NZ207840A

NZ207840A - Diphenylazomethine derivatives and pharmaceutical compositions

Info

Publication number: NZ207840A
Application number: NZ207840A
Authority: NZ
Inventors: J-P Kaplan
Original assignee: Synthelabo
Priority date: 1983-04-14
Filing date: 1984-04-13
Publication date: 1986-02-21
Also published as: FI841484A; JPS59199665A; IL71540A0; PT78429A; DK191684A; GR79857B; AU2682584A; PT78429B; NO841486L; ZA842798B; FR2544309A1; SE8402082L; FI841484A0; NL8401189A; DE3414051A1; FR2544309B1; GB2138000A; IT8420528A0; ES531605A0; DK191684D0

Description

New Zealand Paient Spedficaiion for Paient Number £07840 2 078 40 Priority Date(s): 14.

Complete Specification Filed: 1 Class: CP.a 61 . .'£« ,) . Jfi'?. J .Q&J . . .

Publication Date: .2 I. £EB .19&6 • • • P.O. Journal, No: COMPLETE SPECIFICATION "HYDRQXYLATED DIPHENYLAZOMETHINES, THEIR PREPARATION AND PHARMACEUTICAL COMPOSITIONS CONTAINING THEM" AI We, SYNTHELABO, a French Body Corporate of 58, rue de la. Glaciere, 75621 Paris, France, hereby declare the invention for which X / we pray that a patent may be granted to XitK/us, and the method by which it is to be performed, to be particularly described in and by the following statement:- (followed by page la) 207840 - la- HYDROXYLATED DIPHENYLAZOMETHINES, THEIR PREPARATION AND PHARMACEUTICAL COMPOSITIONS CONTAINING THEM The present invention relates to hydroxylated diphenylazomethines, their preparation and their use in 5 therapy.

The hydroxylated diphenylazomethines according to the invention correspond to the formula (I): in which n is an integer from 1 to 4, X^, and X^, which may be the same or different, each represent a hydrogen atom, a halogen atom, -OCH^ or a straight-chain or branched C^_4~alkyl group, R represents -NH2, -OH or -0_M P (wherein M represents an alkali metal or alkaline earth metal of valency p) and Z represents -COOH, -COOalkyl, -CONH2' -CONHalkyl, -CON(alky1)2, -CH2OH, -CH2Oalkyl, 2 0.78 40 2 -Oalkyl, -NC>2, -NH2, -NHalkyl or -NfalkylJjr each alkyl moiety having 1 to 4 carbon atoms.

Preferred compounds according to the invention are those of the formula wherein the various symbols are as defined above, and more 15 particularly those in which n is 2 or 3, X^ is a halogen atom or methyl, X2 is a halogen atom or methyl, R is -NI^, -OH or -ONa and Z is -CH2OCH3, -N(CH3)2 or -NH2.

According to the invention, the compounds of formula (I) can be prepared by reacting a benzophenone of the formula Z (II) c=o (II) X 2 3 078 40 with a compound of the formula H2N-(CH2)n~COR if appropriate in the form of a salt, such as the hydrochloride. The reaction can be carried out at a temperature of 20 to 80°C and in a solvent, such as methanol.

The starting benzophenones (II) can be prepared by methods described in the literature.

Thus benzophenones of formula (II) in which Z is -COOalkyl, -COOH, -CONH2, -CONHalkyl or -CON(alkyl)2 can be prepared by reacting a compound of formula (III) COOalkyl ch3 (III) with a compound of formula (IV) X ■ coc1 tr (iv) X3 in the presece of AlCl^ and in the solvent CH3N02 to provide a compound of formula (V) COOalkyl C = 0 (V) 2078 40 and, if desired, converting the -COOalkyl group into -COOH (as by treatment with NaOH), -CONH2 (as by treatment with ammonium hydroxide in acetone) or into -CONHalkyl or -CON(alkyl)2 (as by treatment with, say, CH^Nt^ in methanol).

Those benzophenones of formula (II) in which Z is -CH2OH or -CH20alkyl can be prepared by reacting a compound of formula (VI) (VI) with bromine in dichloromethane solvent in the presence of benzoyl peroxide, under reflux conditions, to provide a compound of formula (VII) (VII) and converting the -CH2Br group of the compound of formula (VII) into the group Z by treatment with water (Z = -CH2OH) 2 07840 or an alcohol such as methanol (Z = -COOalkyl) , under reflux conditions.

Benzophenones of formula (II) in which Z is -Oalkyl may be prepared by reacting a compound of formula (IV) above with a compound of formula (VIII) Oalkyl (VIII) in chloroform in the presence of triethylamine to provide a compound of formula (IX) Oalkyl C0C1 (IX) the compound of formula (IX) is introduced into a photochemical reactor with a benzene compound of formula (X) X, (X) and the mixture is irradiated for 20 hours in a nitrogen atmosphere. 2 07840 Finally, benzophenones of formula (II) in which Z is -N02, -NH2, -NHalkyl or -N(alkyl)2 can be prepared by reacting a compound of formula (XI) X (XI) X, in acetic acid with KNO^ dissolved in H2SO^ and, if desired, converting the resulting benzophenone of formula (II) in 15 which Z is -N02 into a benzophenone of formula (II) in which Z is -NH2, -NHalkyl or -N(alkyl)2 in known manner (as by reducing the ~N02 group to -NH2 with hydrogen in the presence of Raney nickel, using a solvent such as ethanol).

The following Examples illustrate the invention. 20 The structure of the compounds are confirmed by analyses and IR and NMR spectra. 2 078 40 Example 1 4-£[(4-Chlorophenyl)-(5-ch lo ro-2-hydroxy-3-metho xyphenyI)-methyleneDamino^j-butanamide. .4 cm' of an ethanolic 0.27 N solution of 5 sodium ethylate (that is to say 2.8 mmol) and 0.8 g (2.69 mmol) of 45-dich loro-2-hydroxy-3-methoxybenzophenone are added to a suspension of 0.37 g (2.69 mmol) of^-aminobutyramide hydrochloride in 20 cm' of absolute ethanol.

The mixture is heated to the reflux temperature for 1 hour and 20 cm' of alcohol are distilled off. 200 cm' of absolute alcohol are added and the same volume is distilled off again.

After evaporation to dryness, 20 cm' of water are 15 added to the residue and the mixture is extracted with methylene chloride.

The extract is washed with water and aried over MgSO^ to give, on evaporation, a residue, which is re-crystallised from absolute ethanol. After washing with 20 petroleum ether and drying at 100°C in vacuo for 8 hours, the product, of melting point 209-10°C, is obtained. 2 07840 Examp le 2 4-|c(4-Chlorophenyl)-(5-chloro-2-hydroxy-3-n)ethoxymethyl-pheny I)-methyleneDami noj-butanoic acid and its sodium salt. 1. 5 g (1.61 x 10-2 mol) of (4-c h lo roph eny I) - (5-c h lo ro-2-hydroxy-3-methoxymethyIphenyI )-methanone, 300 ml of methanol, 3.1 g (3 x 10"^ mol) of Y'aminobutyric acid and 1.6 g (3 x 10~2 mol) of sodium methylate are introduced into a 1 litre flask.

The reaction mixture is brought to the reflux tem perature for 8 hours and is evaporated to dryness, the residue is taken up in 1.8 litres of distilled water and the mixture is acidified to pH 4.5 by addition of citric acid. The mixture is extracted with two 400 ml portions of 15 methylene chloride, the organic phases are combined, washed with 500 ml of water, dried over NajSO^ and filtered and the filtrate is evaporated to dryness.

The acid obtained is recrysta 11 ised from 25 ml of methanol.

Melting point = 104 - 105°C. 2. 4.7 g (1.19 x 10 mol) of the acid obtained above, 100 ml of methanol and 9.7 ml of sodium methylate solution (1.22 N) are introduced into a 500 ml flask. The reaction mixture is evaporated at 60°C, 200 ml of pen-25 tane are introduced and the mixture is stirred for 10 minutes.

After filtration, draining and drying 'in a desic- 2 07840 cator at 60°C in the presence of t^,e' sodium salt is obtained.

Melting point = 136°C.

Example 3 U-\C(4-Ch lorophenyl)- (5-ch loro-2-hydroxy-3-dimethylamino-phenyl)-methylene3amino^-butanamide. 2.35 g (0.017 mol) of ^-aminobutyramide hydrochloride, 500 ml of ethanol, 17 ml of a molar solution of sodium methylate and 5.3 g (0.017 mol) of (4-chloro-10 phenyl)-(5-chloro-2-hydroxy-3-dimethylaminophenyl)-methanone are introduced into a flask.

The reaction mixture is heated to the reflux temperature and the ethanol is distilled off.

The mixture is evaporated to dryness, the residue 15 is taken up in water and chloroform and the organic phase is decanted, dried over magnesium sulphate and evaporated.

The residue is triturated in pentane, filtered off and recrysta 11 ised from a mixture of ethyl acetate/iso-propylether.

Melting point = 144.5 - 145°C. 207840 The structure and properties of compounds of formula (I) are summarised in Table I.

TABLE I Compounds n X1 X2 X3 Z R Melting point (°C) 1 3 -Cl 4-C1 h C00CH3 NH2 168-169 2 3 -Cl 4-C1 H COOCH3 OH 141-142 3 3 -Cl 4-Cl h CONH2 nh2 143-144 4 3 -Cl 4-C1 H COOH OH 235-236 = 3 S-Cl 4-C1 rj orv ...2 - -1 -> 107- = 6 0 -Cl 4-Cl U CH^OH NH2 153 . 5-9 . 5 7 3 -Cl 4-Cl H CM -,CCH , OH T /-s A C lijn - b 8 ' 3 -Cl 4-Cl u CH,0CH, O'la 13 6 (decompo sition) Q y 3 -Cl 4-Cl H CONH, OH 214-5 3 -Cl 4-Cl H C0NHC,H- MH7 202-3 11 3 -Cl 4-Cl H C0N'HCH3 nh2 24 2-3 12 3 -Cl 4-Cl H OCH OH 153-4 13 3 -Cl 4-Cl H coi:hc3k7 ON a 160-1 14 3 -Cl 4-Cl u C0NHCH3 ON a > 250 (de- composition) 2 0/8 40 TABLE x (continued) Compounds n X1 X2 X3 fl z R Melting point (°C) 3 -Cl 4-Cl h OCH3 nh2 209-210 16 3 -Cl 4-Cl II NO 2 NH2 166-7 17 3 -Cl 4-Cl h M(CH3)2 ON a 153-158 18 3 -Cl 4-Cl h N(CH 3)2 nh2 144 . 5-5 19 3 -Cl 4-Cl H no2 ON a 163-165 3 -Cl 4-Cl H NE, ON a 257-9 21 3 -Cl 4-Cl H NH0 NH0 219-220 22 3 -Cl 4-Cl H CONHC3H? OH 216-7 23 -J -Cl 4-Cl H 1 1 COMHCHjj OH 218-9 24 3 -Cl 4-Cl H N(CH 3)2 , OH 159-160 -Cl 4-Cl I H NO 2 { | OH 206-208 i 2 6 3 -Cl 4-Ci! 1 U NH, i- 'OH 16 9 - 17 C The structure and properties of starting benzophenones of formula (II) are summarised in Table II.

TABLE II Compounds x1 X2 X3 z Melting point (°C) 1 -Cl 4-Cl h c02ch3 114-115 2 -Cl 4-Cl h conh2 205-206 3 -Cl 4-Cl h co2h 198-199 4 -Cl 4-Cl h ch2och3 95-97 -Cl 4-Cl h ch20h 102-103 6 -Cl i—1 u i h conhc3h7 103-104 -J / -Cl 4-Cl u C0NHCH3 169-170 8 -Cl 4-Cl k och, 142 . 5-142 9 --1 4-Cl * •* no 2 112-112 . 5 -Cl 4-Cl H .+■ 0 N (pw n r i. 3 ' 2 u 164-166 11 -Cl 4-Cl h nh ? 9 4 . 5-9 5 2078 40 Hydroxylated diphenylazomethines according to the invention have been subjected to tests on mice demonstrating their action on the central nervous system.

The antidepressive activity of the compounds was 5 demonstrated by antagonism to head twitches caused by L-5-hydroxytriptophan (L-5-HTP) in mice.

The mice (CDI males, Charles River France; 18-22 g body weight) received increasing doses of the products to be studied, or the solvent, subcutaneously, together with 10 L-5-HTP in a dose of 250 mg/kg. 45 minutes after this injection of L-5-HTP, the number of head twitches of each mouse is counted for one minute.

For each treatment, the average number of head twitches and the percentage variation relative to a control group are 15 calculated.

AD^q (50% dose or dose which reduces the average number of head twitches by 50%) is determined from the dose-effect curve by the graphical method of Miller and Tainter (1944).

AD,-g on interperitoneal administration of the compounds 20 according to the invention varies from 40 to 60 mg/kg.

The anticonvulsive activity of the compounds was demonstrated by antagonism to the mortality induced by bicuculline in mice.

Bicuculline is a relatively selective blocker of 25 post-synaptic GABA-ergic receptors and its convulsive and lethal effects are antagonised by compounds which increase 2 078 40 the level of cerebral GABA or have a GABA-mimetic activity.

The 50% active dose (AD^q), that is to say the dose which protects 50% of the animals from the effect of bicuculline, of the substances studied was evaluated. 5 AD50 on intraPeritoneal administration of the compounds according to the invention varies from 10 to 100 mg/kg.

The compounds according to the invention are active antidepressants and anticonvulsants and also have antiulcer, anxiolytic,analgesic and antiinflammatory properties. They 10 can be used in human and veterinary therapy for the treatment of various diseases of the central nervous system, for example for the treatment of depressions, psychoses and some neurological diseases, such as epilepsy, spasticity and dyskinesia.

The invention accordingly relates to all pharmaceutical compositions containing the compounds (I) as active principles together with any excipients suitable for their administration, in particular oral (tablets, coated tablets, gelatine capsules, capsules, cachets and solutions or 20 suspensions for oral use) or parenteral administration.

Claims

WHAT WE CLAIM IS:

1. A hydroxylated diphenylazomethine of the formula (I) Z 10 in which n is an integer from 1 to 4, X^, X2 and X^, which may be the same or different, each represent a hydrogen atom, a halogen atom, -OCH^ or a straight-chain or branched C. .-alkyl group, R represents -NH_, -OH or -OM P (wherein M represents an alkali metal or alkaline earth 15 metal of valency p) and Z represents -COOH, -COOalkyl, -CONH2, -CONHalkyl, -CON(alkyl)2, -CH2OH, -CH2Oalkyl, -Oalkyl, -N02, -NH2, -NHalkyl or -N(alkyl)2, each alkyl moiety having 1 to 4 carbon atoms.

2. A compound according to claim 1, of the formula 20 2Q78 4< - 16 - C=N-(CH-) -COR i - n wherein the various symbols are as defined in claim 1.

3. A compound according to claim 1 or 2, in which n is 2 or 10 3, X^ is a halogen atom or methyl, X2 is a halogen atom or methyl, R is -NH2, -OH or -ONa and Z is -CH20CH3, -N(CH3)2 or -nh2.

4. A hydroxylated diphenylazomethine according to claim 1 substantially as described with reference to any one of 15 Compounds 1 to 28 in Table I.

5. A process for the preparation of a hydroxylated diphenylazomethine as claimed in claim 1, which comprises reacting a benzophenone of the formula (II) z X1 25 (ii) with a compound of the formula H2N-(CH2)n~COR, the various symbols being as defined in claim 1. 2078 40 - 17 -

6. A process according to claim 5 substantially as described with reference to Example 1, 2 or 3.

7. A pharmaceutical composition which comprises as active ingredient at least one hydroxylated diphenylazomethine as * r ■» claimed in any one of claims 1 to 4, together with a pharmaceutical^ acceptable excipient. ^ — ;jir Authorised Agents, A. J. PARK & SON N.Z. PATENT OFFI'. £ 13 APR 1914