FR2832152A1 - New 2-amino-thiazoline derivatives having inducible NO-synthase inhibiting activity, useful for treating Parkinson's, cerebral disorders, migraines, depression, diabetes - Google Patents

Abstract

2-Amino-thiazoline derivatives (I), their racemates, enantiomers, and diastereoisomers, their mixtures, tautomers and salts. 2-Amino thiazoline derivatives of formula (I), their racemates, enantiomers, and diastereoisomers, their mixtures tautomers and salts When Y is methylene, X is O, NH, -N(1-4C alkyl), -N(Bn)-, -N(Ph)-, -N(2-Py)-, -N(3-Py)-, -N(4-Py)-, -N(2-pyrimidyl)-, -N(5-pyrimidyl)-, S, SO, SO2, CH2, or -CH(Ph)-; and when Y is CO, X is NH, -N(Ph)-, -N(2-Py)-, -N(3-Py)-, -N(4-Py)-, -N(2-pyrimidyl)-, or -N(5-pyrimidyl)-. Bn = benzyl; Ph = phenyl; and Py = pyridyl. Independent claims are also included for: (1) Preparation of (I); (2) Preparation of an intermediate of formula (II); and (3) Intermediates of formulae (II), (IIa), (IIb), and (IIc) except for: (i) N-(2-hydroxy-1-(4-phenyl-piperazin-1-ylmethyl)ethyl)thiobenzamide, (ii) methyl 2-(N-CBZ-amino)-3-morpholino-propionate, (iii) Boc-DL- beta -(4-morpholinyl)alanine methyl ester, (iv) methyl 2-acetamido-3-piperidinopropanoate, (v) methyl 2-acetamido-3-morphilinopropanoate, (vi) ethyl 2-(N-benzyl-amino)-3-piperidinopropanoate, and (vii) ethyl 2-(N-benzyl-amino)-3-morphilinopropanoate. Ra = amine-protecting group; and Rb = alkyl or alkoxycarbonyl.

Description

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ou leurs sels pharmaceutiquement acceptables comme inhibiteurs de NO-synthase inductible. The present invention relates to the use of 2-amino-thiazoline derivatives of formula: ## STR2 ## The present invention relates to the use of 2-amino-thiazoline derivatives of formula: ## STR2 ##

or their pharmaceutically acceptable salts as inducible NO-synthase inhibitors.

The invention relates to the use of the 2-amino-thiazoline derivatives of formula (I) and their pharmaceutically acceptable salts for the preparation of pharmaceutical compositions intended to prevent and treat diseases in which abnormal production of nitric oxide (NO) by inducible NO-synthase induction (NOS-2 or iNOS) is involved, the pharmaceutical compositions containing the novel 2-amino-thiazoline derivatives and their pharmaceutically acceptable salts and the novel 2-amino-thiazoline derivatives and their pharmaceutically acceptable salts.

Nitric oxide (NO) is a diffusible radical involved in many physiological and pathological processes. It is synthesized by oxidation of L-arginine, a reaction catalyzed by a family of enzymes called nitric oxide synthase or NO-Synthase (NOS), referenced in the international system of nomenclature of enzymes under number E. C. 1.14. 13. 39.

Three isoforms of NOS, two of which are constitutive and one inducible, are known: - A neuronal NOS (NOS-1 or nNOS) has been isolated and originally cloned from nervous tissue where it is a constitutive enzyme. NOS-1 produces NO in response to various physiological stimuli such as activation of membrane receptors by a calcium-dependent mechanism and calmodulin.

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 an inducible NOS (NOS-2 or iNOS) can be induced in response to immunological stimuli such as, for example, cytokines or bacterial antigens in different cells such as, for example, macrophages, endothelial cells, hepatocytes, glial cells , as well as a large number of other types of cells. The activity of this isoform is not regulated by calcium. This is why, once it is induced, it produces large quantities of NO over prolonged periods of time.

an endothelial NOS (NOS-3 or eNOS) is constitutive and calcium / calmodulin dependent. It was originally identified in the cells of the vascular endothelium where it generates NO in response to physiological stimuli such as activation of membrane receptors.

The NO produced by the constituent neuronal and endothelial isoforms (NOS-1 and NOS-3) is generally involved in intercellular signaling functions.

For example, endothelial cells lining the inner lining of blood vessels induce relaxation of underlying smooth muscle cells via NO production. It contributes to the regulation of blood pressure.

NO produced in large quantities by the inducible isoform NOS-2 is, among other things, involved in the pathological phenomena associated with acute and chronic inflammatory processes in a wide variety of tissues and organs.

Excessive production of NO by induction of NOS-2 thus contributes to degenerative pathologies of the nervous system, such as multiple sclerosis, focal or global cerebral ischemia, brain or spinal injuries, Parkinson's disease, Huntington's disease. , Alzheimer's disease, amyotrophic lateral sclerosis, migraine, depression, schizophrenia, anxiety, epilepsy. Similarly, outside the central nervous system, induction of NOS-2 is involved in many pathologies with inflammatory components such as diabetes, atherosclerosis, myocarditis, arthritis, osteoarthritis, asthma , irritable bowel syndrome, Crohn's disease, peritonitis, gastroesophageal reflux, uveitis, Guillain-Barré syndrome, glomerulo- nephritis, lupus erythematosus, psoriasis. NOS-2 has also been implicated in the growth of some forms of tumors such as epitheliomas, adenocarcinomas or sarcomas, and in infections by intracellular or extracellular, Gram-plus or Gram-less bacteria.

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importants joués par l'isoforme constitutive NOS-3 en particulier dans la régulation de la pression artérielle, il est primordial que l'inhibition de l'isoforme NOS-2 affecte le moins possible l'isoforme NOS-3. En effet, il est connu que l'administration d'inhibiteurs non-sélectifs des isoformes de NOS conduit à une vasoconstriction et à un accroissement de la pression artérielle (Moncada, S., Palmer, R. M. J. et Higgs, E. A., Biosynthesis of nitric oxide from L-arginine : a pathway for the regulation of cell function and communication, Biochem. Pharmacol., 1989,38 : 1709-1715). Ces effets sur le système cardiovasculaire sont délétères dans la mesure où ils diminuent l'apport en nutriments aux tissus. Par conséquent, la présente invention concerne des composés présentant une activité inhibitrice vis-à-vis de la NOS-2 significativement plus puissante que son activité inhibitrice vis-à-vis de la NOS-3. In all situations where overproduction of NO is harmful, it therefore seems desirable to reduce the production of NO by the administration of substances capable of inhibiting NOS-2. However, given the physiological roles

Importantly played by the constitutive isoform NOS-3 especially in the regulation of arterial pressure, it is essential that the inhibition of the NOS-2 isoform affects the NOS-3 isoform as little as possible. Indeed, it is known that the administration of non-selective inhibitors of NOS isoforms leads to vasoconstriction and an increase in arterial pressure (Moncada, S., Palmer, RMJ and Higgs, EA, Biosynthesis of nitric oxide from L-arginine: a pathway for the regulation of cell function and communication, Biochem Pharmacol., 1989, 38: 1709-1715). These effects on the cardiovascular system are deleterious to the extent that they reduce the supply of nutrients to tissues. Therefore, the present invention relates to compounds having a NOS-2 inhibitory activity significantly more potent than its inhibitory activity to NOS-3.

Inhibitors of NOS thiazoline derivatives are described in particular in patent applications WO94 / 12165, WO95 / 11231 and WO96 / 14842.

soit Y est un carboxy (C=O) et X est choisi parmi les groupements suivants : NH, NPh, N- (2-Py), N- (3-Py), N- (4-Py), N-2-pyrimidyle, N-5-pyrimidyle pour la préparation de médicaments utiles pour prévenir ou traiter les maladies dans lesquelles une production anormale de monoxyde d'azote (NO) par induction de NOsynthase inductible (NOS-2 ou iNOS) est impliquée. The present invention relates to the use of 2-amino-thiazoline derivatives of formula (I) wherein: either Y is methylene (CH 2) and X is selected from the following groups: O, NH, N-Alkyl (Cl- C4), N-Bn, N-Ph, N- (2-Py), N- (3-Py), N- (4-Py), N-2-pyrimidyl, N-5-pyrimidyl, S, SO, SO2 , CH2 or CHPh;

or Y is a carboxy (C = O) and X is selected from the following groups: NH, NPh, N- (2-Py), N- (3-Py), N- (4-Py), N-2 -pyrimidyl, N-5-pyrimidyl for the preparation of medicaments useful for preventing or treating diseases in which abnormal production of nitric oxide (NO) by inducible NOsynthase induction (NOS-2 or iNOS) is involved.

In the preceding definitions and those which follow, the alkyl radicals contain 1 to 4 carbon atoms in straight or branched chain. Abbreviations Bn, Py, Ph mean respectively benzyl, pyridyl, phenyl.

The compounds of formula (I) have one or more asymmetric carbons and can therefore be in the form of racemic, enantiomeric and

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 diastereoisomers; these are also part of the invention as well as their mixtures.

X Y FNH 1-NH kNk H (la) Ces tautomères font également partie de l'invention. Furthermore, the compounds of formula (1) may be in the tautomeric form (Ia):

These tautomers are also part of the invention.

4- (morpholin-4-ylméthyl)-4, 5-dihydro-1, 3-thiazol-2-ylamine 4- (pypérazin-l-ylméthyl) -4, S-dihydro-l, 3-thiazol-2-ylamine 4- (4-méthyl-pypérazin-1-ylméthyl)-4, 5-dihydro-1, 3-thiazol-2-ylamine leurs racémiques, énantiomères, diastéréoisomères, tautomères ainsi que leurs sels pharmaceutiquement acceptables, Parmi les composés utiles selon l'invention et particulièrement préférés on peut citer le composé suivant : 4- (4-méthyl-pypérazin-l-ylméthyl)-4, 5-dihydro-1, 3-thiazol-2-ylamine son racémique, ses énantiomères, tautomères ainsi que leurs sels pharmaceutiquement acceptables. Among the compounds of formula (I) that are useful according to the invention, mention may be made of the following compounds:

4- (4-morpholin-4-ylmethyl) -4,5-dihydro-1,3-thiazol-2-ylamine 4- (piperazin-1-ylmethyl) -4,5-dihydro-1,3-thiazol-2-ylamine 4- (4-methyl-piperazin-1-ylmethyl) -4,5-dihydro-1,3-thiazol-2-ylamine, racemic, enantiomeric, diastereoisomeric, tautomeric and pharmaceutically acceptable salts thereof; invention and particularly preferred there may be mentioned the following compound: 4- (4-methyl-piperazin-1-ylmethyl) -4,5-dihydro-1,3-thiazol-2-ylamine its racemic, its enantiomers, tautomers as well as their pharmaceutically acceptable salts.

The invention also relates to the pharmaceutical compositions containing as active principle a derivative of formula (I) for which either Y is a methylene (CH 2) and X is chosen from the following groups: O, NH, N-Alkyl (Cl- C4), N-Bn, NPh, N- (2-Py), N- (3-Py), N- (4-Py), N-2-pyrimidyl, N-5-pyrimidyl, S, SO, SO2 , CH2

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 or CHPh; or Y is a carboxy (C = O) and X is selected from the following groups: NH, N-Ph, N- (2-Py), N- (3-Py), N- (4-Py), N -2-pyrimidyl, N-5-pyrimidyl and its racemic, enantiomeric, diastereoisomeric and mixtures thereof, tautomeric and pharmaceutically acceptable salts thereof.

dans laquelle X et Y ont les mêmes significations que dans la formule (1). The compounds of formula (1) can be prepared by cyclization of a derivative of formula:

wherein X and Y have the same meanings as in formula (1).

This cyclization is generally carried out using an acid such as hydrochloric acid, in an aqueous medium, at a temperature in the region of 100 ° C. 6N hydrochloric acid is preferably used.

The derivatives of formula (II) can be obtained according to the following reaction scheme:

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dans ces formules X et Y ont les mêmes significations que dans la formule (1), Ra est un groupe protecteur de la fonction amine tel que ceux décrits par T. W. GREENE, Protective groups in Organic Synthesis, J. Wiley-Interscience Publication (1991), de préférence un radical acétyle ou tert-butoxycarbonyle et Rb est un radical alkyle (1- 4C) ou alcoxycarbonyle, de préférence, méthyle, éthyle ou isobutyloxycarbonyle.

in these formulas X and Y have the same meanings as in formula (1), Ra is a protecting group of the amine function such as those described by TW GREENE, Protective groups in Organic Synthesis, J. Wiley-Interscience Publication (1991) preferably an acetyl or tert-butoxycarbonyl radical and Rb is a (1-4C) alkyl or alkoxycarbonyl radical, preferably methyl, ethyl or isobutyloxycarbonyl.

The reaction is generally carried out in the presence of a Lewis acid such as iron trichloride (III), in a solvent such as dichloromethane or acetonitrile, at a temperature between 10 C and the temperature boiling of the reaction medium. When X represents NH, X may be mono-protected beforehand by a protective group of the amine function such as those described by TW GREENE, Protective groups in Organic Synthesis, J. Wiley-Interscience Publication (1991), preferably a radical tert The reduction reaction b is preferably carried out using a hydride such as sodium borohydride or lithium aluminum hydride, in an alcohol.

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 aliphatic (1-4C) or tetrahydrofuran, at a temperature between 0 C and 30 C.

The deprotection reaction c is carried out with a deprotection agent for the compounds for which Ra is a group protecting the amine function by any deprotection method known to those skilled in the art and in particular those described by TW GREENE, Protective groups in Organic Synthesis, J. Wiley-Interscience Publication (1991). Preferably, when the protective group is an acetyl radical, this reaction is carried out using aqueous hydrochloric acid at a temperature in the region of 100 ° C. When the protective group is a tert-butoxycarbonyl radical, this reaction is carried out by means of hydrochloric acid in the dioxane, at a temperature of 20 C.

The reaction is carried out by the action of tert-butyl isothiocyanate, in an inert solvent such as an aliphatic alcohol (1-4C) (methanol, ethanol preferably), optionally in the presence of a tertiary amine such as triethylamine, at a temperature between 20 C and the boiling temperature of the reaction medium.

l'acide 4-nitroperbenzoïque, l'acide peracétique, l'acide pertrifluoroacétique, l'acide performique, l'acide monoperphthalique) ou un peracide minéral ou un sel d'un peracide minéral (par exemple l'acide periodique ou persulfurique), au sein d'un solvant inerte tel qu'un solvant chloré (chloroforme, dichlorométhane par exemple), à une température comprise entre 0 et 20 C. On peut utiliser également le peroxyde d'hydrogène ou un periodate (periodate de sodium par exemple), au sein d'un solvant inerte tel qu'un alcool aliphatique inférieur, l'eau ou un mélange de ces solvants, à une température comprise entre 0 et 20 C. Ces produits peuvent être aussi préparés à partir des composés de formule (II) correspondants, eux-mêmes obtenus selon le schéma réactionnel suivant : The compounds of formula (1) for which X represents either SO or SO 2 can be obtained by direct oxidation of the compound of formula (1) for which X represents S. This oxidation is carried out according to the known methods for the oxidation of sulfur derivatives. as those described by M. HUDLICKY, Oxidation in Organic Chemistry, ACS Monograph, 186, 252-263 (1990). For example, the reaction is carried out by the action of an organic peracid or a salt of an organic peracid (percarboxylic or persulfonic acid, especially perbenzoic acid, 3-chloro-perbenzoic acid,

4-nitroperbenzoic acid, peracetic acid, pertrifluoroacetic acid, performic acid, monoperphthalic acid) or a mineral peracid or a salt of a mineral peracid (for example periodic or persulfuric acid), in an inert solvent such as a chlorinated solvent (chloroform, dichloromethane for example), at a temperature between 0 and 20 C. It is also possible to use hydrogen peroxide or a periodate (sodium periodate for example) in an inert solvent such as a lower aliphatic alcohol, water or a mixture of these solvents, at a temperature between 0 and 20 C. These products can also be prepared from the compounds of formula (II) ) corresponding, themselves obtained according to the following reaction scheme:

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La réaction d'oxydation a s'effectue selon les méthodes connues d'oxydation des dérivés soufrés comme celles décrites ci-dessus.

The oxidation reaction was carried out according to known methods of oxidation of sulfur derivatives such as those described above.

The deprotection reaction b for the compounds for which Ra is a protective group for the amine function is carried out by any deprotection method known to those skilled in the art and in particular those described by TW GREENE, Protective groups in Organic Synthesis, J. Wiley-Interscience Publication (1991). Preferably, when the protective group is an acetyl radical, this reaction is carried out using aqueous hydrochloric acid at a temperature in the region of 100 ° C. When the protective group is a tert-butoxycarbonyl radical, this reaction is carried out by means of hydrochloric acid in the dioxane, at a temperature of 20 C.

The reaction is carried out by the action of tert-butylisothiocyanate, in an inert solvent such as an aliphatic alcohol (1-4C) (methanol, preferably ethanol), optionally in the presence of a tertiary amine such as triethylamine, at a temperature between 20 C and the boiling temperature of the reaction medium.

The compounds of formula (1) are isolated and can be purified by the usual known methods, for example by crystallization, chromatography or extraction.

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 The enantiomers of the compounds of formula (I) can be obtained by resolution of the racemic compounds, for example by chromatography on a chiral column according to PIRCKLE W.H. et al., Asymmetric synthesis, vol. 1, Academic Press (1983) or by salt formation or synthesis from chiral precursors. The diastereoisomers can be prepared according to known conventional methods (crystallization, chromatography or from chiral precursors).

The compounds of formula (1) may optionally be converted to addition salts with an inorganic or organic acid by the action of such an acid in an organic solvent such as an alcohol, a ketone, an ether or a solvent chlorine. These salts are also part of the invention.

As examples of pharmaceutically acceptable salts, mention may be made of the following salts: benzenesulphonate, hydrobromide, hydrochloride, citrate, ethanesulphonate, fumarate, gluconate, iodate, isethionate, maleate, methanesulphonate, methylene-bis-boxynaphthoate, nitrate, oxalate, pamoate, phosphate, salicylate, succinate, sulfate, tartrate, theophyllinacetate and p-toluenesulfonate.

The compounds of formula (1) are inhibitors of inducible NO-synthase or NOsynthase type 2 (NOS-2) and are thus useful for the prevention and treatment of disorders related to excessive production of NO such as multiple sclerosis. Focal or global cerebral ischemia, brain or spinal trauma, Parkinson's disease, Huntington's disease, Alzheimer's disease, amyotrophic lateral sclerosis, migraine, depression, schizophrenia, anxiety, epilepsy, diabetes, atherosclerosis, myocarditis, arthritis, osteoarthritis, asthma, irritable bowel syndrome, Crohn's disease, peritonitis, gastroesophageal reflux disease, uveitis, Guillain-Barré, glomerulo-nephritis, lupus erythematosus, psoriasis, the growth of certain types of tumors such as epitheliomas, adenocarcinomas or sarcomas, and infections with intracellular or extracellular bacteria ularia, gram-plus or gram-minus.

Their activities as inhibitors of NOS-2 and NOS-3 were determined by measuring the conversion of [H] -L-arginine to [H] -L-citrulline by, respectively, a NOS-2 enzymatic fraction extracted from lungs of rats or mice previously treated with lipopolysaccharides (10 mg / kg ip 6 hours before tissue collection) and with a commercial preparation of recombinant beef NOS-3.

The compounds were incubated for 20 to 30 minutes at 37 ° C in the presence of 5 μM.

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(pour activité NOS-2) ou 10 uM (pour activité NOS-3) de [H]-L-arginine, 1 mM de NADPH, 15 pom de tétrabiopterine, l, uM de FAD, 0. 1 mM de DTT dans un tampon HEPES (50 mM, pH 6,7) contenant 10/lglml de calmoduline et 1.25 mM de CaC12 lorsque l'activité NOS-3 a été mesurée. L'incubation a été arrêtée par addition de tampon HEPES froid (100 mM, pH 5,5) contenant 10 mM d'EGTA et 500 mg d'une résine cationique échangeuse d'ion (AG50W-X8, contre-ion : Na+) pour séparer la [H]-L-arginine de la jH]-L-citrulline. Après 5 min de décantation, la radioactivité restant dans la phase liquide a été mesurée dans un compteur à scintillation en présence d'un liquide scintillant approprié. Le rendement de la récupération de la L- jH] citrulline formée a pu être estimée en utilisant de la L- [ureido-C]-citrulline comme standard externe.

(for NOS-2 activity) or 10 μM (for NOS-3 activity) of [H] -L-arginine, 1 mM NADPH, 15 μM tetrabiopterin, 1 μM FAD, 0.1 mM DTT in a HEPES buffer (50 mM, pH 6.7) containing 10 μg / ml calmodulin and 1.25 mM CaCl 2 when NOS-3 activity was measured. Incubation was stopped by addition of cold HEPES buffer (100 mM, pH 5.5) containing 10 mM EGTA and 500 mg cationic exchange ionic resin (AG50W-X8, counterion: Na +) to separate [H] L-arginine from L-citrulline. After 5 min of decantation, the remaining radioactivity in the liquid phase was measured in a scintillation counter in the presence of a suitable scintillation liquid. The yield of recovery of L-1H] citrulline formed could be estimated using L- [ureido-C] -citrulline as an external standard.

NOS-2 or NOS-3 activity was expressed as picomol (s) of [3H] -L-citrulline formed per minute and per milligram of protein contained in the reaction medium.

In this test on the enzyme NOS-2, the IC50 of the compounds of formula (1) is less than or equal to 10 M.

The selectivity is measured by the ICso NOS-3 / ICso NOS-2 ratio. This selectivity is greater than 45.

The compounds of formula (1) exhibit low toxicity. Their LD50 is greater than 40 mg / kg subcutaneously in mice.

The following examples illustrate the invention.

4- (4-Méthyl-pipérazin-I-ylméthyl) -4, 5-dihydro-thiazol-2-ylamine trichlorhydrate

Example 1

4- (4-Methyl-piperazin-1-ylmethyl) -4,5-dihydro-thiazol-2-ylamine trihydrochloride

Une suspension de 0, 42 g de N- (tert-butyl) -N'-[2-hydroxy-I- (4-méthyl- pipérazin-1-ylméthyl) éthyl]-thiourée dans 3,9 cm3 d'une solution aqueuse d'acide chlorhydrique 6N est chauffée à une température voisine de 100 C pendant 5 heures. Après refroidissement, le milieu réactionnel est ensuite concentré à sec sous pression

A suspension of 0.42 g of N- (tert-butyl) -N '- [2-hydroxy-1- (4-methylpiperazin-1-ylmethyl) ethyl] thiourea in 3.9 cm 3 of a solution aqueous 6N hydrochloric acid is heated at a temperature of 100 C for 5 hours. After cooling, the reaction medium is then concentrated to dryness under pressure

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 reduced (2 kPa) at a temperature of 55 C. The meringue obtained is dried in a desiccator under vacuum (2 kPa) for 4 hours. 0.47 g of 4- (4-methyl-piperazin-1-ylmethyl) -4,5-dihydro-thiazol-2-ylamine trihydrochloride is thus obtained in the form of a very hygroscopic off-white meringue. Spectrum of R. M. N.

 1 H (300 MHz, (CD3) 2SO d6 with addition of a few drops of CD3COOD d4, 8 in ppm): from 2.55 to 2.90 (mf: 4H); 2.80 (s: 3H); from 2.95 to 3.30 (mf: 4H); from 3.30 to 3.60 (mf: 2H); 3.40 (dd, J = 11, 5 and 5.5 Hz: 1H); 3.69 (dd, J = 11, 5 and 7.5 Hz: 1H); 4.51 (mt: 1H).

A une solution de 1 g de 2-amino-3- (4-méthyl-pipérazinl-yl)-l-propanol chlorhydrate dans 20 cm3 d'éthanol anhydre et 1,43 cm3 de triéthylamine, on ajoute 0,78 cm3 de tert-butylisothiocyanate. Le mélange réactionnel est agité sous atmosphère inerte à

une température voisine de 20 C pendant 42 heures puis est chauffé à une température voisine de 50 C pendant 1 heure 30 min. Après refroidissement à une température voisine de 20 C, le milieu réactionnel est évaporé sous pression réduite (2 kPa) à une température voisine de 30 C. Le résidu d'évaporation est repris dans 10 cm3 d'eau et 40 cm3 de dichlorométhane. La phase aqueuse est extraite par 2 fois 30 cm3 de dichlorométhane. Les phases organiques sont réunies, lavées par 15 cm3 d'eau, séchées sur sulfate de magnésium, filtrées puis évaporées sous pression réduite

(2 kPa) à une température voisine de 20 C. On obtient ainsi 0, 42 g de N-(tert-butyl)N'-[2-hydroxy-l- (4-méthyl-pipérazin-I-ylméthyl) éthyl]thiourée, sous forme d'une meringue blanche. Spectre infra-rouge entre lamelles de KBr 3279 ; 3075 ; 2939 ; 1 2806 ; 1533 ; 1459 ; 1359 ; 1295 ; 1204 ; 1010 et 821 cm-l. N- (tert-Butyl) -N '- [2-hydroxy-1- (4-methyl-piperazin-1-ylmethyl) ethyl] thiourea

To a solution of 1 g of 2-amino-3- (4-methyl-piperazin-1-yl) -1-propanol hydrochloride in 20 cm3 of anhydrous ethanol and 1.43 cm3 of triethylamine, 0.78 cm3 of tert -butylisothiocyanate. The reaction mixture is stirred under an inert atmosphere at

a temperature close to 20 C for 42 hours and then is heated to a temperature of 50 C for 1 hour 30 min. After cooling to a temperature in the region of 20 ° C., the reaction medium is evaporated under reduced pressure (2 kPa) at a temperature in the region of 30 ° C. The evaporation residue is taken up in 10 cm 3 of water and 40 cm 3 of dichloromethane. The aqueous phase is extracted with twice 30 cm3 of dichloromethane. The organic phases are combined, washed with water (15 cc), dried over magnesium sulphate, filtered and then evaporated under reduced pressure.

(2 kPa) at a temperature in the region of 20 ° C. This gives 0.42 g of N- (tert-butyl) N '- [2-hydroxy-1- (4-methyl-piperazin-1-ylmethyl) ethyl] thiourea, in the form of a white meringue. Infra-red spectrum between lamellae KBr 3279; 3075; 2939; 2806; 1533; 1459; 1359; 1295; 1204; 1010 and 821 cm -1.

2-Amino-3- (4-methyl-piperazin-1-yl) -1-propanol hydrochloride

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chauffée à une température voisine de 100 C pendant 3 heures. Après refroidissement à une température voisine de 60 C, le milieu réactionnel est filtré et le filtrat est évaporé sous pression réduite (2 kPa) à une température voisine de 60 C. On obtient ainsi 1 g de 2-amino-3-(4-méthyl-pipérazinyl)-1-propanol, chlorhydrate sous forme d'une meringue collante de couleur beige. A suspension of 0.89 g of N- [2-hydroxy-1- (4-methyl-piperazin-1-ylmethyl) ethyl] acetamide in 10.3 cm 3 of a 6N aqueous hydrochloric acid solution is

heated at a temperature of about 100 C for 3 hours. After cooling to a temperature in the region of 60 ° C., the reaction medium is filtered and the filtrate is evaporated under reduced pressure (2 kPa) at a temperature in the region of 60 ° C. This gives 1 g of 2-amino-3- (4- methyl-piperazinyl) -1-propanol, hydrochloride in the form of a sticky meringue of beige color.

IR spectrum (KBr) 3337; 2955; 2637; 2522; 1617; 1457; 1062; 1009 and 962 cm -1.

Une solution sous atmosphère inerte de 3,27 g de 2- (acétylamino)-3- (4-méthyl- pipérazin-l-yl) propanoate de méthyle dans 100 cm3 de méthanol anhydre est refroidie à une température voisine de 10 C, puis on ajoute par spatulées 0,76 g de borohydrure de sodium. Le mélange réactionnel est agité pendant 5 heures à une température voisine de 20 C, puis on ajoute de nouveau 0,26 g de borohydrure de sodium et l'agitation est poursuivie pendant 38 heures. On coule ensuite 5 cm3 d'eau sur la masse réactionnelle qui est ensuite concentrée sous pression réduite (2 kPa) à une température voisine de 30 C. La pâte résiduelle obtenue est triturée avec du dichlorométhane et l'insoluble est filtré. Le filtrat est concentré sous pression réduite (2 kPa) à une température voisine de 20 C. Le résidu est purifiée par chromatographie sous pression d'argon (60 kPa), sur une colonne de gel de silice (granulométrie 40-63, um ; diamètre 5 cm ; hauteur 19 cm), en éluant par des mélanges successifs de dichlorométhane-méthanol-ammoniaque à 20% (98/2/0, 95/5/0,1, 90/10/0,2, 80/20/0,25, 50/50/0,25 en volumes). Les fractions contenant le produit attendu sont réunies et concentrées sous pression réduite (2 kPa) à une température voisine de 40 C. On obtient ainsi 0,92 g de N-[2-hydroxy-l- (4-méthyl- N- [2-Hydroxy-1- (4-methyl-piperazin-1-ylmethyl) ethyl] acetamide

A solution under an inert atmosphere of 3.27 g of methyl 2- (acetylamino) -3- (4-methylpiperazin-1-yl) propanoate in 100 cm3 of anhydrous methanol is cooled to a temperature in the region of 10 ° C. and then 0.76 g of sodium borohydride are added by spatulas. The reaction mixture is stirred for 5 hours at a temperature of 20 C, then 0.26 g of sodium borohydride is added again and stirring is continued for 38 hours. Then poured 5 cm3 of water on the reaction mass which is then concentrated under reduced pressure (2 kPa) at a temperature in the region of 30 C. The residual paste obtained is triturated with dichloromethane and the insoluble matter is filtered. The filtrate is concentrated under reduced pressure (2 kPa) at a temperature in the region of 20 ° C. The residue is purified by chromatography under argon pressure (60 kPa), on a column of silica gel (particle size 40-63 μm; diameter 5 cm, height 19 cm), eluting with successive mixtures of dichloromethane-methanol-ammonia 20% (98/2/0, 95/5 / 0.1, 90/10 / 0.2, 80/20 / 0.25, 50/50 / 0.25 by volume). The fractions containing the expected product are combined and concentrated under reduced pressure (2 kPa) at a temperature in the region of 40 ° C. This gives 0.92 g of N- [2-hydroxy-1- (4-methyl)

<Desc / Clms Page number 13>

pipérazin-l-ylméthyl) éthyl] acétamide, sous forme d'un liquide jaune. Spectre IR CH2Cb 3621 ; 3429 ; 3352 ; 2944 ; 2803 ; 1657 ; 1513 ; 1460 ; 1284 ; 1050 ; 1011 et 816 cm.

piperazin-1-ylmethyl) ethyl] acetamide as a yellow liquid. IR spectrum CH2Cb 3621; 3429; 3352; 2944; 2803; 1657; 1513; 1460; 1284; 1050; 1011 and 816 cm.

Methyl 2- (acetylamino) -3- (4-methyl-piperazin-1-yl) propanoate

A une solution de 8, 57 g de 2-acétamidoacrylate de méthyle dans 500 cm3 de dichlorométhane agitée sous atmosphère inerte, on ajoute 6,65 cm3 de Nméthylpipérazine puis 0,97 g de trichlorure de fer et l'ensemble est agité au voisinage de 20 C pendant 66 heures. On coule alors 300 cm3 d'une solution aqueuse de sulfate de sodium sur le mélange réactionnel qui est agité vivement puis filtré sur de la Célite. Après décantation, la phase organique est séchée sur du sulfate de sodium, filtrée puis concentrée à sec sous pression réduite (2 kPa) à une température voisine de 40 C pour donner un liquide de couleur orangée. La phase aqueuse est extraite par 3 fois 150 cm3 de dichlorométhane et tous les extraits organiques sont réunis, séchés sur du sulfate de sodium, puis concentrés sous pression réduite (2 kPa) à une température voisine de 20 C pour donner une huile jaune. Les deux intermédiaires issus des deux phases organiques sont réunis et purifiés par chromatographie sous pression d'argon (50 kPa), sur une colonne de gel de silice (granulométrie zum diamètre 5 cm ; hauteur 25 cm), en éluant par des mélanges successifs de dichlorométhane-méthanol-ammoniaque à 20% (99/1/0, 97/3/0, 90/10/0,25, 80/20/0,25 en volumes). Les fractions contenant le produit attendu sont réunies et concentrées sous pression réduite (2 kPa) à une température voisine de 30 C. On obtient ainsi 3,3 g de 2- (acétylamino)-3- (4-méthyl-pipérazinyl) propanoate de méthyle sous forme d'un liquide jaune. Spectre IR CCl43437 ; 3318 ; 2941 ; 2798 ; 1749 ; 1685 ; 1499 ; 1458 ; 1374 ; 1286 ; 1204 ; 1168 et 1014 cm-l.

To a solution of 8.57 g of methyl 2-acetamidoacrylate in 500 cm3 of dichloromethane stirred under an inert atmosphere, 6.65 cm3 of N-methylpiperazine and then 0.97 g of iron trichloride are added and the mixture is stirred in the vicinity of C for 66 hours. 300 cm3 of an aqueous solution of sodium sulphate are then poured onto the reaction mixture, which is stirred vigorously and then filtered through celite. After decantation, the organic phase is dried over sodium sulfate, filtered and then concentrated to dryness under reduced pressure (2 kPa) at a temperature in the region of 40 ° C. to give an orange-colored liquid. The aqueous phase is extracted with dichloromethane (3 × 150 cc) and all the organic extracts are combined, dried over sodium sulfate and then concentrated under reduced pressure (2 kPa) at a temperature in the region of 20 ° C. to give a yellow oil. The two intermediates resulting from the two organic phases are combined and purified by chromatography under argon pressure (50 kPa), on a column of silica gel (particle size zum diameter 5 cm, height 25 cm), eluting with successive mixtures of 20% dichloromethane-methanol-ammonia (99/1/0, 97/3/0, 90/10/25, 80/20/25 by volume). The fractions containing the expected product are combined and concentrated under reduced pressure (2 kPa) at a temperature in the region of 30 ° C. 3.3 g of 2- (acetylamino) -3- (4-methyl-piperazinyl) propanoate are thus obtained. methyl in the form of a yellow liquid. IR spectrum CCl43437; 3318; 2941; 2798; 1749; 1685; 1499; 1458; 1374; 1286; 1204; 1168 and 1014 cm -1.

The pharmaceutical compositions according to the invention consist of a compound of formula (I) or an isomer or a tautomer or a salt of such a compound, in the pure state or in the form of a composition in which it is associated with any other pharmaceutically compatible product, which may be inert or physiologically active. The

<Desc / Clms Page number 14>

 The medicaments according to the invention can be used orally, parenterally, rectally or topically.

As solid compositions for oral administration may be used tablets, pills, powders (gelatin capsules, cachets) or granules. In these compositions, the active ingredient according to the invention is mixed with one or more inert diluents, such as starch, cellulose, sucrose, lactose or silica, under an argon stream. These compositions may also comprise substances other than diluents, for example one or more lubricants such as magnesium stearate or talc, a dye, a coating (dragees) or a varnish.

As liquid compositions for oral administration, it is possible to use pharmaceutically acceptable solutions, suspensions, emulsions, syrups and elixirs containing inert diluents such as water, ethanol, glycerol, vegetable oils or vegetable oil. paraffin. These compositions may comprise substances other than diluents, for example wetting agents, sweeteners, thickeners, flavoring agents or stabilizers.

The sterile compositions for parenteral administration may preferably be aqueous or nonaqueous solutions, suspensions or emulsions. As a solvent or vehicle, water, propylene glycol, a polyethylene glycol, vegetable oils, in particular olive oil, injectable organic esters, for example ethyl oleate or other organic solvents may be used. suitable. These compositions may also contain adjuvants, in particular wetting agents, isotonic agents, emulsifiers, dispersants and stabilizers. Sterilization can be carried out in several ways, for example by aseptic filtration, by incorporating sterilizing agents into the composition, by irradiation or by heating. They can also be prepared as sterile solid compositions which can be dissolved at the time of use in sterile water or any other sterile injectable medium.

The compositions for rectal administration are suppositories or rectal capsules which contain, in addition to the active product, excipients such as cocoa butter, semi-synthetic glycerides or polyethylene glycols.

The compositions for topical administration may be, for example, creams, lotions, eye drops, mouthwashes, nasal drops or aerosols.

<Desc / Clms Page number 15>

 In human therapy, the compounds according to the invention are particularly useful for the treatment and / or prevention of multiple sclerosis, focal or global cerebral ischemia, cerebral or spinal traumas, Parkinson's disease, Huntington's disease. , Alzheimer's disease, amyotrophic lateral sclerosis, migraine, depression, schizophrenia, anxiety, epilepsy, diabetes, atherosclerosis, myocarditis, arthritis, osteoarthritis, asthma , irritable bowel syndrome, Crohn's disease, peritonitis, gastroesophageal reflux, uveitis, Guillain-Barré syndrome, glomerulo- nephritis, lupus erythematosus, psoriasis, the growth of certain forms of tumors such as epitheliomas, adenocarcinomas or sarcomas, and infections by intracellular or extracellular, Gram-plus or Gram-less bacteria.

The doses depend on the effect sought, the duration of treatment and the route of administration used; they are generally between 1 mg and 100 mg per day orally for an adult with unit doses ranging from 0.5 mg to 50 mg of active substance.

In general, the doctor will determine the appropriate dosage depending on age, weight and all other factors specific to the subject to be treated.

The following examples illustrate compositions according to the invention: EXAMPLE A Formulas are prepared, according to the usual technique, capsules dosed with 50 mg of active product having the following composition:

<Tb>
<tb> - <SEP> Compound <SEP> of <SEP> formula <SEP> (1) ............................ ......................... <SEP> 50 <SEP> mg
<tb> - <SEP> Cellulose .......................................... ................................. <SEP> 18mg
<tb> - <SEP> Lactose .......................................... ................................... <SEP> 55 <SEP> mg
<tb> - <SEP> Silica <SEP> colloidal ...................................... ........................... <SEP> 1 <SEP> mg
<tb> - <SEP> Carboxymethyl starch <SEP> sodium ...................................... <SEP> 10mg
<tb> -Talc <SEP> 10 <SEP> mg
<tb> - <SEP> Stearate <SEP> of <SEP> Magnesium <SEP> 1 <SEP> mg
<Tb>
EXAMPLE

<Desc / Clms Page number 16>

Tablets containing 50 mg of active product having the following composition are prepared according to the usual technique:

<Tb>
<tb> - <SEP> Compound <SEP> of <SEP> Formula <SEP> (I) <SEP> 50 <SEP> mg
<tb> - <SEP> Lactose <SEP> 104 <SEP> mg
<tb> - <SEP> Cellulose .......................................... ................................ <SEP> 40 <SEP> mg
<tb> - <SEP> Polyvidone .......................................... ............................. <SEP> lOmg
<tb> - <SEP> Carboxymethyl starch <SEP> sodium ...................................... .. <SEP> 22 <SEP> mg
<tb> - <SEP> Talc <SEP> 10 <SEP> mg
<tb> - <SEP> Stearate <SEP> of <SEP> Magnesium <SEP> 2 <SEP> mg
<tb> - <SEP> Silica <SEP> colloidal ...................................... ........................... <SEP> 2mg
<Tb>
- Mixture of hydroxymethylcellulose, glycerin, titanium oxide (72-3.5-24.5) qs 1 film-coated tablet terminated at 245 mg EXAMPLE C A solution for injection containing 10 mg of active product having the following composition is prepared:

<Tb>
<tb> - <SEP> Compound <SEP> of <SEP> formula <SEP> (1) ............................ ........................ <SEP> 10 <SEP> mg
<tb> - <SEP> Benzoic acid <SEP> ...................................... ........................ <SEP> 80mg
<tb> - <SEP> Alcohol <SEP> Benzyl <SEP> 0.06 <SEP> ml
<tb> - <SEP> Benzoate <SEP> of <SEP> sodium <SEP> 80 <SEP> mg
<tb> - <SEP> Ethanol <SEP> to <SEP> 95 <SEP>% .............................. .................................... <SEP> 0.4 <SEP> ml
<tb> - <SEP> Hydroxide <SEP> of <SEP> sodium <SEP> 24 <SEP> mg
<tb> - <SEP> Propylene <SEP> glycol <SEP> 1.6 <SEP> ml
<tb> - <SEP> Water .......................................... ................................ <SEP> q. <SEP> s. <SEP> p. <SEP> 4 <SEP> ml
<Tb>
The present invention also relates to the method of preventing and treating diseases in which abnormal production of nitric oxide (NO) by induction of inducible NO-synthase (NOS-2 or iNOS) is implicated by administration of a compound of formula (I) its racemic, enantiomeric, diastereoisomeric and mixtures thereof, tautomer and pharmaceutically acceptable salts thereof.

Claims (13)

 wherein either Y is methylene (CH 2) and X is selected from the following moieties: O, NH, N-Alkyl (Cl-C4), N-Bn, N-Ph, N (2-Py), N- ( 3-Py), N- (4-Py), N-2-pyrimidyl, N-5-pyrimidyl, S, SO, SO2, CH2 or CHPh; or Y is a carboxy (C = O) and X is selected from the following groups: NH, NPh, N- (2-Py), N- (3-Py), N- (4-Py), N-2 -pyrimidyl or N-5-pyrimidyl, it being understood that the (C1-C4) alkyl radicals contain 1 to 4 carbons in straight or branched chain. Abbreviations Bn, Py, Ph respectively mean benzyl, pyridyl, phenyl, racemic, enantiomeric, diastereoisomeric and mixtures thereof, tautomers and pharmaceutically acceptable salts thereof.

CLAIMS 1 Compounds of formula (1) 2 Compound according to Claim 1, characterized in that it is chosen from: 4- (morpholin-4-ylmethyl) -4,5-dihydro-1,3-thiazol-2-ylamine 4- (pyperazin-1-ylmethyl) ) -4,5-Dihydro-1,3-thiazol-2-ylamine 4- (4-methyl-piperazin-1-ylmethyl) -4,5-dihydro-1,3-thiazol-2-ylamine Their racemates, enantiomers , diastereoisomers and mixtures thereof, tautomers and pharmaceutically acceptable salts thereof. Compound according to any one of Claims 1 to 2, characterized in that it is chosen from: 4- (4-methyl-piperazin-1-ylmethyl) -4,5-dihydro-1,3-thiazol-2 ylamine <Desc / Clms Page number 18>  its racemic, its enantiomers, tautomers and their pharmaceutically acceptable salts. Compound according to any one of claims 1 to 3 used to prepare a medicament. Pharmaceutical composition characterized in that it comprises in a pharmaceutically acceptable medium, a compound defined according to any one of claims 1 to 3. Medicinal product according to claim 4, characterized in that it contains at least one compound defined according to any one of claims 1 to 3 for its therapeutic application in the treatment of diseases in which abnormal production of nitric oxide (NO inducible NO-synthase induction (NOS-2) is implicated. 7 Medicament according to claim 4 characterized in that it contains at least one compound defined according to any one of claims 1 to 3 for its therapeutic application in the treatment of Parkinson's disease. Process for the preparation of the compounds of formula (1) as defined in claim 1, characterized in that a derivative of formula:

 wherein X and Y have the same meanings as in claim 1. 9 Preparation process according to claim 8 characterized in that the cyclization is carried out in an acid medium at a temperature of 100 C. Preparation process according to Claim 9, characterized in that the acidic medium is preferably 6N hydrochloric acid <Desc / Clms Page number 19>  Process for the preparation of the compounds of formula (II) as defined in claim 8 and in which X and Y have the same meaning as in claim 1, characterized in that a compound of formula (IIa) is subjected

 Ra being a protecting group of the amine formation and Rb a (1-4C) alkyl radical or alkoxycarbonyl to the action of a reducing agent to obtain the compound of formula (IIb)

 that is subjected to the action of a deprotection agent in order to obtain a compound of formula (IIc)

 that is subjected to the action of tert-butylisothiocyanate to obtain a compound of formula (II)

<Desc / Clms Page number 20>  As intermediates, the compounds of formulas II, IIa, IIb, IIc as defined in claim 11. N- (tert-Butyl) -N '- [2-hydroxy-1- (4-methylpiperazin-1-ylmethyl) ethyl] thiourea intermediate products; N- [2-Hydroxy-1- (4-methyl-piperazin-1-ylmethyl) ethyl] acetamide; Methyl 2- (acetylamino) -3- (4-methyl-piperazin-1-yl) propanoate