 0.304 g (28.7%). The filtrate was evaporated. The residue was dried (over the weekend under N2 flow). Total yield: 70.4% of compound 67.
m) Methyl chloroformate (0.0036 mol) was added at room temperature to a suspension of compound (17) (0.0032 mol) in CH2C12 (100ml). A mixture of N,N-diethylethan-arrune (0.0097 mol) in CH2CI2 (20ml) was added dropwise. The mixture was stirred at room temperature for the weekend. The solvent was evaporated. The residue was purified by column chromatography over silica gel (eluent: CH2CI2/CH3OH 99/1 to 98/2). The pure fractions were collected and the solvent was evaporated. The residue was crystallized from CH3CN. The precipitate was filtered off and dried. Yield: 0.68g

of 3-(aminocarbonyl)-6,l l-dihydrospiro(5H-imidazo[2,l-b][3]-benzazepine-l 1,4'-piperidine]-r-carboxylate (60%) (comp. 79).
n) A mixture of compound (17) (0.005 mol), KOAc (2g) and paraformaldehyd (0.5g) in methanol (100ml) was hydrogenated with palladium on charcoal 10% (0.5g) as a catalyst in the presence of a thiophene solution (1ml). After uptake of H2 (1 equiv), the catalyst was filtered off and the filtrate was evaporated. The residue was purified by column chromatography over silica gel (eluent: CH2Cl2/(CH3OH/NH3) 97/3). The pure fractions were collected and the solvent was evaporated. This fraction was purified again by column chromatography over silica gel (eluent: CH2C12/(CH30H/NH3) 97/3 to 95/5). The pure fractions were collected and the solvent was evaporated. Yield: 0.43g of 6'11-Kiihydro-r-memylspiro[5H-imida2o[2,l-b][3]benzazepine-ll,4,-piperidine]-3-carboxamide monohydrate (28%) (comp. 80).
Example B8
a) A solution of compound (7) (1.63 mol) in CH2C12 (7500ml) was cooled to 0°C under N2 flow. l-Bromo-2,5-pyrrolidinedione (1.63 mol) was added portionwise (29g each). H20 (3000ml) was added. The mixture was stirred overnight. The organic layer was separated, dried, filtered and the solvent was evaporated. This fraction was purified by HPLC over silica gel (eluent: CH2Cl2/CH3OH 100/0, 98/2, 90/10 and 100/0). A pure fraction was collected and the solvent was evaporated, yielding 189g of 1,1-dimethyl-ethyl 2.3-dib^omo-5,6-dihydrosp^ro[ll//-lmidazo[2,l-b][3]benzazepine-ll,4,-piperidine]-l'-carboxylate (27%) (comp 48). The 3-monobromo analogue (comp. 60; Ex. No. B 10a) can be prepared in a similar way.
b) A mixture of compound (48) (0.02 mol), acetic acid, palladium(2+) salt (0.15g) and l,3-propanediylbis[diphenylphosphinej (0.55g) in THF (150ml) was stirred in an autoclave at 150°C for 16 hours under pressure of CO gas (30 bar) and NH3 gas (10 atm). The mixture was cooled, filtered and the filtrate was evaporated. This fraction was purified over silica gel on a glass filter (eluent: CH2Cl2/CH3OH 95/5). The pure fractions were collected and the solvent was evaporated. The residue was crystallized from CH3CN. The precipitate was filtered off and dried, yielding 1,1-dimethylethyl 2,3-bis(aminocarbonyl)-5,6-dihydrospiro[l lH-imidazo[2,l-b][3]benzazepme-ll,4'-piperidine] 1-1'-carboxylate (comp. 49)
Example B9
Dibenzoyl peroxide (0.5g) was added to a stirring mixture of compound (7) (0.039 mol) in CH2CI2 (210ml). l-Chloro-2,5-pyrrolidinedione (0.078 mol) in a small amount of CH2C12 was added dropwise. The mixture was stirred at room temperature overnight. The solvent was evaporated. H20 was added and the mixture was extracted with

CH2C12. The organic layer was separated, dried, filtered and the solvent was evaporated. The residue was purified over silica gel on a glass filter (eluent: CH2CI2/ CH3OH 100/0,99/1, 98/2,96/4 and 94/6). The pure fractions were collected and the solvent was evaporated. Some starting material (7.5g; 0.02 mol) was recuperated. The reaction was carried out again. Dibenzoyl peroxide (0.5g) was added to a stirring mixture of compound (7) (0.02 mol) in CH2CI2 (210ml). 1 -Chloro-2,5-pyrroIidinedione (0.078 mol) in a small amount of CH2Cl2 was added dropwise. The mixture was stirred at room temperature overnight. The solvent was evaporated. H20 was added and the mixture was extracted with CH2C12. The organic layer was separated, dried, filtered and the solvent was evaporated. The residue was purified over silica gel on a glass filter (eluent: CH2Cl2/CH3OH 100/0,99/1 and 98.5/1.5). The pure fractions were collected and the solvent was evaporated. The residue was combined with the one obtained from the first reaction, yielding 14g of 1,1-dimethylethyl 3-chloro-5,6-dihydrospiro[llH-imidazo[2,l-b][3]ben2azepine-ll,4,-piperidine]-r-carboxylate (93%) (comp. 19).
Example B10
a) CH2C12 (87 ml) was added to 1,1-dimethylethyl 5,6-dihydrospiro[llH-imidazo[2,l-
b][3]benzazepine-l l,4'-piperidinel-l'-carboxylate (comp. 7) in methanol (0,0582 mol).
Water (58 ml) was added. Water (58 ml) and Na2CO3 (0.0582 mol) were added to the
separated organic layer and the mixture was cooled to 0-5°C (solution I).
Br2 (0.0565 mol) was added to a solution of tetrabutylammoniumbromide (0.0565 mol) and CH2C12 (29 ml). This mixture was stirred for 25 minutes at 15-25°C and added to solution 1 during I hour. After stirring for I hour at 20°C, water (58 ml) was added. The separated organic layer was evaporated. 3-Methyl-2-butanone (87 ml) and water (29 ml) were added to the oily residue and this mixture was heated to 80°C. The separated organic layer was wased with water (29ml) at 80°C. The organic layer was azeotroped till 116°C. 3-Methyl-2-butanone (40.7 ml) was distilled off and the product was crystallized during 2 hours at 50°C. The crystallized product was filtered off, washed with 3-methyl-2-butanone and dned (vacuum. 50°C). Yield : 13.03g of 1,1-dimethylethyl 3-bromo-5,6-dihydrospiro[l lH-imidazo[2,l-b][3]benzazepine-l 1,4'-piperidineH'-carboxylate (51.8%) (comp. 60).
b) A mixture of compound (60) (0.257 mol), DMF (515 ml), H20 (26 ml) and CuGN
(1,287 mol) were heated till 132°C, stirred for 17 hours and then cooled to room
temperature. The mixture was poured into 2056 ml of H20 and stirred for 2 hours. The
precipitate was filtered off, washed twice with H2O (149 ml) and dried (vacuum,
100°C). The resulting precipitate was refluxed in 3-methyl-2-butanone (772 ml) for 30

min, followed by cooling the reaction mixture to 50°C and filtering. NH4OH (129 ml) was added to the filtrate at 50°C and stirred for 30 min. The 3-methyl-2-butanone layer was separated and washed with NH4OH (129 ml) as described above. This procedure was repeated for another 5 times. The 3-methyl-2-butanone layer was separated again, azeotroped for 30 min and partially evaporated. The resulting mixture was crystallized and the precipitate was filtered, washed with 3-methyl-2-butanone (7.7 ml) and dried (vacuum, 50°C). Yield : 52.4 g of l,l-dimethylethyl 3-(aminocarbonyl)-5,6-dihydro-spiro[llH-imidazo[2,l-b][3]benzazepine-ll,4'-piperidine]-r-carboxylate (53%) (comp. 16).
Example Bll
a) A mixture of intermediate (18) (0.152 mol) in trifluoromethanesulfonic acid (500ml) was stirred at 158°C for 90 hours. The mixture was cooled, poured out on ice and K2C03 (800g) and extracted with CH2C12. The organic layer was separated, dried (MgSO4), filtered and the solvent was evaporated partially until 100ml while the temperature was kept below 40°C. The concentrate was purified immediately by column chromatography over silica gel (eluent: CH2Cl2/(CH30H/NH3) 95/5). The pure fractions were collected and the solvent was evaporated, yielding 18.lg of 1-methyl-spiro[llH-imidazo[2,l-b][3]benzazepine-l l,4'-piperidin]-6(5H)-one (42%) (comp. 22). Part of this fraction (1.5g) was dissolved in ethanol and converted into the (E)-2-butenedioic acid salt (2:3). The precipitate was filtered off and dned, yielding 1.92g of l-methylspiro[11H-imidazo[2,l b][3]benzazepine-ll,4'-piperidin]-6(5H)-one (E)-2-butenedioic acid salt (2:3) (comp. 22a).
b) A mixture of intermediate (24) (0.041 mol) in HBr 48% solution (250ml) was stirred and refluxed for 4 hours. The mixture was poured out on ice and K2CO3 and extracted with CH2CI2. The organic layer was separated, dried (MgSO4), filtered and the solvent was evaporated, yielding 10.4gof spiro[llH-imidazo[2,l-b][3]benzazepine-ll,4'-piperidin]-6(5H)-one (95%) (comp. 23). Part of this fraction (0.9g) was dissolved in ethanol and converted into the (E)-2-butenedioic acid salt (2:3). The precipitate was filtered off and dried, yielding 0.78g of spiro[ 1 lH-imidazo[2,l-b][3]benzazepine-ll,4'-piperidin]-6(5H)-one (E)-2-butenedioic acid salt (2:3) (comp. 23a).
c) A mixture of compound (23) (0.01 mol) in methanol (300ml) was stirred on an ice bath. NaBH4 (0.02 mol) was added portionwise over a 15-min period. The mixture was stirred on an ice bath for 1 hour. The solvent was evaporated at a temperature below 40°C. The residue was taken up in H2O and the mixture was extracted with CH2CI2/ CH3OH 90/10. The organic layer was separated, dried (MgS04), filtered and the

solvent was evaporated, yielding 2g of 5,6-dihydrospiro[11H-imidazo[2,l-b][3]-benzazepine-ll,4'-piperidine]-6-ol (75%) (comp. 26).
d) A mixture of compound (26) (0.0075 mol) in methanesulfonic acid (50ml) was stirred at room temperature for 40 min. The mixture was poured out on ice, alkalized with a NaOH 50% solution and extracted with CH2CI2- The organic layer was separated, dried (MgS04), filtered and the solvent was evaporated, yielding 2g of spiro[ll H-imidazo[2,l-b][3]benzazepine-l l,4'-piperidine] (100%) (comp.27). Part of this fraction (0.3g) was dissolved in ethanol and converted into the (E)-2-butenedioic acid salt (1:1). The precipitate was filtered off and dried, yielding 0.26g spiro[llH-imidazo[2,l-b](3]benzazepine-l l,4'-piperidine] (E)-2-butenedioic acid salt (1:1) (comp. 27a).
Example B12
A mixture of compound (24) (0.0128 mol) in H2S04(5ml) and methanol (100ml) was stirred and refluxed for the weekend. The solvent was evaporated. The residue was taken up in H2O. The mixture was alkalized with a NaOH solution and extracted with CH2CI2. The organic layer was separated, dried, filtered and the solvent was evaporated, yielding 4.4g of 5,6-dihydro-2,3-bis(methoxymethyl)spiro[l1 H-imidazo¬[2,1,-b][3]benzazepine-11,4'-pipendine] (100%) (comp. 31).
Example B13
a) A mixture of 5,6-dihydrospiro[imidazo(2,l-bl[3]benzazepine-l 1-[11H],4'-pipendine)-r-acetonitrile (comp. 76) (0 055 mol) in NH3/CH3OH (500ml) was hydrogenated with Raney Nickel (2g) as a catalyst at room temperature. After uptake of H2 (2eq), the catalyst was filtered off and the filtrate was evaporated. Yielding : 20.9gof 5,6-dihydrospiro(imidazo(2,l-bl[31benza2epine-ll-[llH],4'-piperidine]-r-ethanamine 2-propanolate(2:l). tnhydrochlonde. sesquihydrate; mp. 245.9°C (comp. 77).
b) A mixture of 2-chloropyrimidme (0.012mol), 5,6-dihydro-spiro[imidazo[2,l-b][3]-benzazepine-1 l-[11H],4'-piperidine]l'-ethanamine (O.Olmol) and Na2C03 (0.02mol) in 4-methyl-2-pentanone (200ml) was stirred and refluxed for 48 hours. The reaction mixture was filtered over dicalite. The filtrate was evaporated. The residue was purified by column chromatography over silica gel (eluent: CH2C12/(CH30H/NH3) 95/5). The pure fractions were collected and the solvent was evaporated. The residue was dissolved in 2-propanol and converted into the hydrochloric acid salt (1:3). The precipitate was filtered off and dried. Yielding: 0.94g of 5.6-dihydro-N-2-pyrimidinyl-spiro[imidazo[2,l-b][3]benzazepine-11 -[ 11H]1,4'-piperidine]-l'-ethanamine trihydrochloride. monohydrate.2-propanolate(l:l) (16.7%) (comp. 78).

c) 3-Chloro-6-(3-methyl4,2,4-th«adiazol-5-yl)pyridazine (0.01 mol) and 5,6-dihydro-spiro[imidazo[2,l-b][3]benzazepine-U-(l lH],4'-piperidinc]-r-ethananune (0.01 mol) were stirred at 140°C for 2h. The mixture was cooled and purified by column chromatography over silica ge! (eluent: CH2Cl2/(CH3OH/NH3) 95/5). The pure fractions were collected and evaporated. The residue was converted into the hydro¬chloric acid salt (1:4) in 2-piopanol and dned. Yielding : 2.22g of 2-[[2-(5,6-dihydro-spiro[imidazo[24-b][3]benza2epine-11-[11H],4'-piperidin]-1-yl)ethyl]amjno]-4(lH) pyrimidinone trihydrochloride.2-propanolate(l.T). sesquihydrate (36.6%) (comp. 68).

The following Tables list compounds of formula (I) as prepared according to one of the above examples (Ex. No.).

(1) cyclohexylsulfamate (1:2); (2) hydrochloric acid (1:2); (3) (E)-2-butenedioate (1:1); (4) (E)-2-butenedioate(2:l)
Table 3

Co
No. Ex. No. R1 -A-B- Salt/Melting point
57 58 B2c B12 H -CH2-0-CH3 -S-CH=CH--CH=CH-CH=CH- -
(3) (E)-2-butenedioate (1:1); (5) hydrochloric acid (I: I); (6) (E)-2-butenedioate (2:3) Table 4

(E)-2-butenedioate (1:1); (5) hydrochloric acid (1:1); (6) (E)-2-butenedioate (2:3)

(2) hydrochloric acid (1.2), (5) hydrochloric acid (1:1); (7) monohydrate; (8) hydrochloric acid (1:3) monohydrate
Table 6

(1) cyclohexylsulfanute (1:2); (2) hydrochloric acid (1:2); (9) hydrochloric acid (13) hydrate (21) ethanolate (2:1); (10) cyclohexylsulfamate (1:2) hydrate (1:2); (11) cyclohexylsulfamate (1:1); (12) hydroiodic acid (I: I); (13) hydrochloric acid (1:3) hydrate (2:3) 2-propanolate (2:1); (14) hydrochloric acid (1:3) hydrate (1:1) 2-propanolate (1:1); (15) hydrochloric acid (1:3) hydrate (2:3) 2-propanolate (1:1)
Table 7

(3) (E)-2-butenedioate (1:1)
C. Pharmacological Example
The ED50 values (mg/kg) in the test "Protection of Rats from Compound 48/80 induced
Lethality" for the compounds of formula (I) are listed in the Table below.

Compound No. ED50 (mg/kg)
1 2.5
3 2.5
17 0.04
18a 0.08
20 0.31
53 0.31
56a 2.5
58 2.5
62 0.63
64 0.31
79 0.04
80 0.63
D. Composition Examples
The following formulations exemplify typical pharmaceutical compositions suitable for
systemic or topical administration to warm-blooded animals in accordance with the
present invention.
"Active ingredient" (A.I.) as used throughout these examples relates to a compound of
formula (I), a prodrug, an addition salt, a N-oxide, a quaternary amine or a
stereochemically isomeric form thereof

Example D1 : Oral drops
500 g of the A.I. is dissolved in 0.5 1 of 2-hydroxypropanoic acid and 1.5 1 of the polyethylene glycol at 60~80°C. After cooling to 30~40°C there are added 35 1 of polyethylene glycol and the mixture is stirred well. Then there is added a solution of 1750 g of sodium saccharin in 2.5 I of purified water and while stirring there are added 2.5 1 of cocoa flavor and polyethylene glycol q.s. to a volume of 50 I, providing an oral drop solution comprising 10 mg/ml of the A.I. The resulting solution is filled into suitable containers.
Example D2: Oral solutions
9 g of methyl 4-hydroxybenzoate and 1 g of propyl 4-hydroxybenzoate are dissolved in 4 I of boiling purified water. In 3 1 of this solution are dissolved first 10 g of 2,3-dihydroxybutanedioic acid and thereafter 20 g of the A.I. The latter solution is combined with the remaining part of the former solution and 12 1 of 1,2,3-propanetriol and 3 1 of sorbitol 70% solution are added thereto. 40 g of sodium saccharin are dissolved in 0.5 1 of water and 2 ml of raspberry and 2 ml of gooseberry essence are added. The latter solution is combined with the former, water is added q.s. to a volume of 20 1 providing an oral solution comprising 5 mg of the A.I. per teaspoonful (5 ml). The resulting solution is filled in suitable containers.
Example D3 : Capsules
20 g of the A.I., 6 g sodium lauryl sulfate, 56 g starch, 56 g lactose, 0.8 g colloidal silicon dioxide, and 12 g magnesium stearate are vigorously stirred together. The resulting mixture is subsequently filled into 1000 suitable hardened gelatin capsules, each comprising 20 mg of the A.I..
Example P4 : Film-coated tablets Preparation of tablet core
A mixture of 100 g of the A.I., 570 g lactose and 200 g starch is mixed well and thereafter humidified with a solution of 5 g sodium dodecyl sulfate and 10 g polyvinyl¬pyrrolidone (Kollidon-K 90®) in about 200 ml of water. The wet powder mixture is sieved, dried and sieved again. Then there are added 100 g microcrystalline cellulose (Avicel®) and 15 g hydrogenated vegetable oil (Sterotex ®). The whole is mixed well and compressed into tablets, giving 10.000 tablets, each comprising 10 mg of the active ingredient. Coating
To a solution of 10 g methyl cellulose (Methocel 60 HG®) in 75 ml of denaturated ethanol there is added a solution of 5 g of ethyl cellulose (Ethocel 22 cps ®) in 150 ml of dichloromethane Then there are added 75 ml of dichloromethane and 2.5 ml

1,2,3-propanetriol. 10 g of polyethylene glycol is molten and dissolved in 75 ml of dichloromethane. The latter solution is added to the former and then there are added 2.5 g of magnesium octadecanoate, 5 g of polyvinylpyrrolidone and 30 ml of concen¬trated colour suspension (Opaspray K-1-2109®) and the whole is homogcnated. The tablet cores are coated with the thus obtained mixture in a coating apparatus.

WE CLAIM:
1. A spiro compound of formula

a prodrug as herein described, a N-oxide as herein described, an addition salt as herein described, a quaternary amine as herein described or a stereochemically isomeric form thereof
wherein
R1 is hydrogen, C1-6alkyl, halo, formyl, carboxyl, C1-
6alkyloxycarbonyl, C1-6alkyl-carbonyl, N(R3R4)C(=0)-,
N(R3R4)C(=0)N(R5)-, ethenyl substituted with carboxyl or C1-6alkyloxycarbonyl or C1-6alkyl substituted with hydroxy, carboxyl, C1-6alkyloxy, C1-6alkyloxycarbonyl, N(R3 R4)C(=0)-, C1-6alkylC(=0)N(R5)-, C1-6alkylS(=0) 2N(R5)-or N(R3 R4)C(=0)N(R5)-;
wherein each R3 and each R4 independently are hydrogen or C1-4alkyl;
R5 is hydrogen or hydroxy;
R2 is hydrogen, C1-6alkyl, hydroxyC1-6alkyl, C1-6alkyloxyC1-6alkyl, N(R3 R4)C(=Q)-, aryl or halo;

n is 1 or 2;
-A-B- represents a bivalent radical of formula
-Y-CH=CH- (a-1);
-CH=CH-Y- (a-2); or
-CH=CH-CH=CH- (a-3);
wherein each hydrogen atom in the radicals (a-1) to (a-3) may independently be replaced by R6 wherein R6 is selected from C1-6alkyl, halo, hydroxy, C1-6alkyloxy, ethenyl substituted with carboxyl or C1-6alkyloxycarbonyl, hydroxyC1-6alkyl, formyl, carboxyl and hydroxycarbonylC1-6alkyl; each Y independently is a bivalent radical of formula -O-, -S- or -NR7-; wherein R7is hydrogen, C1-6alkyl or C1-6alkylcarbonyl; Z is a bivalent radical of formula
-(CH2)p- (b-1), -CH2-C(=0)- (b-5), or
-CH=CH- (b-2), -CH2-C(=NOH)- (b-6),
-CH2-CHOH- (b-3),
- CH2-O- (b-4),
provided that the bivalent radicals (b-3), (b-4), (b-5) and (b-6) are connected to the nitrogen of the imidazole ring via their -CH2-moiety:
wherein p is 1, 2, 3 or 4;
L is hydrogen; C1-6alkyl; C1-6alkenyl; Ci-6alkylcarbonyl; C1-4alkyloxycarbonyl; C1-4alkyl substituted with one or more

substituents each independently selected from hydroxy, carboxyl, C1-4alkylox, C1-6alkyloxycarbonyl, aryl, aryloxy, cyano or R8HN-wherein R8 is hydrogen, C1-6alkyl, C1-6alkyloxycarbonyl, C1-6alkylcarbonyl; or
L represents a radical of formula
-Alk-Y-Het1 (c-1),
-Alk-NH-CO-Het2 (c-2) or
-Alk-Het3 (c-3) wherein
Alk represents C1-4 alkanediyl;
Y represents O, S or NH:
Het1, Het2 and Het3 each represent furanyl, tetrahydrofuranyl, thienyl, oxazolyl, thiazolyl or imidazolyl each optionally substituted with one or two C1-4 alkyl substituents, pyrrolyl or pyrazolyl optionally substituted with formyl, hydroxyC1-4alkyl, hydroxycarbonyl, C1-4alkyloxycarbonyl or with one or two C1-4alkyl substituents; thiadiazolyl or oxadiazolyl optionally substituted with amino or C1-4alkyl; pyridinyl, pyrimidinyl, pyrazinyl or pyridazinyl each optionally substituted with C1-4alkyl, C1-4 alkyloxy, amino, hydroxy or halo; and Het3 may also represent 4,5-dihydro-5-oxo-lH-tetrazolyl substituted with C1-4alkyl, 2-oxo-3-oxazolidinyl, 2-3-dihydro-2-oxo-lH-benzimidazol-l-yl or a radical of formula

A-Z represents S-CH=CH, S-CH2-CH2, S-CH2-CH2-CH2, CH=CH-CH=CH, or CH2-CH2-CH2-CH2;

atyl is phenyl or phenyl substituted with 1, 2 or 3 substituents each independently selected from halo, hydroxy, C1-4alky, polyhaloC1-4alkyl, cyano, aminocarbonyl, C1-4alkyloxy or polyhaloC1-4alkyloxy;
provided that when
L is H or benzyl;
Z is a bivalent radical of formula (b-1) with p being 1 or 2, or (b-2)
R1 is hydrogen, C1-6alkyl, halo, formyl, carboxyl, ethenyl
substituted with carboxyl or C1-6alkyloxycarbonyl, or Ci-ealkyl substituted with hydroxyl, carboxyl or C1-6alkyloxycarbonyl;
R2 is hydrogen, C1-6alkyl, hydroxy C1-6alkyl, aryl or halo; and
R6 is C1-6alkyl, halo, ethenyl substituted with carboxyl or C1-6alkyloxycarbonyl, hydroxy Ciealkyl, formyl, carboxyl or hydroxycarbonylC1-6alkyl;
then n is 2.
2. A compound as claimed in claim 1 wherein L is hydrogen, C1-6alkyl, C1-6alkylcarbonyl, C1-6alkycoxycarbonyl or C1-6alkyl substituted with hydroxy, carboxyl, C1-6alkyloxy or C1-6alkyloxycarbonyl.
3. A compound as claimed in claim 1 wherein L is C1-6alkyl substituted with aryl and C1-6alkyloxycarbonyl.

4. A compound as claimed in any one of the preceding claims wherein -A-B- is a bivalent radical of formula -CH=CH-CH=CH-(a-3) or -CH=CH-Y-(a-2).
5. A compound as claimed in any one of the preceding claims wherein Z is -(CH2) P- (b-1), -CH=CH- (b-2), or -CH2-O- (b-4).
6. A compound as claimed in claims 1, 2, 4 or 5 wherein L is hydrogen, Ciealkyl, hydroxyCi-ealkyl, carboxyCi-6alkyl, C1-6 alkyloxycarbonyl, or Ci-6alkyloxycarbonylCi-6alkyl.
7. A compound as claimed in any one of the preceding claims wherein R1 is hydroxyC1-6alkyl, formyl, C1-6alkyloxycarbonyl, C1-6alkyloxyC1-6alkyl, N(R3R4)C(=0)-, halo or hydrogen.
8. A compound as claimed in claim 1 wherein the compound is
5,6-dihydrospiro [11 H-imidazo [2, l-b][3]benzazepine-ll,4'-piperidine]-3-carboxamide dihydrochloride;
l'-butyl-5,6-dihydrospiro[imidazo[2, l-b][3]benzazepine-11-[ 11H] ,4'-piperidine];
6,1 l-dihydro-l'-methylspiro[5-H-imidazo[2, l-b][3]benzazepine-11,4'-pipendine]cyclohexylsulfamate(l :2);
6,ll-dihydrospiro[5-imidazo[2) l-b][3]benzazepine- 11, 4'-piperidine]-3-methanol) (E) -2-butenedioate (2:1);
3-chloro-6, 1 l-dihydrospir[5H-imidazo[2, l-b][3]benzazepine-11, 4>-piperidine] (E)-2-butenedioate (1:1);

6,1 l-dihydro-3-(methoxymethyl)spiro[5H-imidazo[2,1 -b][3]benzazepine- 11 ,4'- piperidine]. (E)-2-butenedioate (1:1);
6,11 -dihydro-1 '-(2-hydroxyethyl) spiro[5H-imidazo[2, 1 -b] [3]benzazepine-11 ^'-piperidinej-S-carboxamide;
6,11-dihydro-l'-methylspiro[5H-imidazo[2, l-b][3]benzazepine-1 l,4'-piperidine]-3-carboxamide monohydrate;
ethyl 3-(aminocarbonyl)-6, 11 -dihydro-a-phenylspiro[5-imidazo[2, l-b][3)-benzazepine-ll, 4'-piperidine]-l'-prapanoate monohydrochloride; 3-(aminocarbonyl)-6, ll-dihydrospiro[5H-imidazo[2, l-b][3]benzazepine-ll, 4'-piperidine]-r-carboxylate; spiro[ 1 OH-irnidazo[l ,2-a]thieno[3,2-d]azepine-10,4'-piperidine];
6, ll-dihydrospiro[5H-imidazo[2,l-b] [3]benzazepine- 11, 4'-piperidine]-2,3-dicarboxamide dihydrochloride monohydrate;
a prodrug, a N-oxide, an addition salt, a quaternary amine or a stereochemically isomeric form thereof.
A pharmaceutical composition comprising a pharmaceutically acceptable carrier, and as active ingredient a therapeutically effective amount of a compound as claimed in any one of claims 1 to 8.
A spiro compound of formula

a N-oxide, an addition salt, a quaternary amine or a stereochemically isomeric form thereof wherein P is a protective group and n, -A-B-, Z, R1 and R2 are claimed as in claim 1.
provided that 6,11 -dihydro-1 '-(phenylmethyl)-5H-spiro[imidazo[ l,2-b)[3]benzazepine-ll ,4-piperidine] and pharmaceutically acceptable addition salts thereof are not included.
11. A compound as claimed in claim 10 wherein P is benzyl.
12. A process of preparing a compound as claimed in claim 1, wherein it comprises
a) deprotecting an intermediate of formula (II), followed optionally by derivatizing either the piperidine moiety, or the imidazole moiety, or both the piperidine moiety and the imidazole moiety

with -A-B-, Z, L, R1 and R2, and n defined as in claim 1 and P being a protective group;
b) derivatizing an intermediate of formula (II) at the imidazole moiety, leading to the formation of an intermediate of formula (Il-a), followed by deprotecting the piperidine moiety, and followed optionally by derivatizing the piperidine moiety

c) by cyclizing an intermediate of formula (III) in the presence of an appropriate acid, resulting in a compound of formula (I-a)

with -A-B-, L, R1 and R2, and a defined as in claim 1;
and, if desired, converting compounds of formula (I) and (I-a) into each other following art-known transformations, and further, if desired, converting the compounds of formula (I), into a therapeutically active non-toxic acid addition salt by treatment with an acid, or into a therapeutically active non-toxic base addition salt by treatment with a base, or conversely, converting the acid addition salt form into the free base by treatment with alkali, or converting the base addition salt into the free acid by treatment with acid; and, if desired, preparing stereochemically isomeric forms or N-oxide forms thereof.
13. A process of preparing a compound as claimed in claim 10, wherein it comprises
a) cyclizing a compound of formula (XI) with an appropriate acid, leading to a compound of formula (II-k), followed optionally by derivatizing the imidazole moiety, leading to a compound of formula (II-a-I)

with -A-B-, R', R2, n and P defined as in claim 13, and Zi being a bivalent radical of formula -(CH2)p-, wherein p is 1,2,3 or 4.
b) by reacting a tricyclic moiety of formula (XIV) with a reagent of formula (XV) under an inert atmosphere in a reaction inert solvent in the presence of a suitable base, leading the a compound of formula (II-1), followed optionally by derivatizing the imidazole moiety leading to a compound of formula (II-a-2)

with -A-B-, R1, R2, n and P defined as in claim 13, Ws being a suitable leaving group, e.g. a halo, and Z2 being a bivalent radical of formula or -(CH2) p-, or CH2-O-, wherein p is 1, 2, 3 or 4.
Dated this 23rd day of April, 2001
(SHUKADEV KHURAIJAM)
OF REMFRY & SAGAR ATTORNEY FOR THE APPLICANTS

Documents:

in-pct-2001-00441-mum-cancelled page(17-1-2007).pdf

in-pct-2001-00441-mum-claim(granted)-(17-1-2007).doc

in-pct-2001-00441-mum-claim(granted)-(17-1-2007).pdf

in-pct-2001-00441-mum-correspondence(17-1-2007).pdf

in-pct-2001-00441-mum-correspondence(ipo)-(6-12-2006).pdf

in-pct-2001-00441-mum-form 1(23-4-2001).pdf

in-pct-2001-00441-mum-form 13(15-9-2006).pdf

in-pct-2001-00441-mum-form 13(4-7-2005).pdf

in-pct-2001-00441-mum-form 18(8-11-2005).pdf

in-pct-2001-00441-mum-form 1a(12-4-2006).pdf

in-pct-2001-00441-mum-form 1a(26-7-2007).pdf

in-pct-2001-00441-mum-form 2(granted)-(17-1-2007).doc

in-pct-2001-00441-mum-form 2(granted)-(17-1-2007).pdf

in-pct-2001-00441-mum-form 3(12-4-2006).pdf

in-pct-2001-00441-mum-form 3(24-4-2001).pdf

in-pct-2001-00441-mum-form 3(26-7-2007).pdf

in-pct-2001-00441-mum-form 5(24-4-2001).pdf

in-pct-2001-00441-mum-form-pct-ipea-409(24-12-2001).pdf

in-pct-2001-00441-mum-form-pct-isa-210(24-12-2001).pdf

in-pct-2001-00441-mum-petition under rule 137(12-4-2006).pdf

in-pct-2001-00441-mum-petition under rule 138(12-4-2006).pdf

in-pct-2001-00441-mum-power of authority(12-4-2006).pdf

in-pct-2001-00441-mum-power of authority(24-4-2001).pdf

in-pct-2001-00441-mum-power of authority(7-1-2007).pdf

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Patent Number

212018

Indian Patent Application Number

IN/PCT/2001/00441/MUM

PG Journal Number

04/2008

Publication Date

25-Jan-2008

Grant Date

13-Nov-2007

Date of Filing

23-Apr-2001

Name of Patentee

JANSSEN PHARMACEUTICA N.V.

Applicant Address

TURNHOUTSEWEG 30, BEERSE, B-2340, BELGIUM

Inventors:

#	Inventor's Name	Inventor's Address
1	JOSEPH ELISABETH LEENAERTS	TURNHOUTSEWEG 30, 2340 BEERSE, BELGIUM
2	FRANS EDUARD JANSSENS	C/O JANSSEN PHARMACEUTICA N.V. OF TURNHOUTSEWEG 30, 2340 BEERSE, BELGUM.

PCT International Classification Number

C07D 471/20

PCT International Application Number

PCT/EP99/10176

PCT International Filing date

1999-12-15

PCT Conventions:

#	PCT Application Number	Date of Convention	Priority Country
1	98204347.3	1998-12-19	EPO