Title of Invention

A 1-(1,2-DISUBSTITUTED PIPERIDINYL)-4-(FUSED IMIDAZOLE)-PIPERIDINE DERIVATIVES.

Abstract This invention concerns the compounds of formula the N-oxide forms, the pharmaceutically acceptable addition salts and the stereochemically isomeric forms thereof, wherein n is 0, 1 or 2; m is 1 or 2, provided that if m is 2, then n is 1; =Q is =O or =NR3; X is a covalent bond or-O-, -S-, -NR3-; R1 is AT1, Ar1C1-6 alkyl or di(Ar1) C1-6alkyl, wherein each C1-6alkyl group is optionally substituted; R2 is Ar2, Ar2C1-6aIkyl, Het or HetC1-6alkyl; R3 is hydrogen or C1-6alkyl; L is a piperidine derivative of formula (a-1) or a spiro piperidine derivative of formula (a-2); Ar1 is phenyl or substituted phenyl; Ar2 is naphtalenyl; phenyl or substituted phenyl; and Het is a monocyclic or bicyclic heterocycle; each monocyclic and bicyclic heterocycle may optionally be substituted on a carbon atom; as substance P antagonists; their preparation, compositions containing them and their use as a medicine.
Full Text This invention concerns novel l-(l,2-disubstituted piperidinyl)-4-(fused imidazole) piperidine derivatives having tachykinin antagonistic activity, in particular substance P antagonistic activity, and their preparation; it further relates to compositions comprising them, as well as their use as a medicine.
Substance P is a naturally occurring neuropeptide of the tachykinin family. There are ample studies showing that substance P and other tachykinins are involved in a variety of biological actions, and therefore, play an essential role in various disorders (Regoli et al., Pharmacological Reviews 46(4), 1994, p. 551-599, "Receptors and Antagonists for Substance P and Related Peptides"). The development of tachykinin antagonists has led to date to a series of peptide compounds of which might be anticipated that they are metabolically too labile to be employed as pharmaceutically active substances (Longmore J. et al., DN&P 8(1), February 1995, p. 5-23, "Neurokinin Receptors"). The present invention concerns nonpeptide tachykinin antagonists, in particular nonpeptide substance P antagonists, which in general are metabolically more stable, and hence, may be more appropriate as pharmaceutically active substances.
Several nonpeptide tachykinin antagonists are disclosed in the art. For instance, EP-0,532,456-A, published on March 17, 1993, discloses 1-acylpiperidine compounds, in particular 2-arylalkyl-l-arylcarbonyl-4-piperidinamine derivatives, and their use as substance P antagonists.
WO 92/06981, published on April 30, 1992, discloses 1 l-[4-substituted-(piperidinyl or piperidinylidene)]-imidazobenzazepines as agents useful in the treatment of asthma and other allergic diseases and in the treatment of inflammation. WO 92/22553, published on December 23, 1992, discloses 10-(piperidinyl or piperidinylidene)-imidazo[l,2-a](pyrrolo, thieno^and furano)[3,2-d]azepine derivatives having antiallergic activity. WO-94/13680, published on June 23, 1994, discloses 10-(piperidinyl or piperidinylidene)-imidazo[l,2-a](pyrrolo, thieno and furano)[2,3-d]azepine derivatives having antiallergic activity. Further, WO 95/02600, published on January 26, 1995, discloses other piperidinyl- or piperidinylidene substituted imidazoazepine derivatives also having antiallergic activity.
The present compounds differ from the art compounds in that they invariably contain a 4-substituted-piperidine moiety in the 4-position of a 2-substituted-(piperidine- or

-2-
homopiperidine) group or in the 3-position of a 2-substituted-pyrrolidine group, and by their favourable farmacological properties.
Hence, the present invention concerns novel compounds of formula

the N-oxide forms, the pharmaceutically acceptable addition salts and the stereochemically
isomeric forms thereof, wherein
n is 0, 1 or 2;
m is 1 or 2, provided that if rn is 2, then nis1;
=Q is=Oor=NR3;
X is a covalent bond or a bivalent radical of formula -O-, -S-, -NR3-;
R1 is Ar1, Ar'Ci.galkyI or di(Ar1)Ci.6alkyl, wherein each C1.6alkyl group is
optionally substituted with hydroxy, C1-4alkyloxy, oxo or a ketalized oxo substituent of formula -O-CH2-CH2-O- or -O-CH2-CH2-CH2-O-;
R2 is Ar2, Ar2C1_6alkyl, Het or HetCi-ealkyl;
R3 is hydrogen or Ci-galkyl;
L is a radical of formula

wherein the dotted line is an optional bond;
20 each -A-B- independently is a bivalent radical of formula
-Y-CR7=CH- (b-1);
-CH=CR7-Y- (b-2);
-CH=CH-CH==CH- (b-3);
-CH=CR7-CH=CH- (b-4);
25 -CH=CH-CR7=CH- (b-5); or
-CH=CH-CH==CR7- (b-6);
wherein each Y independently is a bivalent radical of formula -O-, -S- or -NR8-;
each R7 independently is C1-galkyl; halo; ethenyl substituted with

-3-
carboxyl or Ci-galkyloxycarbonyl; hydroxyC1-6alkyl; formyl;
carboxyl or hydroxycarbonylCi-ealkyl;
R8 is hydrogen, Ci_6alkyl or Cj^alkylcarbonyl;
each Z independently is Z1 or Z2;
wherein Z1 is a bivalent radical of formula -CH2-, -CH2-CH2- or -CH=CH-; provided that when L is a radical of formula (a-1) and the dotted line is an extra bond, then Z1 is other than -CH2-; Z2 is a bivalent radical of formula -CH2-CHOH-, -CH2-O-, -
CH2-C(==O)- or -CH2-C(=NOH)-, provided that the -CH2- moiety of said bivalent radicals is connected to the nitrogen of the imidazole ring; each R4 independently is hydrogen; Ci-ealkyl; halo; ethenyl substituted with
carboxyl or Ci_6alkyloxycarbonyl; Ci.6alkyl substituted with carboxyl or C^alkyloxycarbonyl; hydroxyCi-salkyi; formyl or carboxyl; each R5 independently is hydrogen, Ci-ealkyl, hydroxyCi.galkyl, Ar1 or halo;
or R4 and R5 taken together may form a bivalent radical of formula -
CH=CH-CH=CH- or -CH2-CH2-CH2-CH2; each R6 is hydrogen, Ci.salkyi or Ar^i^alkyl;
Ar1 is phenyl; phenyl substituted with 1, 2 or 3 substituents each independently selected from halo, C1-4alkyl, haloCi.4alkyl, cyano, aminocarbonyl, Ci-4alkyloxy or haloC1-4alkyloxy;
Ar2 is naphtalenyl; phenyl; phenyl substituted with 1, 2 or 3 substituents each independently selected from hydroxy, halo, cyano, nitro, amino, mono- or di(C1_4alkyl)amino, C1-4alkyl, haloC1-4alkyl, C1-4alkyloxy, haloCj^alkyloxy, carboxyl, Ci.4alkyloxycarbonyl, aminocarbonyl and mono- or di(Ci_4alkyl)-aminocarbonyl; and
Het is a monocyclic heterocycle selected from pyrrolyl, pyrazolyl, imidazolyl, furanyl, thienyl, oxazolyl, isoxazolyl, thiazolyl, isothiazolyl, pyridinyl, pyrimidinyl, pyrazinyl and pyridazinyl; or a bicyclic heterocycle selected from quinolinyl, quinoxalinyl, indolyl, benzimidazolyl, benzoxazolyl, benzisoxazolyl, benzothiazolyl, benzisothiazolyl, benzofuranyl and benzothienyl; each monocyclic and bicyclic heterocycle may optionally be substituted on a carbon atom by 1 or 2 substituents selected from halo, C1-4alkyl or mono-, di- or
tri(halo)methyl. The heterocycles in the definition of Het are preferably connected to the rest of the

_4-molecule, i.e. X, -C(=Q)- or C1-6alkyl, by a carbon atom.
As used in the foregoing definitions and hereinafter, halo is generic to fluoro, chloro, bromo and iodo; C1-4alkyl defines straight and branched chain saturated hydrocarbon radicals having from 1 to 4 carbon atoms such as, for example, methyl, ethyl, propyl, butyl, 1-methylethyl, 2-methylpropyI and the like; Ci_6alkyl is meant to include Ci_4alkyl and the higher homologues thereof having 5 to 6 carbon atoms such as, for example, pentyl, 2-methylbutyI, hexyl, 2-methylpentyl and the like; Ci^alkanediyl defines bivalent straight and branched chain saturated hydrocarbon radicals having from 1 to 4 carbon atoms such as, for example, methylene, 1,2-ethanediyl, 1,3-propanediyl, 1,4-butanediyl, and the like; C^alkanediyl is meant to include Ci_4alkanediyl and the higher homologues thereof having form 5 to 6 carbon atoms such jag, for example, 1,5-pentanediyI, 1,6-hexanediy not claim?
As used in the foregoing definitions and hereinafter, haloC1-4alkyl is defined as mono- or polyhalosubstituted C1-4alkyl, in particular C1-4alkyl substituted with 1 to 6 halogen atoms, more in particular difluoro- or trifluoromethyl.
The pharmaceutically acceptable addition salts as mentioned hereinabove are meant to comprise the therapeutically active non-toxic acid addition salt forms which the compounds of formula (I) are able to form. Said salts can conveniently be obtained by treating the base form of the compounds of formula (I) with appropriate acids such as, 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, malonic, succinic, maleic, fumaric, malic, tartaric, citric, methanesulfonic, ethanesulfonic, benzenesulfonic, p-toluenesulfonic, cyclamic, salicylic, p-aminosalicylic, pamoic and the like acids.
The pharmaceutically acceptable addition salts as mentioned hereinabove are also meant to comprise the therapeutic ally active non-toxic base, in particular, a metal or amine addition salt forms which the compounds of formula (I) are able to form. Said salts can conveniently be obtained by treating the compounds of formula (I) containing acidic hydrogen atoms with appropriate organic and inorganic bases such as, for example, the ammonium salts, the alkali and earth alkaline metal salts, e.g. the lithium, sodium, potassium, magnesium, calcium salts arid the like, salts with organic bases, e.g. the benzathine, N-methyl-D-glucamineJiydrabamine salts, and salts with amino acids such as, for example, arginine, Iysine not claim

-5-
Conversely said salt forms can be converted by treatment with an appropriate base or acid into the free acid or base form.
The term addition salt as used hereinabove also comprises the solvates which the compounds of formula (I) as well as thesaltsthereof, are able to form. Such solvates are for example hydrates, alcoholates
For isolation and purification purposes, it is also possible to use pharmaceutically unacceptable salts. Only the pharmaceutically acceptable, non-toxic salts are used therapeutically and those salts are therefore preferred.
The term "stereochemically isomeric forms" as used hereinbefore defines all the possible isomeric as well as conformational forms which the compounds of formula (I) may possess. Unless otherwise mentioned or indicated, the chemical designation of compounds denotes the mixture, more in particular the racemic mixture, of all possible stereochemically and conformationally isomeric forms, said mixtures containing all diastereomers, enantiomers and/or conformers of the basic molecular structure. More in particular, stereogenic centers may have the R- or S-configuration. For the compounds having two or more stereogenic centers, the relative stereodescriptors R* and S* are used in accordance with the Chemical Abstracts rules (Chemical Substance Name Selection Manual (CA), 1982 Edition, Vol. Ill, Chapter 20). Substituents on bivalent cyclic saturated radicals may have either the cis~ or tamr-configuration. More in particular, the substituents R1 and L are substituted on. the nitrogen containing ringsystem in a cis or trans configuration. For compounds of formula (I) wherein L is a radical of formula (a-1), the substituents R6, provided it is other than hydrogen, and the fused imidazolyl moiety, provided it is connected to the piperidine ring by a single bond, may be substituted on the piperidine ring in a cis or trans configuration. The radicals >C=NR3 and C3_galkenyl may have the E- or Z-configuration. All stereochemically isomeric forms of the compounds of formula (I) both in pure form or mixtures thereof are intended to be embraced within the scope of the present invention.
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. For instance, compounds of formula (I) wherein X is -NH- and =Q is =O may exist in their corresponding tautomeric form.
The A^-oxide forms of the compounds of formula (I) are meant to comprise those compounds of formula (I) wherein one or several nitrogen atoms are oxidized to the

-6-so-called AT-oxide, particularly those iV-oxides wherein a piperidine-nitrogen is iV-oxidized.
Whenever used hereinafter, the term "compounds of formula (I)" is meant to also include their N-oxide forms, their pharmaceutically acceptable addition salts, and their stereo-chemically isomeric forms.
A special group of compounds are those compounds of formula (I) wherein Het is a mono-cyclic heterocycle selected from pyrrolyl, pyrazolyl, imidazolyl, furanyl, thienyl, oxazolyl, isoxazolyl, thiazolyl, isothiazolyl, pyridinyl, pyrimidinyl, pyrazinyl and pyridazinyl; or a bicyclic heterocycle selected from quinolinyl, benzimidazolyl, benzoxazolyl,
benzisoxazolyl, benzothiazolyl, benzisothiazolyl, benzofuranyl and benzothienyl; each monocyclic and bicyclic heterocycle may optionally be substituted on a carbon atom by 1 or 2 substituents selected from halo, Ci^alkyl or mono-, di- or tri(halo)methyl.
A first group of interesting compounds consists of those compounds of formula (I) wherein one or more of the following restrictions apply :
a) R1 is A^Ci^alkyl; or
b) R2 is furanyl; naphtalenyl; quinolinyl; indolyl; pyrazinyl; benzofuranyl; benzothienyl;
benzothiazolyl; isoxazolyl; quinoxalinyl; each of said monocyclic or bicyclic
heterocycle may optionally be substituted on a carbon atom by 1 or 2 substituents
selected from halo, Ci_4alkyl or mono-, di- or tri(halo)methyl; or R2 is phenylC^alkyl; phenyl or phenyl substituted with 1, 2 or 3 substituents each independently selected from Ci_4alkyl, Ci,4alkyloxy, Cj^alkyloxycarbonyl and haloCi.4alkyl, in particular, selected from methyl and trifluoromethyl; or
c) n is 1; or
d) m is 1; or
e) -Q is =O; or
f) X is a covalent bond or a bivalent radical of formula -O- or -NR3-.
A second group of interesting compounds consists of those compounds of formula (I)
wherein L is a radical of formula (a-1), suitably, a radical of formula (a-1) wherein -A-B-is a radical of formula (b-1), (b-2) or (b-3); Z is Z1; R4 is hydrogen, formyl or hydroxy-Ci^alkyl; R5is hydrogen; or R4 and R5 taken together form a bivalent radical of formula -
CH=CH-CH=CH-; R^is hydrogen.
A third group of interesting compounds consists of those compounds of formula (I) wherein L is a radical of formula (a-2), suitably, a radical of formula (a-2) wherein -A-B-is a radical of formula (b-3); Z is Z1; R4, R5 and R6 are hydrogen.

-7-
A fourth group of interesting compounds consists of those compounds of formula (I)
wherein L is a radical of formula (a-1) wherein -A-B- is a radical of formula (b-1), (b-2),(b-3), (b-5) or (b-6); Z is Z1 orZ2; R4 is hydrogen, halo, C].6alkyl, formyl,
Ci^alkyloxycarbonyl or hydroxyCi_6alkyl; R5is hydrogen, C]_6alkyl or hydroxyCj.6alkyl;
or R4 and R5 taken together form a bivalent radical of formula -CH=CH-CH=CH-; R6 is hydrogen.
Of special interest are those compounds of formula (I) wherein R1 is A^Ci-ealkyl, R2 is phenyl substituted with 2 substituents selected from methyl or trifluoromethyl, X is a covalent bond and =Q is =O.
Further of special interest are those compounds of formula (I) wherein n and m are 1.
A particular group of compounds consists of those compounds of formula (I) wherein R1 is phenylmethyl; R2is phenyl substituted with 2 substituents selected from methyl or trifluoromethyl; n, m are 1; X is a covalent bond; and =Q is =O.
Another particular group of compounds consists of those compounds of formula (I) wherein L is a radical of formula (a-1) wherein
the dotted line is an optional bond; -A-B- is a radical of formula (b-1) wherein Y is -S-; and R7 is hydrogen; or -A-B- is a radical of formula (b-2) wherein Y is -S- or -NR8-; and R7 is hydrogen; or -A-B- is a radical of formula (b-3); Z is Z1 or Z2 wherein Z1 is a bivalent radical of formula -CH2- or -CH2-CH2-, provided that when the dotted line is an extra bond, then Z1 is other than -CH2-; and Z2 is a bivalent radical of formula -CH2-O-, -CH2CHOH- or CH2-C(=O)-, provided that the -CH2- moiety of said bivalent radicals is connected to the nitrogen of the imidazole ring; R4 is hydrogen, formyl or hydroxymethyl; R5 is hydrogen; or R4 and R5 taken together form a bivalent radical of formula -CH=CH-CH=CH-; R6 is hydrogen.
Yet another particular group of compounds consists of those compounds of formula (I) wherein L is a radical of formula (a-2) wherein -A-B- is a radical of formula (b-3); Z is a bivalent radical of formula -CH2-CH2-; R4, R5 and R6 are hydrogen.
Preferred compounds are those compounds of formula (I) wherein R1 is phenylmethyl; R2 is phenyl substituted with 2 substituents selected from methyl or trifluoromethyl; n, m are 1; X is a covalent bond;and =Q is =O.
More preferred compounds are those particular groups of compounds wherein R1 is phenylmethyl; R2 is phenyl substituted with 2 substituents selected from methyl or

-8-trifluoromethyl; n, m are 1; X is a covalent bond; and =Q is =O.
Most preferred are
l-[3,5-bis(trifluoromethyl)benzoyl]-4-(5,6-dihydrospiro[lli/-imidazo[2,l-b][3]-benzazepine-ll,4'-piperidin3-l-yl)-2-(phenylmethyl)piperidine;
l-tS^-bisCtrifluoromethyDbenzoylJ^-^-CS.e^.lO-tetrahydro-imidazofl.a-aJthieno-[2,3-d]azepin-10-ylidene)-l-piperidinyI]-2-(phenylmethyl)piperidine; l-[3,5-bis(trifIuoromethyl)benzoyl]-4-[4-(5,6,7,10-tetrahydro-7-methylimidazo-[l,2-a]pyrrolo[3,2-d]azepin-10-yIidene)-l-piperidinyI]-2-(phenylmethyI)piperidine; and l-[3,5-bis(trifluoromethyl)benzoyI]-4-[4-(3-formyl-5,6-dihydro-ll//-imidazo-[2,1 -b] [3]benzazepin-11 -ylidene)-1 -piperidinyl]-2-(phenylmethyl)piperidine; 4-[4~(5,6,7,10-tetrahydro-7-methylimidazo[ 1,2-a]pyrrolo[3,2~d]azepin-10-ylidene)-1 -piperidinyl]-l-(3,5-dimethylbenzoyl)-2-(phenylmethyl)piperidine; and 4-[4-(5,6-dihydro-6-oxo-10ff-imida2o[l,2-a]thieno[3,2-d]azepin-10-ylidene)-l-piperidinyl]-l-(3,5-dimethylbenzoyl)-2-(pheny]methyl)piperidine; the stereoisomeric forms and the pharmaceutically acceptable acid addition salts thereof.
The compounds of formula (I) can be prepared by reductively A^-alkylating an intermediate of formula (III) with an intermediate of formula (II). Said reductive N-alkylation may be performed in a reaction-inert solvent such as, for example, dichloromethane, ethanol, toluene or a mixture thereof, and in the presence of a reducing agent such as, for example, a borohydride, e.g. sodium borohydride, sodium cyanoborohydride or triacetoxy borohydride. In case a borohydride is used as a reducing agent, it may be convenient to use a catalyst such as, for example, titanium(IV) isopropylate as described in J. Org. Chem, 1990, 55, 2552-2554. Using said catalyst may also result in an improved cisltrans ratio in favour of the trans isomer. It may also be convenient to use hydrogen as a reducing agent in combination with a suitable catalyst such as, for example, palladium-on-charcoal or platinum-on-charcoal. In case hydrogen is used as reducing agent, it may be advantageous to add a dehydrating agent to the reaction mixture such as, for example, aluminium fer/-butoxide. In order to prevent the undesired further hydrogenation of certain functional groups in the reactants and the reaction products, it may also be advantageous to add an appropriate catalyst-poison to the reaction mixture, e.g., thiophene or quinoline-sulphur. Stirring and optionally elevated temperatures and/or pressure may enhance the rate of the reaction.


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In this and the following preparations, the reaction products may be isolated from the reaction medium and, if necessary, further purified according to methodologies generally known in the art such as, for example, extraction, crystallization, trituration and chromatography.
The compounds of formula (I) can also be prepared by reacting an intermediate of formula (IV) wherein W1 is an appropriate leaving group such as, for example, a halogen, e.g. chloro or bromo, or a sulfonyloxy leaving group, e.g. methanesulfonyloxy or benzene-sulfonyloxy, with an intermediate of formula (V). The reaction can be performed in a reaction-inert solvent such as, for example, a chlorinated hydrocarbon, e.g. dichloro-methane, an alcohol, e.g. ethanol, or a ketone, e.g. methyl isobutylketone, and in the presence of a suitable base such as, for example, sodium carbonate, sodium hydrogen carbonate or triethylamine. Stirring may enhance the rate of the reaction. The reaction may conveniently be carried at a temperature ranging between RT and reflux temperature.

The compounds of formula (I) may also be converted into each other following art-known transformations. For instance, compounds of formula (I) wherein R4, R5 or both R4 and R5 are hydroxyC].6alkyl may be oxidized to the corresponding aldehyde or carboxylic
acid by reaction with suitable reagents such as, for example, manganese(IV) oxide, respectively, silver nitrate.
The compounds of formula (I) may also be converted to the corresponding iV-oxide forms following art-known procedures for converting a trivalent nitrogen into its W-oxide form. Said TV-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, benzenecarboperoxoic acid or halo substituted benzenecarboperoxoic acid, e.g. 3-chlorobenzenecarboperoxoic acid,

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peroxoalkanoic acids, e.g. peroxoacetic acid, alkylhydroperoxides, e.g. tbutyl hydro-peroxide. Suitable solvents are, for example, water, lower alkanols, 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 starting materials and some of the intermediates are known compounds and are commercially available or may be prepared according to conventional reaction procedures generally known in the art. For example, intermediates of formula (III) wherein L is a radical of formula (a-1) wherein Z is Z1, said intermediates being represented by formula (III-a-1-1), may be prepared as described in EP-0,518,435-A, EP-0,518,434-A and EP-0,672,047-A.
The intermediates of formula (III) wherein L is a radical of formula (a-1) wherein Z is Z2, said intermediates being represented by formula (III-a-1-2), may in general be prepared by debenzylating a compound of formula

following art known procedures, e.g. catalytic hydrogenation.
In particular, the intermediates of formula (III-a-1-2) wherein Z2 is a radical of formula -CH2-C(=O)-, said intermediates being represented by formula (III-a-l-2-a), can be
prepared by reacting an intermediate of formula (VI) in the presence of an acid, e.g. trifluoromethanesulfonic acid, and the like.


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The intermediates of formula (III-a-l-2-a) can also be prepared by hydrolizing an intermediate of formula (VII) in the presence of an acid, e.g. hydrobromic acid, Erifluoroacetic acid and the like.

The intermediates of formula (Ill-a-1 -2) wherein Z2 is a radical of formula -CH2-CHOH-,
said intermediates being represented by the formula (III-a-l-2-b), can be prepared by reacting the compounds of formula (III-a-l-2-a) in the presence of a reducing reagent, e.g. sodium borohydride, in a reaction-inert solvent, e.g. methanol and the like.

The intermediates of formula (III-a-1 -2) wherein Z2 is a radical of formula -CH2-C(=NOH>, said intermediates being represented by the formula (III-a-l-2-c), can be
prepared by reacting the compounds of formula (III-a-l-2-a) with hydroxylamine or a salt, e.g. the hydrochloride salt thereof, in a reaction-inert solvent, e.g. pyridine and the like.

Intermediates of formula (III) wherein L is a radical of formula (a-2) wherein Z is Z1, said intermediates being represented by formula (III-a-2-1), may be prepared by cyclizing an intermediate of formula (VIII) with a suitable reagent such as, for example, trifluoroacetic

-12-
aci, and subsequently, debenzylating the thus formed intermediate following art known procedures, e.g. catalytic hydrogenation.

Intermediates of formula (II) may be prepared by condensing an intermediate of formula (IV) with an intermediate of formula (IX) analogous to the procedure described in EP-0,532,456-A.

Ways to prepare intermediates of formula (IX) are also described in EP-0,532,456-A. However, intermediates of formula (IX) wherein R1 is optionally substituted A^Ci.ealkyl or di(Ar1)Ci_6alkyl, said R1 being represented by -CH(Rla)2 and said intermediates being represented by formula (IX-a), may also be prepared as depicted in scheme 1.
Scheme 1


-13-
In scheme 1, the intermediates of formula (X-b) may be prepared by reacting an intermediate of formula (X-a) with an aldehyde or a ketone of formula (XI). The C^alkyl-carbamate moiety in the intermediates of formula (X-b) may be converted into a fused oxazolone which in turn may be reduced to an intermediate of formula (X-d). Said intermediate (X-d) may in turn be deprotected, thus forming an intermediate of formula (IX-a). Subsequently, intermediates of formula (IX-a) may be reacted with an intermediate of formula (IV) to prepare intermediates of formula (II) wherein R1 is defined as -CH(Rla)2, said intermediates being represented by formula (Il-a). The reactions performed in scheme 1 may all be conducted following conventional methods that are generally known in the art.
Intermediates of formula (V) may suitably be prepared by reacting an intermediate of formula (IX-1), being a protected intermediate of formula (IX) with a protecting group P such as, for example, a Ci.6alkyloxycarbonyl group, with an intermediate of formula (III)
according to the previously described reductive 7V-alkylation procedure, and subsequently deprotecting the thus formed intermediate.


The ketalized intermediate of formula (X-c) may be transformed to the corresponding ketone of formula (X-e) which subsequently may be reductively aminated with a
In particular, intermediates of formula (V) wherein R1 is -CH(Rla)2, said intermediates being represented by formula (V-a), may be prepared as is depicted in scheme 2.

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pyrrolidine, piperidine- or homopiperidine derivative of formula (III). The thus obtained intermediate may then be reduced with a suitable reducing agent to an intermediate of formula (V-a).
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 subsequently 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 starting materials, provided that the reaction occurs stereospecifically. 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.
The compounds of formula (I) have valuable pharmacological properties in that they interact with tachykinin receptors and they antagonize tachykinin-induced effects, especially substance P-induced effects, both in vivo and in vitro and are thus of use in the treatment of tachykinin-mediated diseases, and in particular in substance P-mediated diseases.
Tachykinins, also referred to as neurokinins, are a family of peptides among which substance P (SP), neurokinin A (NKA), neurokinin B (NKB) and neuropeptide K (NPK) may be identified. They are naturally occurring in mammals, including human beings, and are distributed throughout the central and peripheral nervous system, where they act as neurotransmitters or neuromodulators. Their actions are mediated through several subtypes of receptors, such as, for example, NK], NK2 and NK3 receptors. Substance P displays highest affinity for NKj receptors, whereas NKA preferentially binds to NK2 receptors and NKB preferentially binds to NK3 receptors. However, the selectivity of these tachykinins is relatively poor and under physiological conditions the

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action of any of these tachykinins might be mediated by activation of more than one receptor type.
Substance P and other neurokinins are involved in a variety of biological actions such as pain transmission (nociception), neurogenic inflammation, smooth muscle contraction, plasma protein extravasation, vasodilation, secretion, mast cell degranulation, and also in activation of the immune system. A number of diseases are deemed to be engendered by activation of neurokinin receptors, in particular the NK] receptor, by excessive
release of substance P and other neurokinins in particular cells such as cells in the neuronal plexi of the gastrointestinal tract, unmyelinated primary sensory afferent neurons, sympathetic and parasympathetic neurons and nonneuronal cell types (DN&P 8(1), February 1995, p. 5-23, "Neurokinin Receptors" by Longmore J. et al.; Pharmacological Reviews 46(4), 1994, p. 551-599, "Receptors and Antagonists for Substance P and Related Peptides" by Regoli et al.).
The compounds of the present invention are potent inhibitors of neurokinin-mediated effects, in particular those mediated via the NKi receptor, and may therefore be
described as tachykinin antagonists, especially as substance P antagonists, as indicated in vitro by the antagonism of substance P-induced relaxation of pig coronary arteries which is described hereinafter. The binding affinity of the present compounds for the human, guinea-pig and gerbil neurokinin receptors may be determined in vitro in a receptor binding test using 3H-substance P as radioligand. The subject compounds also show substance-P antagonistic activity in vivo as may be evidenced by, for instance, the antagonism of substance P-induced plasma extravasation in guinea-pigs, or the antagonism of drug-induced emesis in ferrets (Watson et al., Br. J. Pharmacol. 115, 84-94, 1995).
In view of their capability to antagonize the actions of tachykinins by blocking the tachykinin receptors, and in particular antagonizing the actions of substance P by blocking the NKj receptor, the subject compounds are useful in the prophylactic and
therapeutic treatment of tachy kin in-mediated diseases such as, for example, - pain, in particular traumatic pain such as postoperative pain; traumatic avulsion pain such as brachial plexus; chronic pain such as arthritic pain such as occurring in osteo-, rheumatoid or psoriatic arthritis; neuropathic pain such as post-herpetic neuralgia, trigeminal neuralgia, segmental or intercostal neuralgia, fibromyalgia, causalgia, peripheral neuropathy, diabetic neuropathy, chemotherapy-induced neuropathy, AIDS-related neuropathy, occipital neuralgia, geniculate neuralgia, glossopharyngeal neuralgia, reflex sympathetic dystrophy, phantom limb pain;

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various forms of headache such as migraine, acute or chronic tension headache, temperomandibular pain, maxillary sinus pain, cluster headache; odontalgia; cancer pain; pain of visceral origin; gastrointestinal pain; nerve entrapment pain; sport's injury pain; dysmennorrhoea; menstrual pain; meningitis; arachnoiditis; musculoskeletal pain; low back pain e.g. spinal stenosis; prolapsed disc; sciatica; angina; ankylosing spondyolitis; gout; burns; scar pain; itch; and thalamic pain such as post stroke thalamic pain;
- respiratory and inflammatory diseases, in particular inflammation in asthma,
influenza, chronic bronchitis and rheumatoid arthritis; inflammatory diseases of the
gastrointestinal tract such as Crohn's disease, ulcerative colitis, inflammatory bowel
disease and non-steroidal anti-inflammatory drug induced damage; inflammatory
diseases of the skin such as herpes and eczema; inflammatory diseases of the bladder
such as cystitis and urge incontinence; and eye and dental inflammation;
- emesis, i.e. nausea, retching and vomiting, including acute emesis, delayed emesis
and anticipatory emesis, no matter how emesis is induced, for example, emesis may
be induced by drugs such as cancer chemotherapeutic agents such as alkylating
agents, e.g. cyclophosphamide, carmustine, lomustine and chlorambucil; cytotoxic
antibiotics, e.g. dactinomycin, doxorubicin, mitomycin-C and bleomycin; anti-
metabolites, e.g. cytarabine, methotrexate and 5-fluorouracil; vinca alkaloids, e.g.
etoposide, vinblastine and vincristine; and others such as cisplatin, dacarbazine,
procarbazine and hydroxyurea; and combinations thereof; radiation sickness;
radiation therapy, e.g. irradiation of the thorax or abdomen, such as in the treatment
of cancer; poisons; toxins such as toxins caused by metabolic disorders or by
infection, e.g. gastritis, or released during bacterial or viral gastrointestinal infection;
pregnancy; vestibular disorders, such as motion sickness, vertigo, dizziness and
Meniere's disease; post-operative sickness; gastrointestinal obstruction; reduced
gastrointestinal motility; visceral pain, e.g. myocardial infarction or peritonitis;
migraine; increased intercranial pressure; decreased intercranial pressure (e.g.
altitude sickness); opioid analgesics, such as morphine; and gastro-oesophageal
reflux disease, acid indigestion, over-indulgence of food or drink, acid stomach, sour
stomach, waterbrash/regurgitation, heartburn, such as episodic heartburn, nocturnal
heartburn, and meal-induced heartburn and dyspepsia;
- central nervous system disorders, in particular psychoses such as schizophrenia,
mania, dementia or other cognitive disorders e.g. Alzheimer's disease; anxiety;
AIDS-related dementia; diabetic neuropathy; multiple sclerosis; depression;
Parkinson's disease; and dependence on drugs or substances of abuse;

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- allergic disorders, in particular allergic disorders of the skin such as urticaria, and
allergic disorders of the airways such as rhinitis;
- gastrointestinal disorders, such as irritable bowel syndrome;
- skin disorders, such as psoriasis, pruritis and sunburn;
- vasospastic diseases, such as angina, vascular headache and Reynaud's disease;
- cerebral ischaemia, such as cerebral vasospasm following subarachnoid
haemorrhage
- stroke, epilepsie, head trauma, spinal cord trauma and ischemic neuronal damage;
- fibrosing and collagen diseases, such as scleroderma and eosinophilic fascioliasis;
- disorders related to immune enhancement or suppression, such as systemic lupus
erythematosus;
- rheumatic diseases, such as fibrositis;
- neoplastic disorders;
- cell proliferation; and
- cough.
The compounds of the present invention have a favourable metabolic stability and exhibit good oral availability. They also have an advantageous onset and duration of action. The compounds of formula (I) also have the ability to penetrate the central nervous system as may be demonstrated in vivo by their inhibitory effect on the change in behaviour induced by intracerebroventricular-applied substance P in the gerbil.
In view of the utility of the compounds of formula (I), there is provided a method of treating warm-blooded animals, including humans, suffering from tachykinin-mediated diseases as mentioned hereinabove, in particular, pain, emesis or asthma. Said method comprises the systemic administration of an effective tachykinin antagonizing amount of a compound of formula (I), a N-oxide form, a pharmaceutically acceptable addition salt or a possible stereoisomeric form thereof, to warm-blooded animals, including humans. Hence, the use of a compound of formula (I) as a medicine is provided, and in particular a medicine to treat pain, emesis or asthma.
For ease of administration, the subject compounds may be formulated into various pharmaceutical forms for administration purposes. To prepare the pharmaceutical compositions of this invention, a therapeutically effective amount of the particular compound, optionally in addition salt form, as the active ingredient is combined in intimate admixture with a pharmaceutically acceptable carrier, which may take a wide variety of forms depending on the form of preparation desired for administration. These pharmaceutical compositions are desirably in unitary dosage form suitable,

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preferably, for administration orally, rectally, percutaneously, or by parenteral injection. For example, in preparing the compositions in oral dosage form, any of the usual pharmaceutical media may be employed, such as, for example, water, glycols, oils, alcohols and the like in the case of oral liquid preparations such as suspensions, syrups, elixirs and solutions; or solid carriers such as starches, sugars, kaolin, lubricants, binders, disintegrating agents and the like in the case of powders, pills, capsules and tablets. Because of their ease in administration, tablets and capsules represent the most advantageous oral dosage unit form, in which case solid pharmaceutical carriers are obviously employed. For parenteral compositions, the carrier will usually comprise sterile water, at least in large part, though other ingredients, for example, to aid solubility, may be included. Injectable solutions, for example, may be prepared in which the carrier comprises saline solution, glucose solution or a mixture of saline and glucose solution. Injectable solutions containing compounds of formula (I) may be formulated in an oil for prolonged action. Appropriate oils for this purpose are, for example, peanut oil, sesame oil, cottonseed oil, corn oil, soy bean oil, synthetic glycerol esters of long chain fatty acids and mixtures of these and other oils. Injectable suspensions may also be prepared in which case 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, optionally 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 or as an ointment. Acid or base addition salts of compounds of formula (I) due to their increased water solubility over the corresponding base or acid form, are obviously more suitable in the preparation of aqueous compositions.
In order to enhance the solubility and/or the stability of the compounds of formula (I) in pharmaceutical compositions, it can be advantageous to employ a-, p- or y-cyclodextrins or their derivatives, in particular hydroxyalkyl substituted cyclodextrins, e.g. 2-hydroxypropyl-p-cyclodextrin. Also co-solvents such as alcohols may improve the solubility and/or the stability of the compounds of formula (I) in pharmaceutical compositions.
It is especially advantageous to formulate the aforementioned pharmaceutical compositions in dosage unit form for ease of administration and uniformity of dosage. Dosage

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unit 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 pharmaceutical carrier. Examples of such dosage unit forms are tablets (including scored or coated tablets), capsules, pills, powder packets, wafers, injectable solutions or suspensions, teaspoonfuls, tablespoonfuls and the like, and segregated multiples thereof.
Those of skill in the treatment of tachykinin mediated diseases could determine the effective therapeutic daily amount from the test results presented hereinafter. An effective therapeutic daily amount would be from about 0.001 mg/kg to about 40 mg/kg body weight, more preferably from about 0.01 mg/kg to about 5 mg/kg body weight. It may be appropriate to administer the therapeutically effective dose once daily or as two, three, four or more sub-doses at appropriate intervals throughout the day. Said sub-doses may be formulated as unit dosage forms, for example, containing 0.05 mg to 500 mg, and in particular, 0.5 mg to 50 mg of active ingredient per unit dosage form.
The exact dosage and frequency of administration depends on the particular compound of formula (I) used, the particular condition being treated, the severity of the condition being treated, the age, weight and general physical condition of the particular patient as well as other medication the patient may be taking, as is well known to those skilled in the art. Furthermore, it is evident that said effective daily amount may be lowered or increased depending on the response of the treated patient and/or depending on the evaluation of the physician prescribing the compounds of the instant invention. The effective daily amount ranges mentioned hereinabove are therefore only guidelines.
The following examples are intended to illustrate and not to limit the scope of the present invention.
Experimental part
Hereinafter, "THF" means tetrahydrofuran, "RT" means room temperature. Of some compounds of formula (I) the absolute stereochemical configuration was not experimentally determined. In those cases the stereochemically isomeric form which was first isolated is designated as "A" and the second as "B", without further reference to the actual stereochemical configuration.

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A. Preparation of the intermediate compounds Example Al
a) A mixture of N-(l-methylethyl)-2-propanamine (16.7 g) in THF (600ml) was stirred at -
70°C under N2 flow. Butyllithium in hexane (63 ml; 2.5 M) was added portionwise and the
temperature was allowed to rise to -40°C and stirring was continued for 15 minutes. The mixture was cooled to -70°C and a suspension of l-(phenylmethyl)benzimidazole (31.3 g) in THF was added dropwise. After stirring for 1 hour at -70°C, 4-(ethoxy-carbonyl)-l-piperidinecarboxylic acid 1,1-dimethylethyl ester (42.5 g) was added dropwise and stirring at -70°C was continued for 1.5 hours. The temperature was allowed to rise to RT and the mixture was decomposed with water, and further extracted with CH2CI2. The organic layer
was separated, dried, filtered and the solvent evaporated. The residue was crystallized from acetonitrile, yielding 54 g (85.8%) of (1,1-dimethylethyl) 4-[[l-(phenylmethyl)-l//-benzimidazol-2-yl]carbonyl]-l-piperidinecarboxylate (interm. 1; mp. 121.5°C).
b) A mixture of intermediate (1) (25.2 g) and hydrochloric acid in 2-propanol (60 ml) in
methanol (400 ml) was stirred and refluxed for 1 hour. The solvent was evaporated,
crystallized from 2-propanol and recrystallized from ethanol, yielding 20.7 g (97%) of
[l-(phenylmethyl)-l//-benzimidazol-2-yl](4-piperJdinyI)methanonemonohydrochloride
(interm. 2; mp. 197.7°C).
c) Intermediate (2) (10.7 g) was dissolved in H2O and alkalized with K2CO3. The free
base was extracted with CH2C12- The organic layer was dried, filtered and the solvent
evaporated. The residue was dissolved in methanol (100 ml), sodium borohydride (4 g)
was added and the mixture was stirred during 1 hour at RT. The solvent was evaporated,
then dissolved in H2O/CH2CI2 and extracted with CH2CI2. The organic layer was dried,
filtered and the solvent evaporated. The concentrate was boiled in CH3CN, yielding 8.1 g
(84%) of l-(phenylmethyl)-a-(4-piperidinyl)-li/-benzimidazole-2-methanol (interm. 3);
d) Intermediate (3) (6.4 g) was stirred overnight in trifluoromethanesulfonic acid (25 ml)
under N2-flow. The reaction mixture was poured out into ice, alkalized with NaOH and
extracted with CH2CI2. The organic layer was dried, filtered and the solvent evaporated.
The residue was purified by column chromatography over silica gel (eIuent:CH2Cl2 /
(CH3OH/NH3) 90/10). The pure fractions were collected and evaporated, yielding 5.4 g of
6,1 l-dihydro-6-(4-piperidinyl)benzimidazo[l,2-b]isoquinoline (interm. 4a). A sample (1.4
g) was converted into the cyclohexanesulfamic acid salt (1:2) in CH3CN/C2H5OH,
yielding 2.84 g of 6,n-dihydro-6-(4-piperidinyl)benzimidazo[l,2-b]isoquinoline
cyclohexylsulfamate (1:2) (interm. 4; mp. 205.8°C).
Example A2
a) A mixture of N-(l-methylethyl)-2-propanamine (26.3 g) in THF (800ml) was stirred
under N2 and the mixture was cooled to -70°C. Butyllithium in hexane (104 ml; 2.5 M)

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was added portionwise and the mixture was brought to -40°C and stirred for 15 minutes. l-(2-phenylethyI)-l#-imidazole (34.4 g) dissolved in THF was added dropwise at -70°C and the mixture was stirred for 1 hour. l-(PhenyImethyl)-4-piperidinone (45.4 g) dissolved in THF was added dropwise at -70°C and the mixture was stirred for 1 hour. The mixture was brought to RT and stirred at RT for 18 hours. The mixture was decomposed with water and the solvent evaporated. The residue was taken up in water, extracted with CH2CI2, dried and the solvent 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 evaporated. A sample (1.5 g) was converted into the (Z)-2-butenedioic acid salt (1:2) in 2-propanone, yielding 1.92 g of 4-[l-(2-phenyl-ethyl)-lH-imidazol-2~yI]-Hphenylmethyl)-4-piperidinoI (Z)-2-butenedioate (1:2) (interm. 5; mp. 156.4°C).
b) A mixture of the free base of intermediate (5) (36 g) in trifluoroacetic acid (200 ml)
was stirred at 70°C for 48 hours. The mixture was cooled, poured into ice water, alkalized
with NaOH (50%), extracted with CH2CI2, dried, filtered and the solvent evaporated. The
residue was purified on a glass filter over silica gel (eluent: CH2CI2/ CH3OH 95/5). The
pure fractions were collected and the solvent evaporated. The residue was converted into
the (E)-2-butenedioic acid salt (1:2) in ethanol, yielding 38.7 g (67%) of 6,11-dihydro-l1-
(phenylmethyl)-5H-spiro[imidazo[l,2-b][3]benzazepine-ll,4'-piperidine] (E)-2-butene-
dioate(l:2) (interm. 6; mp. 214.3°C).
c) A mixture of the free base of intermediate (6) (6.9 g) in methanol (150 ml) was
hydrogenated with palladium on activated carbon (10%; 2 g) as a catalyst at 50 °C for
18 hours. After uptake of hydrogen, the catalyst was filtered and the filtrate was
evaporated, yielding 5,6-dihydrospiro[imidazo[l,2-b][3]benzazepine-l 1[1 IH],
4'-piperidine] (interm. 7a). A sample was converted into the hydrochloric acid salt (1:1) in
CH3CN, yielding 5,6-dihydrospiro[imidazo[l,2-b][3]benzazepine-l 1[1 IH], 4r-piperidine] .
monohydrochloride (interm. 7; mp. 21$.5°C).
Example A3
a) A mixture of 1,1-dimethylethyl l,4-dioxo-8-azaspiro[4.5]-8-carboxylate (0.1 mol) in diethylether (150ml) and N.N.N'.N'-tetramethyl-ethylenediamine (33.2ml) was cooled on a 2-propanol/CO2 bath under a N2 flow. Sec. buthyllithium (1.3 M; 0.11 mol) was added dropwise at a temperature below -60°C and the mixture was stirred for 3 hours. A mixture of 3,5-(difluoro)benzaldehyde (0.12 mol) in diethylether (75ml) was added dropwise. The mixture was stirred slowly overnight and allowed to warm to RT. The mixture was decomposed with water and separated into its layers. The aqueous layer was extracted with CH3C12. The combined organic layer was dried, filtered and the

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solvent was evaporated, yielding 38.5g of (±)-l,l-dimethylethyI 7-[(3,4-difIuoro-phenyl)hydroxymemyl]-l,4-dioxa-8-azaspiro[4.5]-decane-8-carboxylate (interm. 8).
b) A mixture of intermediate 8 (0.1 mol) and 2-methyl-2-propanol, potassium salt (lg)
in toluene (200ml) was stirred and refluxed for 2 hours. The solvent was evaporated and the residue was taken up in CHjC^/water. The organic layer was separated, dried,
filtered and the solvent was evaporated. The residue was purified by column chromato-graphy over silica gel (eluent: CH2CI2/CH3OH 98/2). The pure fractions were collected
and the solvent was evaporated. The residue was suspended in petroleum ether and the precipitate was filtered off and dried, yielding lOg (32%) of (±)-r-(3,4-difluorophenyl)-tetrahydrospiro[l,3-dioxolan-2J7l(l'H)-[3H]-oxazolo[3,4-a]pyridin]-3-one(interm. 9).
c) A mixture of intermediate 9 (0.032 mol) in methanol (250ml) was hydrogenated at
50°C with palladium on activated carbon (10%; 2g) as a catalyst. After uptake of
hydrogen, the catalyst was filtered off and the filtrate was evaporated, yielding 9g
(100%) of (±)-2-[(3,4-difluorophenyl)methyl]-l,4-dioxa-8-azaspiro[4.5]decane
(interm. 10).
d) A mixture of intermediate 10 (0.032 mol) in HC1, (6N; 90ml) was stirred at 75°C,
then cooled. CH2CI2 was added and the mixture was alkalized with NaOH at a
temperature below 20°C. The organic layer was separated, dried, filtered and the solvent was evaporated. The residue was dried, yielding 7.2g of (±)-2-[(3,4-difluoro-phenyl)methyl]-4-piperidinone (interm. 11). In a similar way as described in procedure d), (±)-2-(phenyImethyl)-4-piperidinone
(interm. 12) was prepared.
e) A mixture of intermediate 12 in CH2Cl2, 3,5-dimethylbenzoyl chloride (7.4 g) and
triethylamine (11 ml) was stirred overnight at RT. Dilute NaOH was added. The organic layer was separated, dried, filtered and the solvent evaporated. The residue was crystallized from diisopropylether yielding 7.44 g (58%) of (±)-l-(3,5)-dimethylbenzoyl)-2-(phenylmethyl)-4-piperidinone (interm. 13). In a similar way as described in procedure e), (±)-l-[3,5-bis(trifluoromethyl)benzoyl]-2-[(3,4-difluorophenyl)methyl]-4-piperidinone (interm. 14) was prepared.
Example A4
A mixture of (±)-8-tert-butoxycarbonyI-7-(phenylmethyl)-l,4-dioxa-8-azaspiro[4.5]-decane (33.34 g) in HC1, 6 N (250 ml) was stirred at 70°C for 1 hour 30 minutes. The mixture was cooled, CH2CI2 (100 ml) was added and the mixture was alkalized with
NaOH while cooling till 25°C. The organic layer was separated and the aqueous layer was extracted with CH2CI2. Triethylamine (20.2 g), followed by 3,5-bis(trifluoro-methyl)benzoyl chloride (27.7 g) dissolved in a little CH2CI2 were added and the

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mixture was stirred for 2 hours. Water was added and the layers were separated. The organic layer was dried, filtered and evaporated. The residue was crystallized from DIPE, the precipitate was filtered off and dried, yielding a first crop. The mother layer was evaporated and the residue was crystallized from diisopropylether. The precipitate was filtered off and dried, yielding a second crop. The two solid fractions were put together and taken up in water and CH2CI2. NaOH was added and the mixture was extracted. The organic layer was dried, filtered off and evaporated, yielding 16.14 g
(38%)(±)-l-[3,5-bis-(trifluoromethyl)benzoyI]-2-(phenylmethyl)-4-piperidinone (interm. 15, mp. 102.5 °C).
B. Preparation of the final compounds Example B1
A mixture of (±)- l-(3,5-dimethyIbenzoyI)-2-(phenylmethyl)-4-piperidinone (2.5 g) and 6,ll-dihydro-ll-(4-piperidinylidene)-5H-imidazo[2,l-b][3]benzazepine (2.1 g) in methanol (150 ml) and a solution of thiophene (4%; 1 ml) was hydrogenated at 50°C overnight with palladium on activated carbon (10%; 2 g) as a catalyst. After uptake of hydrogen, the catalyst was filtered off and the filtrate was evaporated. The residue was purified by column chromatography over silica gel (eluent: CH2CI2/ (CH3OH/ NH3) 98/2
to 95/5). The desired fraction was collected, the solvent evaporated, yielding 0.54 g (12.3%) of (±)-cw-4-[4-(5,6-dihydro-l l//-imidazo[2,1-b][3]benzazepin-11 -ylidene)-1 -piperidinyl]-l-(315-dimethylbenzoyl)-2-(phenylmethyl)piperidine (comp. 1; mp. 138.7°C).
Example B2
a) The free base of intermediate (4) (3 g) was added to (±)-l-[3,5-bis(trifluoromethyl)-
benzoyl]-2-(phenylmethyl)-4-piperidinone (4.3 g) in CH2CI2 (40 ml). Titanium(IV)-
isopropoxide (3.41 g) was added and the mixture was stirred for 3 hours at RT. Ethanol (15 ml) and sodium cyanoborohydride (0.62 g) were added and the resulting reaction mixture was stirred overnight at RT. Water (5 ml) was added and the mixture was filtered over dicalite and the filtrate was evaporated. The residue was partitioned between water and CH2CI2. The organic layer was separated and the aqueous phase was extracted with CH2CI2. The separated organic layer was dried, filtered, and the solvent was evaporated. The residue was purified by HPLC (eluent: (0.5% ammoniumacetate in H2O)/CH3OH 30/70), yielding two desired fractions. A first fraction yielded 0.63 g (9%) (±)-cw-l-[3,5-bis(trifluoromethyl)benzoyl]-4-[4-(6,11 -dihydrobenzimidazo[ 1,2-b]isoquinolin-6-yl)-l -piperidinyl]-2-phenylmethyl)piperidine. (comp. 14; mp. 132.2°C). A second fraction yielded 0.32 g (5%) of (±)-rran^-l-[3,5-bis(trifluoromethyl)benzoyl]-4-[4-(6,ll-dihydro-benzimidazo[l,2-b]isoquinolin-6-yl)-l-piperidinyl]-2-phenylmethyl)piperidine(comp. 15; mp. 138.1°C).

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b) A mixture of intermediate 8 (0.02 mol) and 5,6-dihydrospiro[llH-imidazo[2,l-b]-[3]benzazepine-l l,4'-piperidine] (0.02 mol) in 2-propanol (20ml) was stirred at RT. Titanium(IV)isopropoxide (0.024 mol) was added. The mixture was stirred at 40°C for 3 hours and then cooled to RT. Ethanol (140ml) and sodiumborohydride (0.2 mol) were added. The mixture was stirred at FT overnight. Water was added, the mixture was filtered over celite and the filtrate was evaporated. The residue was taken up in water and CHjClj, and the mixture was separated into its layers. The aqueous layer was extracted with CH2C12. The combined organic layer was dried, filtered and the solvent was evaporated. The residue was purified by HPLC over silica gel (eluent: CH^yC^OH 98/2 to 95/5). Two pure fractions were collected and their solvents were evaporated, yielding 1.41g (13%) of (±)-cis-4-(:5,6-dihydrospiro[ll#-imidazo[2,l-b][3]benzazepine-1 l,4'-piperidin]-l-yl)-l-(3,5-dimethylbenzoyl)-2-(phenylmethyl)piperidine (comp. 119) and 2.36g (21%) of (±)-trans-4-(5,6-dihydrospiro[l l//-imidazo[2,l-b][3]benzazepine-1 l,4'-piperidin3-l-yl)-l-(3,5-dimethylbenzoyl)-2-(phenylmethyl)piperidine (comp. 120).
Example B3
Sodium triacetoxyborohydride (8.5 g) and acetic acid (2.4 g) were added dropwise
to a mixture of (±)-l-[3)5-bis(trifluoromethyl)benzoyl]-2-(phenylmethyl)-4-piperidinone
(4.3 g) and 5,6,7,10-tetrahydro-7-methyI-10-(4-piperidinyIidene)imidazo[l,2-a]pyrrolo-
[3,2-d]azepine (2.7 g) in 1,2-dichloroethane (100ml) and the mixture was stirred at RT
overnight. Water and K2CO3 (5 g) were added and the layers were separated. The
aqueous layer was extracted with CH2CI2. The combined organic layers were dried,
filtered and the solvent evaporated. The residue was purified by HPLC over silica gel (eluent: CH2CI2/CH3OH 96/4 to 85/15). The pure fractions were collected and
evaporated, yielding 1.04 g (15%) of fraction 1 and 0.26 g (4%)of (±)-rran^-l-[3,5-bis-(trifluoromethyl)benzoyl]-4-[4-(5,6,7,10-tetrahydro-7-methylimidazo[l,2-a]pyrrolo[3,2-d]azepin-10-ylidene)-l-piperidinyl]-2-(phenylmethyl)piperidine (comp. 2; mp. 141.5°C). Fraction 1 was repurified by HPLC over NH2-Kromasil (eluent: 100% CH2CI2). The pure
fractions were collected and the solvent was evaporated, yielding 0.75 g (11%) of (±)-cw-l-[3,5-bis(trifluoromethyl)benzoyl3-4-[4-(5,6,7T10-tetrahydro-7-methylimidazo[l,2-a]-pyrrolo[3,2-d]azepin-10-ylidene)-1 -piperidinyl]-2-(phenylmethyl)piperidine (comp. 3; mp. 133.0°C).
Example B4
A mixture of (±)-c^-l-[3,5-bis(trifluoromethyl)benzoyl]-4-[4-[5,6-dihydro-3-(hydroxy-methyl)-1 l//-imidazo[2,1 -b] [3]benzazepin-11 -y lidene]-1-piperidinyl]-2-(phenylmethyI)-piperidine (4.5 g) and manganese dioxide (20 g) in CHCI3 (200 ml) was stirred and
refluxed for 1 hour. The mixture was filtered warm over dicalite and the filtrate was

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evaporated. The residue was purified over silica gel on a glass filter (eluent: CH2CI2/ CH3OH 95/5). The pure fractions were collected and the solvent was evaporated. The residue was purified by HPLC (eluent: CH2CI2/CH3OH 100/0 to 95/5). The pure fractions were collected and the solvent was evaporated, yielding 3.1 g (70%) of (±)-m-l-[3,5-bis-
(trifiuoromethyl)benzoyI]-4-[4-(3-formyl-5,6-dihydro-llH-imidazo[2tl-b][3]benzazepin-ll-yHdene)-l-piperidinyI]-2-(phenylmethyl)piperidine(comp. 11; mp. 125.8°C).
Example B5
A mixture of compound 11 (0.00345 mol), sodium cyanide (0.0189 mol) and manganese dioxide (0.069 mol) in methanol (50ml) was stirred at RT. Acetic acid (1.2ml) was added dropwise. The mixture was stirred and refluxed overnight, then cooled and filtered over dicalite. The filtrate was evaporated. The residue was taken up in water/CH2Cl2. K2CO3 (2g) was added and the mixture was separated into its layers. The aqueous layer was extracted with CH2C12. The combined organic layer was dried, filtered and the solvent was evaporated. The residue was purified by HPLC over silica gel (eluent: CH2CyCH3OH 97/3;). The pure fractions were collected and the solvent was evaporated, yielding 2g (79%).of(±)-methyl cis-1 l-[l-[l-[3,5-bis(trifluoromethyl)benzoyl]-2-(phenylmethyl)-4-piperidinyl]-4-piperidinylidene]-6,ll-dihydro-5H-imidazo[2,l-b][3]benzazepine-3-carboxylate (comp. 17).
Example B6
3,5-di(trifluoromethyl)benzoyl chloride (0.003 mol) and then triethylamine (0.0045 mol) were added dropwise to a mixture of (±)-trans-6-[l-[2-[(3,4-dichloro-phenyl)-methyI]-4-piperidinyl]-4-piperidinyl]-ll,12-dihydro-6H-benzimidazo[2,l-b]-[3]benzazepine (0.003 mol) in CH2C12 (25ml). The mixture was stirred at RT overnight, washed with water and separated into its layers. The organic layer was dried, filtered and the solvent was evaporated. The residue was purified over silica gel on a glass filter (eluent: CH2CI2/CH3OH 98/2 to 96/4). The pure fractions were collected and the solvent was evaporated. The residue was dried, yielding 1.23g (51%) of (±)-trans-l-[3,5-bis(trifluoromethy!)benzoyl]-2-[(3,4-dichlorophenyl)methyl]-4-[4-(ll,12-dihydro-6H-benzimidazo[2,l-b][3]benzazepin-6-yl)-l-piperidinyl]piperidine (comp. 63).
Example B7
(±)-trans-6,l 1-dihydro-l l-[l-[2-(phenylmethyl)-4-piperidinyl ] -4-piperidinyIidene]-5#-imidazo[2,l-b][3jbenzazepine (0.00023 mol) was added to l/f-indole-5-carboxylic acid (± 0.080 g) and lH-benzotriazole-1-ol (0.060 g) in CH2C12 (3 ml). The mixture was

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stirred and cooled on an ice-bath, under N2 flow. Triethylamine (0.5 ml) was added dropwise. A solution of (CH3)2-N-(CH2)3-N=N-CH2-CH3 (0.080 g) in CH2CI2 (5 ml) was added dropwise and the reaction mixture was allowed to warm to RT, under N2. The reaction mixture was stirred overnight. The solvent was evaporated and the residue was purified by HPLC (eluent gradient: (0.5% ammoniumacetate in H2O)/CH3OH/ CH3CN 70/15/15 upgrading over 0/50/50 to 0/0/100). The desired fractions were collected and the solvent was evaporated, yielding 0.040 g of (±)-rra/u-A^-(2,6-di-methyIphenyl)-4-[2-(phenylmethyl)-4-piperidinyl]-1 -piperazineacetamide (comp. 81).
The following tables list compounds of formula (I) as prepared according to one of the above examples (Ex. No.).
Table 1


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& d.b. means double bond and s.b. means single bond
Table 2

& d.b. means double bond and s.b. means single bond



Table 3
5 Table 4

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Co.No Ex. No R2 X physical data
94 B6 2-benzothienyl direct bond (±)-cis
95 B6 l-phenylethyl direct bond (±)-cis
96 B7 6-benzothiazolyl direct bond (±)-cis
97 B6 5-methyl-3-isoxazolyl direct bond (±)-trans
98 B6 2-naphthalenyl direct bond (±)-trans
99 B6 l-phenylethyl direct bond (±)-trans
100 B6 3,5-di(trifluoromethyl)phenyl NH (±)-trans
101 B7 3 -methy lbenzofuran-2-y 1 direct bond (±)-trans
102 B7 6-benzothiazolyl direct bond (±)-trans
103 B7 3,4-dichlorophenyl direct bond {±)-trans
Table 5


Co.No Ex. No R9 -Z-* -A-B- physical data
104 B2b CH3 CH2-O -CH=CH-CH=CH- d.b. (±)-(cis + trans)
105 B2b CF3 CH2-CH(OH)- -CH=CH-S- d.b. (±)-A
106 B4 CF3 CH2-C(=O)- -CH=CH-S- d.b. (±)-cis
107 B4 CF3 CH2-C(=O)- -CH=CH-S- d.b. (±)-trans
108 B2b CH3 CH2 -CH=CH-CH=CH- s.b. (±)-cis
109 B2b CH3 CH2 -CH=CH-CH=CH- s.b. (±)-trans
110 B2b CH3 CH2-CH(OH)- -CH=CH-S- d.b. (±)-B
111 B4 CH3 CH2-C(=O)- -CH=CH-S- d.b. (±)-cis
112 B4 CH3 CH2-C(=O)- -CH=CH-S- d.b. (±)-trans
113 B2b CF CH2-O -CH=CH-CH=CH- d.b. (±)~cis
114 B2b CF3 CH2-0 -CH=CH-CH=CH- d.b. (±)-trans
115 B2b CF3 CH2 -CH=CH-CH=CH- s.b. (±)-cis
116 B2b CR CH, -CH=CH-CH=CH- s.b. (±)-trans
* the -CH2- group is always connected to the nitrogen of the imidazole moiety 5 & d.b. means double bond and s.b. means single bond

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Table 6


Co.No Ex. No R9 physical data 117 B2a CF3 (±)-cis 118 B2a CF3 (±)-tmns 119 B2b CH3 (±)-cis 120 B2b CH, (±)-trans
C. Pharmacological examples
Example C.I : Antagonism of substance P induced relaxation of the pig coronary arteries Segments of coronary arteries taken from pigs (killed by injection of an overdose of sodium pentobarbital) were inverted and mounted for recording of isometric tension in organ baths (volume 20 ml) with the endothelium at the outside. The preparations were bathed in Krebs - Henseleit solution. The solution was kept at 37 °C and gassed with a mixture of O2 / CO2 (95/5). After stabilisation of the preparations, prostaglandin F2a (10"
5 M) was administered to induce a contraction. This was repeated until contractile responses became stable. Then prostaglandin F2ot was again administered and substance P
(3xl0~10 M and 10~9 M cumulatively) was added. Substance P induced endothelium dependent relaxations. After washing away the agonists, a known concentration of a compound of formula (I) was added. After an incubation period of 30 minutes, prostaglandin F2a (10~5 M) and the same concentrations of substance P as described
above were again administered in the presence of the compound to be tested. Relaxations caused by substance P were expressed as relaxations under control conditions, and percentage inhibition (% inhibition) of the response to 10"" M substance-P was taken as a measure of the antagonistic activity of the compound to be tested. The results for the compounds of the present invention at a certain test concentration are listed in table 7.

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Table 7
Comp. Concentration % Comp. Concentration % No. test compound inhibition No. test compound inhibition
1 3 x 1O8 52.3 57 3 x 10-9 667 2 3x10-8 96.5 58 3 x 10"9 91.5 3 3 x 10-9 37.3 59 3 x 10'9 76.5 4 3 x 10-8 97.0 60 3 x 10"9 89.9 5 3xlO~9 100.0 61 3xlO"9 7.5 6 3 x 10-8 93.9 62 3 x 10*9 49.0 7 3xlO"9 83.1 63 3 x 10"9 61.4 8 3 x 10-9 82.3 64 3 x 10'9 26.4 9 3x10-8 IOO.O 65 3xlO"9 27.3 10 3x10-8 17.9 66 3xlO-9 56.6 11 3xlO"9 96.1 67 3xlO-9 64.4 12 3xlO-8 93.2 68 3 x 10'9 93.1 13 3xlO"9 74.2 69 3 x 10"9 8 14 3x10-9 56.6 70 3 x 10"9 31.2 15 3x10-8 95.4 71 3 x 10'9 53.1 16 3 x 10-9 98.9 72 3 x 10'9 97.4 17 3x10-9 35.3 73 3 x 10-9 2.8 18 3x10-9 39.8 74 3x10-9 8.6 19 3xlO-9 78.1 75 3 x 10"9 13.7 20 3 x 10-9 9.5 77 3 x 10"9 3.2 22 3 x 10"9 83.2 78 3 x 10"9 7.5 23 3xlO'9 13.4 80 3 x 10"9 10.9 24 3xlO"9 38.3 81 3 x 10"9 2.2 25 3 x 10-9 ioO.O 84 3 x 10~9 2.4 26 3x10-9 25.6 85 3 x 10-9 1.8 27 3x10-9 5.1 89 3 x 109 1.1 28 3xlO-9 37.4 91 3 x 10"9 9.2 29 3x10-9 8.1 92 3 x 10'9 6.7 30 3x10-9 15.3 93 3 x 109 3.1 31 3xlO"9 82.7 94 3 x 10'9 8.2 32 3xlO-9 71.6 96 3 x 10"9 17.3 34 3xlO-9 43.5 97 3 x 109 5.8 35 3 x lO-9 27.7 98 3 x 10"9 23.2 36 3xlO-9 23.7 99 3x10-9 i8.2

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Comp. Concentration % Comp. Concentration % No. test compound inhibition No. test compound inhibition
37 3xlO-9 81.9 100 3 x 10~9 13.9 38 3x 10"9 27.1 101 3x 10'9 11.8 39 3 x lO"9 42.9 102 3 x 10'9 17 40 3 x 10"9 8.4 103 3 x 10"9 8.3 41 3 x 10-9 40.6 104 3 x 10'9 83.0 43 3xlO"9 16 106 3xlO"9 92.3 44 3 x lO"9 63.9 107 3 x 10"9 96.3 45 3 x lO'9 7.9 108 3 x 10-9 2.6 46 3 x 10"9 54.3 109 3 x 10'9 13.5 48 3 x 10-9 59.7 111 3 x 10~9 22.6 49 3xlO"9 52.5 112 3 x 10"9 66.7 50 3xlO-9 25 113 3xlO~9 87.9 51 3 x 10"9 86.3 114 3 x 10"9 100.0 52 3 x 10"9 77.8 115 3 x 1O"9 60.2 53 3xlO"9 44.4 116 3 x 10"9 69.6 54 3xlO'9 69.8 119 3 x 10'9 9.3 56 3xlO"9 9.5 120 3xlQ-9 7.7
Example C.2 : Antagonism of substance P induced plasma extravasation in guinea-pigs Plasma extravasation was induced by injection of substance P (2 mg/kg) in the femoral artery of female guinea-pigs. Evans Blue dye (30 mg/kg) was injected simultaneously. The test compound or solvent was administered subcutaneous (s.c.) or orally (p.o.) 1 hour prior to substance P injection. 10 minutes after challenge, the animals were checked for blue colouring (a direct measure for plasma extravasation) of the nose, the forepaws, and the conjunctiva. 30 minutes after challenge, the animals were sacrificed by CO2 gas inhalation and checked for blue colouring of the trachea and the urinary bladder. Doses which actively inhibit substance P-induced plasma extravasation are defined as thoses doses at which only 1/3 or less of the total surface area of the nose, forepaws, conjunctiva, trachea or urinary bladder are coloured blue by an intensive extravasation. Table 8 lists the lowest active doses (LAD) in mg/kg for the tested compounds.

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D, Composition examples
"Active ingredient" (A.I.) as used throughout these examples relates to a compound of formula (I) a pharmaceutically acceptable addition salt, a stereochemically isomeric form thereof or a yV-oxide form thereof.
Example D. 1 : ORAL SOLUTION
Methyl 4-hydroxybenzoate (9 g) and propyl 4-hydroxybenzoate (1 g) were dissolved in boiling purified water (4 I). In 3 1 of this solution were dissolved first 2,3-dihydroxy-butanedioic acid (10 g) and thereafter A.I (20 g). The latter solution was combined with the remaining part of the former solution and 1,2,3-propanetriol (12 1) and sorbitol 70% solution (3 1) were added thereto. Sodium saccharin (40 g) were dissolved in water (500 ml) and raspberry (2 ml) and gooseberry essence (2 ml) were added. The latter solution was combined with the former, water was added q.s. to a volume of 201 providing an oral solution comprising 5 mg of the active ingredient per teaspoonful (5 ml). The resulting solution was filled in suitable containers.
Example D.2 : FILM-COATED TABLETS
Preparation of tablet, core
A mixture of A.I. (100 g), lactose (570 g) and starch (200 g) was mixed well and thereafter humidified with a solution of sodium dodecyl sulfate (5 g) and polyvinylpyrrolidone (10 g) in water (200 ml). The wet powder mixture was sieved, dried and sieved again. Then there was added microcrystalline cellulose (100 g) and hydrogenated vegetable oil (15 g). The whole was mixed well and compressed into tablets, giving 10.000 tablets, each containing 10 mg of the active ingredient. Coating

-36-
To a solution of methyl cellulose (10 g) in denaturated ethanol (75 ml) there was added a solution of ethyl cellulose (5 g) in CH2C12 (150 ml). Then there were added CH2C12 (75 ml) and 1,2,3-propanetriol (25 ml). Polyethylene glycol (10 g) was molten and dissolved in CH2C12 (75 ml). The latter solution was added to the former and then there were added agnesium octadecanoate (2.5 g), polyvinylpyrrolidone (5 g) and concentrated colour suspension (30 ml) and the whole was homogenated. The tablet cores were coated with the thus obtained mixture in a coating apparatus.
Example P.3 : INJECT ABLE SOLUTION
Methyl 4-hydroxybenzoate (1.8 g) and propyl 4-hydroxybenzoate (0.2 g) were dissolved in boiling water (500 ml) for injection. After cooling to about 50°C there were added while stirring lactic acid (4 g), propylene glycol (0.05 g) and the A.I, (4 g). The solution was cooled to RT and supplemented with water for injection q.s. ad 11, giving a solution comprising 4 mg/ml of A.I.. The solution was sterilized by filtration and filled in sterile containers.

-37-
I. A compound of formula

an N-oxide form, a pharmaceutically acceptable addition salt or a stereochemically isomeric
form thereof, wherein
n is I;
m is I;
=Q is =O;
X is a covalent bond or a bivalent radical of formula -O- or -NR-*-;
R1 isAr1C1-6alkyI;
R2 is Ar2, Ar2C 1-6alkyl or Het ;
R3 is hydrogen ;
L is a radical of formula

wherein the dotted line is an optional bond:
each -A-B- independently is a bivalent radical of formula
-Y-CR7=CH- (b-1);
-CH=CR7-Y- (b-2);
-CH=CH-CH=CH- (b-3),
-CH^CH-CR7=CH- (b-5); or
-CH=CH-CH=CR7- (b-6);
wherein each Y independently is a bivalent radical of formula -S- or -NR"-: each R7 independently is C|.(,a!kyl or halo, or
R7 i> hydrogen m case -A-B- is a radical of formula (b-1 ) or (b--).
R8 isC|.fvilkyl :
each Z indcpcndcnily is "/) or Z~.

38
wherein Z1 is a bivalent radical of formula -CH2- or -CH2-CH2- ; provided
that when L is a radical of formula (a-1) and the dotted line is an extra bond, thenZ1 is other than -CH2-;
Z2 is a bivalent radical of formula -CH2-CHOH-, -CH2-O- or -CH2-C(=O)-, provided that the -CH2- moiety of said bivalent
radicals is connected to the nitrogen of the imidazole ring; each R^ independently is hydrogen, Cj-^alkyl, halo, hydroxyC|_6alkyl, formyl,
Cj^alkyloxycarbonyl orcarboxyl; each R^ independently is hydrogen, C]-6alkyl or hydroxyCj-galkyl ; or
R^ and R~> taken together may form a bivalent radical of formula
-CH=CH-CH=CH- ; each R6 is hydrogen ;
Ar' is phenyl; orphenyl substituted with 2 halo-substituents ;
Ar2 is naphtalenyl; phenyl; or phenyl substituted with 1, 2 or 3 substituents each
independently selected from halo, C|_4alkyl, haloC|_4alkyI, C|-4alkyloxy and
C]-4alkyloxycarbonyl ; and
Hct is a monocychc heterocycle selected from furanyl, thienyl, isoxazolyl and
pyrazinyl; or a bicyclic heterocycle selected from qumolinyl, quinoxalinyl, indolyi, benzol hiazolyl, benzofuranyl and benzothienyl; each monocyclic and bicyclic heterocycle may optionally be substituted on a carbon atom by 1 or 2 substituents selected from halo and C ] _4alkyl.
2. A compound according to claim 1 wherein Het is a monocyclic heterocycle selected from furanyl, thienyl, oxazolyl, isoxazolyl and pyrazinyl; or a bicyclic heterocycle selected from quinolinyl, benzothiazolyl, benzofuranyl and benzothienyl; each monocyclic and bicyclic heterocycle may optionally be substituted on a carbon atom by I or 2 substituents selected from halo and C]_4alkyl.
3 A compound according to claim 1 or 2 wherein R' is Ar'Cj_6alkyl, R2 is phenyl substituted with 2 substituenls selected from methyl or trifluoromethyl, and X is a uovalent bond
I 0
4. A compound according to any one of chums ! 10 3 wherein R ' is phenyimethyl. R- i.s phenyl substiiuicd with 2 suhstituenls seLv led from methyl or iriiluoromcthyl- n. m are I and X is a covalent hond.

39
5. A compound according to any one of claims 1 to 4 wherein L Is a
radical of formula (a-1) wherein -A-B- Is a radical of formula (b-1)
wherein Y is -S-; and R7 is hydrogen; or -A- B- is a radical of formula
(b-2) wherein Y is -NCH3-; and H7 is hydrogen; or -A-B- is a radical of
formula (b-3); Z Is a bivalent radical of formula -CH2- or -CH^-CH?-,
provided that when the dotted line is an extra bond, then Z is other
than -CH3-; R4 is formyt; and Rs is hydrogen; R6 is hydrogen; or L is a
radical of formula (a-2) wherein - A-B- is a radical of formula (b-3); Z Is
a bivalent radical of formula -CH2-CH2-; R4, R5 and RB are hydrogen.
6. A compound according Jo claim 1, wherein the compound Is
i-tS^-blsftrlfluoromethyObenzoylJ^^S.e-dlhydrosplrotHH-lmldazo^.i-
bjtSjbenzazepine-H^'-piperidinj-i-yO-S^phenylmethyOpiperidine;
i-fS.S-bisOrifluoromethyObenzoyQ-^^^S.e.S.IO-tetrahydro-
imidazo[1,2-a]thleno-[2,3-d]azepirM0-ylidene)-1-plperdinyt]-2-
(pheny!meLhyl)piperid!ne;
i-ES^-bisOrifluoromethyObenzoyn^-^-CS.ej.iO-tetrahydro-?-
methylimldazoti^-aJ-pyrrolotS^-dJasepin-IO-ylidenej-i-plperldinyiJ^-
(phenylmethyl)piperidlne; and
i-tS^-bisOrinuoromethyObenzoyO^-K^S-formyl^.e-dihydro-IIH-
lmida2O[2l1-b][3]-benzazepin-11-ylidene)-1-piperidinyl3-2-
(phenyimethyl)piperldine;
4-[4-(5,6,7,10-tetrahydro-7-methyiim id azo[1,2-a]pyrrolo[3,2-d]a2epin-
10-yiidene)-1-piperidiny(]-1-(3,5-dimethylbereoyl)-2-
(phenyimethyOpiperldlns; and
4-[4-(5l6-dihydro-6-oxo-i0H-tmida2O[1,2-s]thieno[3)2-d3azepin-10-
y(idene)-1-plperidjnyn-i-(3J5-dfmethy(benzoyr)-2-

- 40-
(phenylmethytyplperldjne; a stereolsomerlc form, or a pharmsceutlcairy acceptable acid addition salt thereof.
7. A process of preparing a compound as claimed in claim 1, characterized by,
(a) reductrvely N-afkylating an intermediate of formula (III) wherein L is according lo claim 1, with an intermediate of formula (II)

wherein Rf, R:, X, Q, n and m are according to claim 1, in a reaction-Inert solvent, in (he presence of a reducing agent and optionally in the presence of a suitable catalyst; (b) reacting an Intermediate of formula (IV) wherein R2, X and Q are
according io claim 1 and W1 Is an appropriate leaving group with an
intermediate of formula (V)

wherein R1, L, n and m ara according to claim 1, in a reaction-inert solvent snd in tne presence of a suitable base;

¦41-
and, if desired, converting compounds of formula (0 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.
Dated this 23rd day of December, 1996.

This invention concerns the compounds of formula
the N-oxide forms, the pharmaceutically acceptable addition salts and the stereochemically isomeric forms thereof, wherein n is 0, 1 or 2; m is 1 or 2, provided that if m is 2, then n is 1; =Q is =O or =NR3; X is a covalent bond or-O-, -S-, -NR3-; R1 is AT1, Ar1C1-6 alkyl or di(Ar1) C1-6alkyl, wherein each C1-6alkyl group is optionally substituted; R2 is Ar2, Ar2C1-6aIkyl, Het or HetC1-6alkyl; R3 is hydrogen or C1-6alkyl; L is a piperidine derivative of formula (a-1) or a spiro piperidine derivative of formula (a-2); Ar1 is phenyl or substituted phenyl; Ar2 is naphtalenyl; phenyl or substituted phenyl; and Het is a monocyclic or bicyclic heterocycle; each monocyclic and bicyclic heterocycle may optionally be substituted on a carbon atom; as substance P antagonists; their preparation, compositions containing them and their use as a medicine.


Documents:

02224-cal-1996 abstract.pdf

02224-cal-1996 claims.pdf

02224-cal-1996 correspondence.pdf

02224-cal-1996 description(complete).pdf

02224-cal-1996 form-1.pdf

02224-cal-1996 form-18.pdf

02224-cal-1996 form-2.pdf

02224-cal-1996 form-3.pdf

02224-cal-1996 form-6.pdf

02224-cal-1996 g.p.a.pdf

02224-cal-1996 latters patent.pdf

02224-cal-1996 priority document.pdf

02224-cal-1996 reply f.e.r.pdf

2224-CAL-1996-(29-03-2012)-FORM-27.pdf

2224-CAL-1996-(29-03-2012)-PA.pdf

2224-cal-1996-granted-abstract.pdf

2224-cal-1996-granted-claims.pdf

2224-cal-1996-granted-description (complete).pdf

2224-cal-1996-granted-form 2.pdf

2224-cal-1996-granted-specification.pdf

2224-cal-1996-priority document.pdf


Patent Number 212127
Indian Patent Application Number 2224/CAL/1996
PG Journal Number 47/2007
Publication Date 23-Nov-2007
Grant Date 20-Nov-2007
Date of Filing 23-Dec-1996
Name of Patentee JANSSEN PHARMACEUTICA N.V.,
Applicant Address TURNHOUTSEWEG 30, B-2340-BEERSE, BELGIUM,
Inventors:
# Inventor's Name Inventor's Address
1 FRANS EDUARD JANSSENS TINSTRAAT 79 B-2820-BONHEIDEN
2 JOSEPH ELISABETH LEENAERTS POTBERGSTRAAT 35 B-2310-RIJKEVORSEL BELGIUM.
3 YVES EMIEL MARIA VAN ROOSBROECK ZONDERSCHOTSESTEENWEG 26 B-2220-HEIST-OPDEN-BERG BELGIUM.
PCT International Classification Number C07D 471/20
PCT International Application Number N/A
PCT International Filing date
PCT Conventions:
# PCT Application Number Date of Convention Priority Country
1 NA