Title of Invention

A PYRIDINE-1-OXIDE DERIVATIVE, AND PROCESS FOR ITS TRANSFORMATION INTO PHARMACEUTICALLY EFFECTIVE COMPOUNDS"

Abstract The invention relates to N-[2-hydroxy-3-(1-piperidinyl)-propoxy]-pyridine-l-oxide-3-carboxamidine and its optically active enantiomers. (R)-(-)-N-[2-hydroxy-3-(l-piperidinyl)-propoxy]-pyridine-1-oxide-3-carboxamidine and (S)-(+)-N-[2-hydroxy-3-(1-piperidinyl)-propoxy]-pyridine-l-oxide-3-carboxamidine. Furthermore, the invention relates to the preparation of N-[2-hydroxy-3-(l-piperidinyl)-propoxy]-pyridine-l-oxide-3-carboxyimidoyl chloride, which may be used as an active ingredient of medicaments, and the preparation of the optically active enantiomers of this compound using the compounds of the invention as intermediate substances.
Full Text 2
derivatives of the compound are also claimed, but there is no specific mention of the N-[2-ydroxy-3-(1-piperidinyl)-propoxy]-pyridine-1-oxide-3-carboximidoyl -ehioride, end itspreparation process is not described either.
N-[2-hydroxy-3-(1-piperidinyl)-propoxy]-pyridine-1-oxide-3-carboximidoyl chloride is disclosed and claimed as a novel compound in WO 00/50403, and its production process is described there as well. The compound Is produced by the oxidation of the N-[2-hydroxy-3-(1-plperidinyl)-propoxy]-pyridine-3-carboximidoyl chioride. In the course of oxidation with peracids, the bis-N-oxide derivative oxidized on the N-atoms of both the piperidine ring and the pyridine ring, or the piperidine-N-oxide derivative are formed preferentially, and therefore the oxidation with peracid must be performed in the presence of a strong acid to ensure the dominance of the formation of the pyridine-N-oxide derivative in the course of the oxidation process. The yield of this process, however, is not satisfactory. The optically active enantiomers of the N-[2-hydroxy-3-(1-plperidinyl)-propoxyI-pyridine-1-oxide-3-carboximid-oyl chloride are also described in WO 00/50403. They are prepared in a way similar to the preparation of the raceme compound using the suitable optically active starting substances.
Considering the fact that the N-[2-hydroxy-3-(1-piperidinyl)-propoxy]-pyridine-1-oxide-3-carboximidoyl chloride and its optically active enantiomers are not only useful in the treatment of diabetic complications, primarily retinopathy, neuropathy and nephropathy, but simultaneously reduce chronic insulin resistance, these compounds are valuable active Ingredients in pharmaceutical products. However, in order for these compounds to be useful

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in the pharmaceutical industry, an easier process is necessary for their production.
DISCLOSURE OF INVENTION
We have found that N-[2-hydroxy-3-(1-plperidinyl)-propoxy]-pyridine-1-oxide-3-carboxamidine of formula (I), which is a new compound, is useful as intermediate for making possible the simple production of N-[2-hydroxy-3-(1-piperidinyl)-propoxy)-pyridine-1-oxide-3-carboximidoyl chloride in high purity and in a high yield.
Based on this observation, the present invention relates to the N-[2-hydroxy-3-(1-piperidinyI)-propoxy]-pyridine-1-oxide-3-carboxamidine. and its acid addition salts. The invention also rotates to the optically active enantiomers of the aforementioned compound, the (R)-(-)-N-[2-hydroxy-3-(1-piperidinyl)-propoxy]-pyridine-1-oxide-3-carboxamidine and the (S)-(+)-N-[2-hydroxy-3-(1-plperidinyl]-propoxy]-pyridine-1-oxide-3-carboxamidine, and the acid addition salts of these compounds.
Hereafter, "optically active enantiomer" refers to a compound whose optical purity is at least 80%, preferably at least 90%, most preferably at least 86%, that is, the compound contains at least this mass ratio of the specified optically active enantiomer. "Acid addition salts" refers to salts produced from the compounds with mineral or organic salts, by the known process.
As mentioned above, the compounds of the invention may be used as intermediates in the production of N-[2-hydroxy-3-(1-piperidinyl)-propoxy]-pyridine-1-oxide-3-carboximidoyl chloride. Therefore, the Invention relates to the

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use of N-[2-hydroxy-3-(1-pIperidinyl)-propoxy]-pyrldlne-1-oxide-3-carboxamldine and its optically active enantiomers in the preparation of N-[2-hydraxy-3-(1--plperidinyl)-propoxy]-pyridine-1-oxid-3-carboximidoyl-chloride-and-its-optically-active enantiomers.
The compound N-[2-hydroxy-3-(1-plperidinyl)-propoxy]-pyridine-1-oxide-3-carbox-amidine of the invention is preferably prepared by the following method.
3-cyano-pyridine is used as a starting compound, and the 3-cyano-pyridlne-1-oxide of formula (II), which fs known from the literature [J. Chem. Soc. 3680 (1959)], can be produced by oxidation. A peracld Is used as oxidant preferably m-chloro-perbenzoic acid. The thus obtained product may be purified by orystalization, but the raw product may also be used in the next step of the synthesis.
By reacting the 3-cyano-pyridine-1-oxide of formula (II) wtth hydroxyfamine, 3-pyridine-amidoxim-1-oxide of formula (III) is produced. The reaction is performed in a suitable aqueous solution, at room temperature, by reacting 3-cyano-pyridine-1-oxide with hydroxylamine, added in excess and liberated in water in situ from its hydrochloride salt with sodium bicarbonate. The product precipitates, therefore it can easily be isolated and purified by crystallization.
N-[2-hydroxy-3-(1-plperidinyl)-propoxy]-pyridine-1-oxide-3-carboxamidine of formula (I) is prepared from the 3-pyrldine-amidoxim-1-oxide of formula (lll), by reacting the compound with a reactive 3-(1-plperidino)-2-hydroxy-propane derivative. As reagent a 1-halo- or 1,2-epoxy-derivative may be used, but

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preferably a cyclic derivative, a halide of 2-hydroxy-4-azoniaspiro[3,5]nonane should be used as reagent. The most preferable reagent Is the 2-hydroxy-4--azoniaspiro[3-5]nonane-chloride-of-formula (IV). The reaction is performed in an
alkaline medium, using a suitable alcohol, preferably an alkanol of 1-3 carbon atoms, mora preferably ethanol as solvent The reagents may be added In any order. Preferably, the reactive 3-(1-piperidino)-2-hydroxy-propane derivative is applied in a slight excess. The reaction is performed at an elevated temperature, preferably at the boiling-point of the solvent
The thus obtained compound of formula (I) is either isolated as a base and used as Intermediate in the preparation of the biologically effective N-[2-hydroxy-3-(1-piperidinyl)-propoxy]-pyridine-1-oxide-3-carboximidoyl chloride, or the compound is transformed into an acid addition salt with a mineral or organic acid. Thus mono or dihydrochloride, maleate, or any other acid addition salt may be prepared which are suitable. for the use of the compound as Intermediate in the preparation of the above mentioned end product However, it is not necessary to isolate the N-[2-hydroxy-3-(1-plperidinyl)-propoxy]-pyridine-1-oxide-3-carboxamidine to be used as Intermediate. The next step in the synthesis of N-[2-hydroxy-3-(1-piperidinyl)-propoxy]-pyridine-1-oxide-3-carboximidoyl chloride may be performed without the isolation of the compound of formula (I) as well.
When preparing of an optically active product is desired, the compound of formula (I), prior to the transformation, can be resolved by reacting it with an optically active acid suitable for the formation of a dlastereomer salt pair, by the well known methods of resolution. When the salt of the required optical purity is

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obtained, the optically active base may ba liberated from it. Thereafter, if needed, an add addition salt may be produced from the base with a mineral or organio-acid Either the base or the salt may then be used for the next step of the process of the invention.
According to the Invention, N-[2-hydroxy-3-(1-plperidinyl)-propoxy]-pyridine-1-oxide-3-carboxamidine of formula (I) is transformed into N-[2-hydroxy-3-(1-piperidinyl)-propoxy]-pyridine-1-oxide-3-carboximidoyl chloride by dlazotation in the presence of hydrochloric acid. The diazotation is performed by the usual method, at a temperature of between -5"C and 0oC, with the slow addition of an alkali-nitrlte, preferably of sodium-nitrite. In the presence of hydrochloric add, the thus obtained diazonium salt decomposes at the temperature of the dlazotation into N-[2-hydroxy-3-(1-plperidinyl)-propoxy]-pyridine-1-oxide-3-carboximidoyl chloride of formula (V). Then the reaction mixture is aikalified, while cooling, and the product Is isolated in the form of a base by the usual method. The obtained base may be further purified if needed, or transformed into an acid addition salt with a mineral or organic acid. Preferably, maleate or citrate is formed from the compound of formula (V). but It may also be transformed into hydrochloride, dihydrochloride or any pharmaceutically acceptable acid addition salt
The required optically active enantiomers of the N-[2-hydroxy-3-(1-piperidirryl)-propoxy]-pyridine-1-oxide-3-carboximidoyl chloride of formula (V) prepared by diazotation are prepared by resolution from the raceme compound. The resolution is again performed by the formation of a dlastereomer salt pair.

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preferably with dibenzoyl-tartaric acid, using its suitable optically active form for the salt formation.
if-the-above-described -dlazotation of N [2-hydroxy-3-(1-piperidinyl)-propoxy]-pyridine-1-oxide-3-carboxamidine of formula (I) is performed on an optically active enaritiomer, the enantiomer of the N-[2-hydroxy-3-(1-plperidinyl)-propoxy]-pyridine-1-oxide-3-carboximldoyl chloride of formula (V) of opposite rotation is formed, of satisfactory optical purity. Therefore, according to another version of the process of the Invention, the optically active N-[2-hydroxy-3-(1-plperidllnyl)-propoxy]-pyridine-1-oxide-3-carboximidoyl chloride of formula (V) is prepared by performing the above described diazotation on the suitable optically active enantiomer of N-[2-hydroxy-3-(1-piperidinyl)-propoxy]-pyridine-1-oxide-3-carboxamidine of formula (I). The thus obtained base may be further purified rf needed, or an acid addition salt may be formed with a mineral or organic acid.
The advantage of the invention is that by the use of the compound of formula (I) of the invention as intermediate, it makes possible the production of highly pure N-[2-hydroxy-3-(1-piperidinyl)-propoxy]-pyridlne-1-oxide-3-carboximidoyl chloride, which has valuable biological effects. Contrary to the process described in WO 00/50403 mentioned in the Introduction, in which this compound is prepared by the oxidation of N-[2-hydroxy-3-(1-piperidinyl)-propoxy]-pyridine-3-carboximidoyi chloride, in this current process the appearance of the products of competitive reactions need not be taken into account By the process of the invention, the base form of N-[2-hydroxy-3-(1-piperidinyl)-propoxyJ-pyridine-1-oxide-3-carboximidoyl chloride is obtained in

8
high purity. Up to this point, this was only possible by lengthy purification, or by liberation of the base from the maleate salt.
A further advantaga of the invention is that the N [2-hydroxy-3-(1-plperidinyl)-propoxy]-pyrldine-1-oxide-3-carboxamldine may be produced by the merge of the steps described above and Illustrated in the following examples In greater detail, without the isolation and/or purification of each intermediate product, still obtaining satisfactory purity. This way, the production of the intermediate N-[2-hydroxy-3-(1-piperidinyl)-propoxy]-pyridine-1-oxide-3-carboxamidine becomes possible in the circumstances of pharmaceutical production, which makes possible the Industrial production of the biologically effective N-[2-hydroxy-3-(1-plperidlnyl)-propoxy]-pyridine-1-oxide-3-carboximidoyl chloride.
BEST MODE OF CARRYING OUT THE INVENTION
The invention is illustrated by the following examples.
Example 1.
The preparation of 3-cyano-pyridine-1-oxide (compound of formula ll)
86g (0.378 mol) of 76% m-chloro perbenzolc acid is dissolved in 730ml of dtehloro-methane at 20-25°C, and 220 ml of the solution of 38.3g (0.37B mol) of 3-cyano-pyridine in dichloro-methane is added at 20-28*C. The reaction mixture is stirred at 20-24"C for 24 hours. At the end of the reaction, the solvent is evaporated. The evaporation residue is dlgerated in 430ml of methyl terc-butyl ether, the precipitate is filtered, washed and dried. 59g of raw product Is obtained.

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By recrystallizing the raw product twice from hot ethanol, 36.6g (80%) of pure 3-cyano-pyridine-1-oxide is obtained, which melts at 174-176.5°C (literature: 174 175ºC-J-Ghem. Soc. 3680 (1959)):
Example 2.
The preparation of 3-pyridine-amidoxim-1-oxide (compound of formula III)
25.41g (0.366 mol) of hydroxylamine hydrochlorlde and 36,6g (0.305 mol) of 3-cyano-pyridine-1-oxide are dissolved in 540ml of water, then 30.72g (0.366 mol) of sodium-hydrogen carbonate Is added In small portions. The reaction mixture is stirred for 2 hours at 20-25ºC. The suspension is filtered, the precipitate is washed with water, dried, and recrystallized from a 9:1 mixture of methanol and water. The precipitate separating on cooling is filtered, washed and dried. 37.3g (80%) of the title compound is obtained, which melts at 212-215°C while decomposing.
IR: v (KBr, cm-1): 3407, 3337, 2840, 1660, 1470, 1429, 1397, 1227, 947, 925, 808. 792.
Example 3.
a) The preparation of N-[2-hydroxy-3-(1-piperidinyl)-propoxy]-pyridine-1-oxide 3-carboxamidine (compound of formula I)
13.5g (0.34 mol) of sodium-hydroxide is dissolved in 35ml of water, and the solution is cooled to 10ºC. 60.75g (0.34 mol) of 2-hydroxy-4-azonlasplro[3,5]nonane chloride is added, and the reaction mixture is stirred for 40 minutes at 5-10°C. 540ml of ethanol and 40.5g (0.26 mol) 3-pyridine-

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amidoxim-1-oxide are added. The reaction mixture is heated for 2 hours under a reflux condenser. The solution is cooled, the separated sodium chloride Is filtered, washed with 100ml of ethanol, and then the solvent is evaporated off. The evaporation residue is digerated with diethyl-ether, the precipitate separated in the cooler is filtered, washed with ether, dried, and crystallized hot from fsopropanol. 47.4g (62%) of the title compound is obtained, which melts at 130-132.5ºC.
IR: v (KBr, cm-1): 3397. 3189. 2928,1647.1610,1570,1505, 1425.1247, 1226, 1033. 042. 901, 782. 662. 531.
b) The preparation of N-[2-hydroxy-3-(1-plperidinyl)-propoxy]-pyrldine-1-oxide-3-carboxamidine monohydrochloride
The obtained base of formula (I) is dissolved in ethanol, and 1 equivalent
of ethanolic hydrochloric add solution is added. The solution is evaporated, and
the residue fe digerated with isopropanol. The separated salt is filtered, washed
and dried. N-[2-hydroxy-3-pIperidinyl)-propoxyl-pyridine-1-oxido-3-
carboxamidine monohydrochloride is obtained. Melting point 142-144.5ºC 1H-NMR: (Solvent DMSO; referent DMSO; MHz: 75.4) 5 [ppm]: 9.65 (bs.1H,NH*); 8.42 (s,1H,2-pyridine); 8.22 (d,1H,6-pyridine); 7.56 (d.1H.4-pyridine); 7.42 (t.1H.5-pyridine); 6.50 (s.2H,NH2); 5.72 (d.1H,OH); 4.24 (bm.1H,OCH); 3.86 (m.2H.NOCH2); 3.42 (m,2H,2 x NCH); 3.18 (m,2H,NCH2); 2.92 (m,2H,2 x NCHxx); 136-1.8 (m,6H,3-, 4- and 5-piperidine).
13C-NMR: (Solvent: DMSO; Referent: DMSO; MHr 75.4) 0 [ppm]:
148.2 (CNO); 139.2(2-pyridine); 135.9 (6-pyridine); 131.8 (3-pyridine); 126.3 (5-
pyridine); 122.9 (4-pyridine); 74.9 (CHOH); 63.6 (NOCH2); 58.9 (NCH2); 53.6

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and 51.9 (2C.2 x piperidine NCH2); 22.1 (2C,3- and 5-plperidine); 21.2 (4-piperidine). CT content According to Mohr (calculated/measured); 10.7 /10:45.
Example 4.
a) The preparation of N-[2-hydroxy-3-(1-piperidinyl)-propoxy]-pyridine-1-oxide-3-carboximidoyl chloride (Compound of formula V)
The solution of 6.1g (0.088 mol) of sodium nitrite in 40ml of water ts added dropwlse at -5 - 0'C to the solution of 20g (0.068 mol) of N-[2-hydroxy-3-(1-piperidinyl)-propoxy]-pyridino-1-oxide-3-carboxamidine in 110ml of 1M hydrochloric acid cooled to -5"C. The reaction mixture is stirred for 1.5 hours at between -5ºC and 0"C, and then, by intense cooling (t IR o (KBr, cm-1): 3224, 2935, 2800, 2780, 1570, 1555, 1428, 1301, 1290, 1200, 1100, 1054, 1044, 1023,1015, 995, 845, 827. 785, 710. 685.
b) The preparation of N-[2-hydroxy-3-(1 -piperidlnyl)-propoxy}-pyridine-1-oxide-3-carboximidoyl chloride maleate

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50g of the base prepared as described above is dissolved in 50ml of acetone, and an equivalent amount (1.85g) of maleic acid is added to it The separated-precipitate-is-filtered, washed with aoetone and dried. The product is recrystallized from ethanol. 6.0g (67%) of N-[2-hydroxy-3-(1-piperidinyl)-propoxy]-pyridine-1-oxide-3-carboximidoyl chloride maleate (1:1) is obtained, Which melts at 150.5-154.5ºC.
1H-NMR: (Solvent DMSO; Referent: DMSO; MHz: 300) D [ppm]:
8.55 (s, 1H, 2-pyridine); 8.35 (d, 1H. 6-pyridine); 7.88 (d. 1H, 4-pyridine); 7.55 (m, 1H, 5-pyridine); 6.00 (s, 2H, CH=CH); 4.23-4.48 (m, 3H. CH-OH and NOCH2); 2.95-3.50 (m, 6H. 3 NCH2); 120-1.90 (m, 6H. piperidine: 3 CH2)
13C-NMR: (Solvent: DMSO; Referent DMSO; MHz: 75.4) D [ppm]: 167.6 (2C, 2 COOH); 141.0 (2-pyridine). 136.8 (6-pyridine); 136.4 (2C, CH=CH); 133.4 (CCI); 131.9 (3-pyridine); 127.2 (4-pyridine); 123.6 (5-pyridine); 77.9 (NOCH2); 63.6 (CH2N); 58.3 (CHOH); 52.0-55.0 (2C. piperidine: 2 NCH2); 22.6 and 21.7 (3C. piperidine: 3 CH2).
c) The preparation of (R.S)-N-[2-hydroxy-3-(1-piperidinyl)-propoxy]-pyridine 1-oxide-3-carboximidoyl-chloride monohydrochloride
0.64 g (2,0 mmotes) of (R,S)-N-[2-hydroxy-3-(1-piperidlnyI)-propoxy]-pyridine-1-oxide-3-caboximidoyl-chloride base is dissolved In 20 ml of ethylacetata and 0.64 ml of the etheric solution of 3.2 M hydrochloric acid is added while stirring. A sticky precipitate is formed. After evaporating the solvent 15 ml of acetone is added and refrigerated overnight The precipitate is crystallized with the addition of some drops of ethanol, then the white

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hygroscopic material rs quickly filtered, and dried in a desiccator over
phosphorous-pentoxide.
Yield. 0:4g (66.3 %)
Melting point: 115-122 °C
CI %(Ionic): 11.2 % (theoretical: 10.1 %)
IR (KBr, crn-1): 3240, 3080, 2950, 2860, 2760, 1575, 1550, 1465. 1450, 1431, 1310, 1293, 1240, 1195. 1155, 1120, 1090, 1075, 1045, 1005, 945, 925. 830, 792.715,671,550.
Example 5.
a) The preparation of (R)-(+)-N-[2 hydroxy-3-(1-piperidinyI)-propoxy]-pyndine-1-oxide-3-carboximidoyl chloride by the resolution of the raceme compound
54g (0.172 mot) of raceme N-[2-hydroxy-3-(1-plperidinyr)-propoxy]-pyridine-1-oxide-3-carboximidoyl chloride is dissolved in 720ml of dry ethanol. After complete dissolution, 64.7g (0.172 mol) of (-)-dibenzoyl-L-tartaric acid monohydrate is added. After" seeding, it is crystallized at room temperature, then the separated precipitate Is filtered, washed and dried. The obtained residue is crystallized twice from dry ethanol. 38g (65%) of (R)-(+)-N-[2-hydroxy-3-(1-piperidinyl)-propoxy]-pyridine-1-oxide-3-carboximidoyl chloride dibenzoyl-L-tartaric acid salt is obtained.
The thus obtained 38g (0.056 mol) of tartaric acid salt Is then added to 230ml of 1M K2CO3 solution, and the mixture is extracted with 3 x 225ml of

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dichlcro-mothane. The organic phases are pooled, dried on anhydrous MgS04, treated with charcoal, filtered and evaporated. The compound is obtained in a pura form from the crude buse by crystallization with hexanar. YIeldr 14.0g (80%). Metting point 91-93ºC.
IR: o (KBr, cm-1): 3181, 2938, 2800,1575, 1555, 1473 1431, 1350, 1300,1288, 1251, 1232, 1186,1162, 1555, 1095, 1055, 1044, 1020, 1011, 963, 928, 908, 899, 850,831,803, 700, 670.
1H-NMR: (Solvent CDCl3; Referent CDCl3 MHZ300) S [ppm]:
8.62 (s,1H,2-pyridin), 8.20 (d,1H,6-pyridine); 7.64 (m,1H.4-pyridine); 7.26
(m,1H,5-pyridine); 4.24 (d,2H,NOCH2); 4.02 (m,1H.OCH); 2.58 (m,2H,NCH2);
2.32 (m,4H,2 x piperidine NCH2); 1.5-1.6 (m,4H,3- and 5-piperidine); 1.42
(m,2H,4-plperidine).
13C-NMR: (Solvent: CDCl3; Referent CDCl3; MHz:75.4????ppm]: 140.0 (2-pyridine); 137.5 (6-pyridine); 132.7 (CNO); 132.4 (3-pyridine); 125.5 (5-pyridine); 123.8 (4-pyridine); 78.8 (OCH); 64.9 (NOCH2); 60.6 (NCH2); 54.6 (2C,2x piperidin NCH2); 26.0 (2C,3- and 5-piperidine); 24.1 (4-piperidine).
b) The preparation of (R)-(+)-N-[2-hydroxy-3-(1-piperidinyl)-propoxy]-pyridine-1-oxide-3-carbuximidoyl chloride maleate
18.0 g of crude (evaporation residue from the process a/) or isolated base is dissolved in 62ml of acetone, and then the solution of 6.6 g mateic acid in 46ml of acetone is added. The precipitate separating on cooling is filtered, washed with 10ml of acetone and dried. The precipitate (approx. 23g) is crystallized from 120ml of hot ethanol. The precipitate separating on cooling is filtered washed and dried.

15 Yield: 20g (82%) Melting point: 132.0-133.5ºC
Enantiomer ratio. 98/2 (HPLC measurement on a Chiral AGP 100x4mm column)
IR: u (KBr, cm-1): 3270 (b); 2835; 2850, 1581; 1484; 1436; 1349; 1293 (a); 1205 (s); 1067; 1047; 999 (a); 865 (s); 830; 800, 682, 558. The 1H-NMR and 13C-NMR spectra were the same as those of the raceme compound (Example 4/b).
c) The preparation of (R)-(+)-N-[2-hydroxy-3-(1-piperidinyl)-propoxy]-
pyridine 1 oxide 3 carboximidoyl chloride citrate
2.43g (7.75 mmol) of (+)-/R/-N-[2-hydroxy-3-(1-piperidinyI)-propoxy]-pyridine-1-oxide-3-carboximidoyl chloride is dissolved in 15ml of acetone while heating gently, then 5ml of the solution of 1.63g (7.75 mmol) of citric acid in acetone is added. The separating white sticky substance becomes a powder on the addition of 6rnt of methanol. The solution rs refrigerated until the following day. The precipitate is filtered, washed with acetone, and dried. 3.99g (98%) of product is obtained. Melting point 163-165ºC.
13C-NMR: (SolventDMSO/CDCls; Referent CDCl3; MHz:75.4) 5 [ppm]: 175.2 (COOH); 169.9 (2C, 2 COOH); 138.6 (2 pyridine), 134.7 (4-pyridine); 131.0 (CCI); 129.9 (3-pyridine); 125.0 (6-pyridine); 122.5 (5-pyridine); 78.0(COH); 69.7(CHOH); 62.0 (NOCH2); 57.0 (CH2N); 51.5 (2C, 2 x piperidine NCH2); 42.3(2C,2x CH2); 21.0 (2C. 3- and 5-plperidine CH2); 20.0(4-piperidine).

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d) The preparation of (R)-(+)-N-[2-hydroxy-3-(1-piperidinyl)-propoxyl-pyridine-1 -oxtde-3-carboximidoyl-chlotlde monohydrochloride
0:88 g (208 mmoles) of (R)-(+)-N-[2-hydroxy-3-(1-plperidinyl)-propoxyl]-pyridine-1-oxide-3-carboximidoyl-chloride base (prepared from its maleate using dichloromethane/10 % aqueous sodium-carbonate solution) is dissolved in 25 ml of ethylaoetate and 0.87 ml of the etheric solution of 3.2 M hydrochloric acid is added while stirring.
After evaporating the solvent, 15 ml of acetone is added to the residual
sticky oil and crystallized with with the addition of some drops of ethanol. The
white compound is filtered and washed with acetone and diethyl ether.
Yield: 0.8 g (81.6%)
Melting point: 127-131 °C
Cl %(ionic): 12.1 % (theoretical: 10.1%)
IR (KBr, cm-1): 3510, 3365. 3120, 3075, 2950, 2930, 2890, 2855, 2725,
2655, 2568, 2527, 1620, 1600, 1562, 1483, 1460, 1428, 1407, 1350, 1335, 1294, 1238, 1197,1170, 1125, 1072, 1019,1002, 942. 910, 877, 859, 825, 802. 708, 671, 629. 608, 556, 501.
e) The preparation of (R)-(+)-N-[2-hydroxy-3-(1-plperidinyI)-propoxy]-pyridine-1-oxide-3-carboxirnidoyl-chloride dihydrochloride
0.65 g (2.0 mmoles) of (R)-(+)-N-[2-hydroxy-3-(1-piperidinyl)-propoxy]-pyridine-1-oxide-3-carboximidoyt-chloride base (prepared from its maleate using dichloromethane/10 % aqueous sodium-carbonate solution) is dissolved

17
in 25 ml of ethyiacetate and 1.4 ml of the etheric solution of 3.2 M hydrochloric acid is added while stirring.
After evaporatin the solvent, 15 ml of aoetone is added to the residual
sticky oil and crystallized with the addition of some drops of ethanol. The white
compound is filtered and washed with cold acetone and diethylether.
Yield: 0.4 g (55.0%)
Melting point 160-164 0C
CI % (Ionic): 18.5 % (theoretical: 18.3 %)
IR (KBr, cm'1): 3510, 3365, 3120, 3075, 2950. 2830, 2890, 2855, 2725,
2568, 2527,1620. 1600. 1562, 1483, 1460, 1428, 1407, 1350. 1335, 1294, 1238, 1197, 1170, 1125, 1072, 1019, 1002, 942, 910, 877, 859, 825, 802, 708, 671,629,608,556,501.
Example 6.
a) The preparation of (S)-(+)-N-[2-hydroxy-3-(1-plperidinyl)-propoxy]-pyridine-1-oxide-3-carboxamidine by the resolution of the raceme compound
1.74g (5.9 mmol) of raceme N-[2-hydroxy-3-(1-piperidinyl)-propoxy]-pyridine 1 oxide 3 carboxamidine is dissolved in 15ml of ethanol, and then 2.1g (5.9 mmol) of /+/-dibenzoyl-D-tartaric acld is added to the solution, it is crystallized at room temperature, the separated salt is filtered, washed with ethanol, and dried. The 2.1g product is then crystallized twice from ethanol to give 0.33g (17%) of (S)-(+)-N-[2-hydroxy-3-(1-plperidinyl)-propoxy]-pyridine-1-oxide-3-carboxamidine diebnzoyl-D-tartaric acid salt (melting point 156-158ºC).

18
The (S)-(+)-N-[2-hydroxy-3-(1-piperidinyl)-propoxy]-pyridine-1-oxide-3-carbox-amidine is liberated from the obtained salt by distribution between 2M K2CO3 solution and chloroform, evaporation of the chloroform soludon and
isolation with ether. Yield: 0.11g (13%).
Melting point 123-126ºC.
IR: o (KBr, cm-1): 3398, 3188, 2936, 2800, 1647, 1600, 1560, 1500, 1426, 1245, 1226, 1033, 942, 907, 800, 667. Rotation: [a]o = + 4,5º (c = 1, methanol).
To determine the optical purity of the product, a small sample is transformed into the corresponding chloro compound, (S)-(-)-N-[2-hydroxy-3-(1-plperidinyl)-propoxy]-pyridine-1-oxide-3-carboximidoyl chloride by the diazotation process described in example 4/a, and its optical purity is determined by HPLC on a Chiral AGP column. Determined by this method, the optical purity of the product gained by the described resolution process is 96%.
b) The preparation of (R)-(-)-N-[2-hydroxy-3-(1-plperidinyl)-propoxy]-pyridine-1-oxide-3-carboxamidine by the resolution of the raceme compound
Following the process described in a), but this time using (-)-dibenzoyl-L-tartaric acid for the resolution, the yield of the obtained dibenzoyf-tartarate salt is 20%, and its melting point is 156.5-158ºC. After liberating the base from this, (R)-(-)-N-[2-hydroxy-3-(1-piperidrnyl)-propoxy-pyridine-1-oxide-3-carboxamidine is obtained of optical purity of 96%. Rotation: [a]o = -4,5º (c = 1, methanol).
its melting point and IR spectrum are the same as those of the other enantiomor.

19
c) The preparation of (S)-(+)-N-[2-hydroxy-3-(1-piperldinyl)-propoxy]-pyridine-1-oxide-3-carboxamidine monohydrochloride
The (S)-(+)-N-[2-hydroxy-3-(1-plperidinyl)-propoxy]-pyridine-1-oxide-3-
carbox-amidine base prepared by the example 6/a is dissolved in isopropanol.
Equivalent amount of isopropanolic hydrochloric acid solution is added. The
crystallized monohydrochloride salt is filtered and dried.
Melting point 164-165.5°C
IR: o (KBr, cm-1): 3400, 3317, 3191, 2948, 2862, 2710, 2690, 2655, 1651, 1562, 1429, 1407,1308,1232,1112,1052,1010, 962, 944, 880,797, 670,
d) The preparation of (S)-(+)-N-[2-hydroxy-3-(1-piperidinyI)-propoxy]-pyridine-1-oxide-3-carboxamidine maleate
The maleate salt of the (S)-(+)-N-[2-hydroxy-3-(1-plperidinyl)-propoxy]-pyridine-1-oxide-3-carboxamidine base prepared by example 6/a is prepared by the addition of equivalent maleic acid in an isopropanolic solution.
Melting point 148-150.5°C.
IR: u (KBr, cm-1): 3465, 3381, 3360, 3092, 3058, 2945, 2855, 1651, 1619, 1582, 1561, 1499, 1474, 1459, 1451, 1432, 1318, 1352, 1250, 1230, 1204, 1086, 1035, 1015, 931, 867, 805, 797, 782, 696, 675, 564,
Example 7.
The preparation of (S)-(-)-N-[2-hydroxy-3-(1-plperidinyl)-propoxy]-pyridine-1-oxide-3-carboximidoyl chloride by diazotation

20
By diazotation according to the process described in example 4. followed by the decomposition of the diazonlum salt, 5g of the (S)-(+)-N-[2-hydroxy-3-(1-plperidinyl)-propoxy]-pyridine-1-oxide-3-carboxamidine, prepared under
example 6/a by the resolution of N-[2-hydroxy-3-(1-plperidinyl)-propoxy]-pyridine-1-oxide-3-carboxamidine, is transformed into (S)-(-)-N-[2-hydroxy-3-(1-plperidinyl)-propoxy]-pyridine-1-oxide-3-carboximidoyl chloride. 4.4g (82%) of the product is obtained. The characteristics of the obtained product are the same as those given for the other enantiomer in example 5.
The base is reacted with maleic add by the process given in example 5, and thus the corresponding maleats salt is obtained, whose characteristics are also the same as those given in example 5.


21 WE CLAIM:
1. N-[2-hydroxy-3-(1-piperidinyl)-propoxy]-pyridIne-1-oxide-3-carboxamidine and its acid addition salts.
2. (R)-(-)-N-[2-ydroxy-3-(1-piperidinyI)-propoxy]-pyridine-1-oxide-3-carboxamidine and its acid addition salts.
3. (S)-(+)-N-[2-hydroxy-3-(1-plperidinyI)-propoxy]-pyridine-1-oxide-3-carboxamidine and its acid addition salts.
4. Process for the preparation of N-[2-hydroxy-3-(1-plperidinyl)-propoxy]-pyridine-1-oxide-3-carboximidoyl chloride and its acid addition salts, comprising:

a) the diazotation of N-[2-hydroxy-3-(1-plperidinyl)-propoxy]-pyridine-1-oxide-3-carboxamidine by reacting with an alkall-nitrita in the presence of hydrohcloric acid, or
b) the diazotation of N-[2-hydroxy-3-(1-plperidinyI)-propoxy]-pyridine-1-oxide-3-carboxamidine by reacting with an alkali-nitrite in the presence of hydrohcloric acid, and the transformation of the obtained base into an acid addition salt.


22
5. Process for the preparation of (R)-(+)-N-[2-hydroxy-3-(1-
plperidinyl)-propoxy]-pyridine-1-oxide-3-carboximidoyl chloride and (S)-(-)-N-[2-
hydroxy-3-(1-plperidinyl)-propoxy]-pyridine-1-oxide-3-carboximldoyl chioride,
and their acid addition salts, comprising
a) the diazotation of (R)-(-)-N-[2-hydraxy-3-(1-plperidinyl)-propoxy]-pyridine-1-oxide-3-carboxamidine or (S)-(+)-N-[2-hydroxy-3-(1-plperidinyI)-propoxy]-Pyridine-1-oxide-3-carboxamidine by reacting with an alkali-nitrite in the presence of hydrochloric acid, or
b) the resolution of N-[2-hydroxy-3-(1-plperldinyl)-propoxy]-pyridine-1-oxide-3-carboxamidine, and the diazotation of the obtained optically active (R)-(-) enantiomer or (S)-(+) enantiomer in the presence of hydrochloric acid by reacting with an alkali-nitrite, or
c) the diazotation of N-[2-hydroxy-3-(1-plparidinyl)-propoxy]-pyridine-1-oxide-3-carboxamidine in the presence of hydrochloric acid by reacting with an alkali-nitrite, and the isolation of the required (R)-(+) or (S)-(-) enantiomer by resolving from the obtained raceme N-[2-hydroxy-3-(1-plperidinyl)-propoxy]-pyridine-1-oxide-3-carboximidoyl chloride, or
d) the transformation of (R)-(+)-N-[2-hydroxy-3-(1-plperidinyl)-propoxy]-pyridine-1-oxide-3-carboximidoyl chloride or (S)-(-)-N-[2-hydroxy-3-(1-piperidinyl)-propoxy]-pyridine-1-oxide-3-carboximidoyl chloride, prepared by any of the process variants under a)-c), into an acid addition salt
The invention relates to N-[2-hydroxy-3-(1-piperidinyl)-propoxy]-pyridine-l-oxide-3-carboxamidine and its optically active enantiomers. (R)-(-)-N-[2-hydroxy-3-(l-piperidinyl)-propoxy]-pyridine-1-oxide-3-carboxamidine and
(S)-(+)-N-[2-hydroxy-3-(1-piperidinyl)-propoxy]-pyridine-l-oxide-3-carboxamidine. Furthermore, the invention relates to the preparation of N-[2-hydroxy-3-(l-piperidinyl)-propoxy]-pyridine-l-oxide-3-carboxyimidoyl chloride, which may be used as an active ingredient of medicaments, and the preparation of the optically active enantiomers of this compound using the compounds of the invention as intermediate substances.

Documents:


Patent Number 206723
Indian Patent Application Number IN/PCT/2002/01301/KOL
PG Journal Number 19/2007
Publication Date 11-May-2007
Grant Date 10-May-2007
Date of Filing 18-Oct-2002
Name of Patentee BIOREX KUTATO ES FEJLESZTO RT
Applicant Address H-8200 VESZPREM-SZABADSAGPUSZTA HUNGARY
Inventors:
# Inventor's Name Inventor's Address
1 UROGDI LASZLO H-1184 BUDAPEST, TELEKI U.80, HUNGARY
2 JEGESNE CSAKAIZITA H-6090 KUNSZENTMIKLOS PETOFL LTP. B/19, HUNGARY
3 GRUBER LAJOS H-1025 BUDAPEST, CSERJE U.18 1/2, HUNGARY
4 OTVOS LASZLO H-1025 BUDAPEST BOROKA U.13 11/10, HUNGARY
5 TOMOSKOZI ISTVAN H-1025 BUDAPEST SZEPVOLGYI UT 106, HUNGARY
6 SZAKACSNE SCHMIDT ANIKO H-8200 VESZPREM ALKOTMANY U7 1/3, HUNGARY
7 REIDER FERENCNE` H-8200 VESZPREM SOLYI U.2 111/9, HUNGARY
8 SCHNEIDERNE BARLAY MARIA H-8200 VESZPREM ADY ENDRE, UT 67, HUNGARY
9 TOTH JOZSEF H-1022 BUDAPEST ALSO TOROKVESZ UT 10,
PCT International Classification Number C07D 213/89
PCT International Application Number PCT/HU01/00046
PCT International Filing date 2001-04-17
PCT Conventions:
# PCT Application Number Date of Convention Priority Country
1 P 0001583 2000-04-18 Hungary