FR2590566A1 - Keto-naphthalene derivatives, process for their preparation and their application in the pharmaceutical and cosmetic fields - Google Patents

Abstract

Keto-naphthalene derivatives, characterised in that they correspond to the following general formula: in which: R1-R4 represent -H or lower alkyl, or R1 and R3 together represent methylene or dimethylene, and R5 represents lower alkyl, -CH2OH or -CO-R6, R6 being especially -H, -OH, alkoxy, amino, dialkylamino and the like, their preparation and their application as therapeutic and/or cosmetic agents especially in the treatment of dermatological illnesses connected to keratinisation disorders.

Description

 The present invention relates to keto-naphthalene derivatives hereinafter designated under the name of "keto-naphthodifferins", their preparation process and their use in the therapeutic and cosmetic fields.

 Keto-naphthodifferins find application in the topical and systemic treatment of dermatological conditions linked to a disorder of keratinization (dlfférenclation, proliferation) and of dermatological conditions, or others, with an inflammatory and / or immuno-allergic component and in the treatment degenerative diseases of the connective tissue, as well as anti-tumor activity.

 In addition, these derivatives can be used in the treatment of atopy, whether cutaneous or respiratory, and rheumatoid psoriasis.

 They also find an application in the ophthalmological field, in particular for the treatment of corneopathies.

dans laquelle
R1, R2, R3 et R4 > identiques ou differents, représentent un atome
d'hydrogène ou un radical alkyle inférieur ayant de 1 à 6 atomes de carbone,
ou R1 et R3 pris ensemble forment un pont méthylène ou diméthylène,
R5 représente un radical alkyle inférieur, le radical -CH20H ou le radical -COR
R6 représentant un atome d'hydrogène, le radical -OR7

représentant un atome d'hydrogène, un radical alkyle ayant de 1 à 20 atomes de
carbone, un radical monohydroxyalkyle ou polyhydroxyalkyle, un radical aryle n*s ara1Evle ventuellement substitué(s), ou un reste d'un sucre, ou encore le radical

p étant 1,2 ou 3,
r' et r" identiques ou différents, représentant un atome d'hydrogène, un radical alkyle inférieur, un radical monohydroxyalkyle ou polyhydroxyalkyle éventuellement interrompu(s) par un hétéroatome, un radical aryle éventuellement substitué ou un reste d'amino-acide, d'amino ester ou de sucre aminé, ou encore pris ensemble forment un hétérocycle, substitué ou non,
et les sels des dits composés de formule (I).The keto-naphthodifferins according to the invention can be represented by the following general formula

in which
R1, R2, R3 and R4> identical or different, represent an atom
hydrogen or a lower alkyl radical having from 1 to 6 carbon atoms,
or R1 and R3 taken together form a methylene or dimethylene bridge,
R5 represents a lower alkyl radical, the radical -CH20H or the radical -COR
R6 representing a hydrogen atom, the radical -OR7

representing a hydrogen atom, an alkyl radical having from 1 to 20 atoms of
carbon, a monohydroxyalkyl or polyhydroxyalkyl radical, an aryl radical n * s ara1Evle optionally substituted, or a residue of a sugar, or the radical

p being 1,2 or 3,
r 'and r "identical or different, representing a hydrogen atom, a lower alkyl radical, a monohydroxyalkyl or polyhydroxyalkyl radical optionally interrupted by a heteroatom, an optionally substituted aryl radical or an amino acid residue, d amino ester or amino sugar, or taken together form a heterocycle, substituted or not,
and the salts of said compounds of formula (I).

 By alkyl radical having from 1 to 20 carbon atoms should be understood in particular the methyl, ethyl, propyl, ethyl-2-hexyl, octyl, dodecyl, hexadecyl and octadecyl radicals.

 By lower alkyl radical is meant a radical having from 1 to 4 carbon atoms, in particular the methyl, ethyl, isopropyl, butyl and tert-butyl radicals.

 The term “monohydroxyalkyl radical” should be understood to mean a radical having from 2 to 4 carbon atoms, in particular a 2-hydroxyethyl, 2-hydroxypropyl or 2-hydroxyethoxyethyl radical.

 The term “polyhydroxyalkyl radical” should be understood to mean a radical containing from 3 to 6 carbon atoms and from 2 to 5 hydroxyl groups such as the 2,3-dihydroxy-propyl, 1,3-dihydroxy-1,3-propyl radicals or the rest of pentaerythritol.

 The remainder of a sugar should be understood to mean a residue derived from glucose, mannitol or erythritol.

 Among the amino sugar residues, mention may be made of those derived from glucosamine, galactosamine or mannosamine.

 Among the alkoxy radicals having from 1 to 6 carbon atoms, there may be mentioned the methoy, isopropoxy and tert-butoxy radical.

 When the radicals r 'ct r "taken together form a heterocycle, this is preferably a piperidino, piperazino, morpholino pyrrolidino or (2-hydroxyethyl) -4 piperazino radical.

 When the compounds according to the invention are in the form of salts, they may be either zinc salts, an alkali or alkaline earth metal, or an organic amine, when they contain at least one function free acid (R5-COOH) or salts. of a mineral or organic acid, in particular of hydrochloride, hydrobromide or citrate when they contain at least one amine function.

dans laquelle
R1, R2, R3 et R4, identiques ou différents représentent un atome d'hydrogène ou le radical -CH3,
R5 représente le radical -CH2OH ou le radical -COR6,
R6 représentant un atome d'hydrogène, le radical -OR7

Among the keto-naphthodifferins of formula (I) which are particularly preferred according to the invention, mention may be made of those corresponding to the following formulas

in which
R1, R2, R3 and R4, identical or different, represent a hydrogen atom or the radical -CH3,
R5 represents the radical -CH2OH or the radical -COR6,
R6 representing a hydrogen atom, the radical -OR7

R7 representing a hydrogen atom or an alkyl radical having from 1 to 6 carbon atoms,
and r ′ or r ″ representing a hydrogen atom, a lower alkyl, 4-hydroxy phenyl, 2-hydroxy ethoxy ethyl or carboxy-1 methylthio-3 propyl radical.

in which R6 represents -OR7 or

R7 representing a hydrogen atom or an alkyl radical having from 1 to 6 carbon atoms,
and r 'or r "representing a hydrogen atom or a lower alkyl radical.

Among the compounds of formula (I), the following may especially be mentioned
1) (tetrahydro-5,6,7,8 tetramethyl-5,5,8,8 naphthyl) -20 carbonyl-6 naphthalene-carboxylic-2 and its methyl ester,
2) N-ethyl [(tetrahydro-5,6,7,8 tetramethyl-5,5,8,8 naphthyl) -2] carbonyl-6 naphthalene carboxamide-2,
3) rc (tetrahydro-5,6,7,8 tetramethyl-5,5,8,8 naphthyl) -20 carbonyl-6 naphthalene carboxaldehyde-2,
4) tetrametbyl-5,5,8,8 tetrahydro-5,6,7,8 naphthyl) -il carbonyl-6 hydroxymethyl-2 naphthalene,
5) N-hydroxy-2 ethoxyethyl [(tetramethyl-5,5,8,8 tetrahydro-5,6,7,8 naphthyl carbonyl-6 naphthalene, carboxamide-2,
6) Np-hydroxyphenyl (tetramethyl-5,5,8,8 tetrahydro-5,6,7,8 naphthyl-2) carbonyl-6 naphthalene carboxamide-2,
7) N- (ethoxycarbonyl-1-methylthio-propyl) [(tetramethyl-5,5,8,8 tetrahydro-5,6,7,8 naphthyl) -2 carbonyl-6 naphthalene carboxamide-2, 8) N - (carboxy-1-methylthio-propyl) t (tetramethyl-5,5,8,8 tetrahydro-5,6,7,8 naphthyl) -2] carbonyl-6 naphthalene carboxamide-2,
9) methano-5,8 tetrahydro-5,6,7,8 naphthyl) -2 carbonyl-6 naphthalene carboxylic-2 and its methyl ester,
10) acid 0 (tetrahydro-5,6,7,8 naphthyl) - carbonyl-6 naphthalene carboxylic-2 and its methyl ester,
11) N-ethyl [(tetrahydro-5,6,7,8 naphthyl) - carbonyl-6 naphthalene carboxamide-2,
the particularly preferred compounds according to the invention being the compounds of formula II above, and more particularly compounds 1 to 6 and 8.

The present application also relates to the process for the preparation of keto-naphthodifferins of formula (I) by condensation under the conditions of the FRIEDEL-CRAFTS reaction of a naphthalenic acid halide (2) on 1,2-tetrahydro , 3,4 naphthalene (1) optionally substituted in position-1,4, according to the following reaction scheme

X = lal (preferably Cl)
This reaction is carried out at room temperature in a chlorinated solvent such as dichloromethane or 1,2-dichloroethane.

Among the substituted derivatives of 1,2,3,4 tetrahydro naphthalene of formula (1) (R1 = R2 5 R3 = R4 7 {H particularly suitable for the condensation reaction, there may be mentioned 1,1,4 tetramethyl , 4-1,2,3,4 tetrahydro naphthalene (described in JACS, 62, 36-44, 1940) and 1,4-methano-1,2,3,4 naphthalene or benzonorbornene (described in
JOC 32, 893-901, 1967).

Preferably, the condensation reaction is carried out using a 6-alkoxycarbonyl acid halide-2 naphthalene carboxylic acid (compound of formula (2) in which R5 = COOR7, R7 = C1-C6 alkyl \
The halides of the alkoxy-carbonyl-6 naphthalene carboxylic-2 acids are obtained by monosaponification reaction of a 2,6-alkyl naphthalene dicarboxylate and formation of the corresponding acid chloride by action of thionyl chloride.

From the esters thus obtained, it is possible to access the corresponding acids by saponification reaction, the latter being able to be transformed into amides, by the action of an amine in the presence of
N, N'-carbonyl diimidazole (CDI) or also by reaction of this amine with the acid halides.

 Similarly, from the esters, access can be obtained by reduction to the corresponding alcohols and then by oxidation of the latter to the aldehydes.

 The present invention also relates to, as medicament, the keto-naphthodifferins of formula (I) as defined above.

 These compounds exhibit excellent activity in the ornithine decarboxylase inhibition test, after induction by "tape stripping" in the naked rat (see Dermatologica 169 n "4, 1984 M. Bouclier et al). measurement of the action of retinoids on cell proliferation phenomena.

 The keto-naphthodifferins according to the invention also exhibit activity in the differentiation test of mouse embryonic teratocarcinoma cells (Fg cell: Cancer.Res. 43 p.52-68, 1983). Finally, these compounds exhibit bactericidal activity and in particular on the specific germs of acne.

 The keto-naphthodifferins according to the invention have, compared to compounds of the same type, better stability to light and to oxygen, this being essentially due to the fact that they do not have an easily isomerizable or oxidizable double bond.

These compounds are particularly suitable for treating dermatological conditions linked to a disorder of keratinization (differentiation-proliferation) as well as dermatological conditions, or others, with an inflammatory and / or immunoallergic component in particular.
- vulgar, comedonian or polymorphic acnes, senile, solar acnes, and medical or professional acnes.

- widespread and / or severe forms of psoriasis, and other keratinization disorders, including ichthyosis and ichthyosiform states
- Darier's disease
- palmoplantar keratoderma
- leukoplakias and leukoplasiform states, lichen planus
- any benign or malignant, severe or extensive dermatological proliferation.

 They are also active in the treatment of tumors, rheumatoid psoriasis, cutaneous or respiratory atopy and for certain ophthalmological problems relating to corneopathies.

 The present invention therefore also relates to a new medicinal composition, intended in particular for the treatment of the aforementioned conditions, characterized in that it comprises, in a pharmaceutically acceptable carrier, at least one compound of formula (I) and / or one of its salts.

 As support for the compositions, any conventional support can be used, the active compound being dissolved either in the dissolved state or in the dispersed state in the vehicle.

 Administration can be by enteral, parenteral, topical or ocular route. Enterally, the drugs can be in the form of tablets, capsules, dragees, syrups, suspensions, solutions, powders, granules, emulsions. Parenterally, the pewent compositions are in the form of solutions or suspensions - for infusions or for injections.

 The compounds according to the invention are generally administered at a daily dose of approximately 0.01 pg / kg to 1 mg / kg of body weight.

 Topically, the pharmaceutical compositions based on the compounds according to the invention are in the form of ointments, tinctures, creams, ointments, powders, patches, soaked pads, solutions, emulsions, lotions, gels, sprays or suspensions.

 These topical compositions can be presented either in anhydrous form or in aqueous form according to the clinical indication.

 When the compounds according to the invention are used topically, good activity of these compounds is observed over a very wide dilution range; one can use, in particular, concentrations of active product ranging from 0.0001 Z to 5 Z by weight. It is of course possible to use higher concentrations when this is made necessary for a particular therapeutic application; however, the preferred concentrations of active product are between 0.001% and 1% by weight.

 By ocular route, these compositions are preferably in the form of eye drops.

 the keto-naphthodifferins of formula (I), according to the invention, also find an application in the cosmetic field, in particular in body and hair hygiene and in particular for acne for hair regrowth, anti-fall , to combat the oily appearance of the skin or hair, in the prevention or treatment of the harmful effects of the sun or in the treatment of physiologically dry skin.

 The present invention therefore also relates to a cosmetic composition containing, in a cosmetically acceptable carrier, at least one compound of formula (I) or one of its salts, this composition being in particular in the form of a lotion, gel, soap or shampoo.

 The concentration of compound of formula (I), in the cosmetic compositions, is between 0.0001 and 2% by weight and preferably between 0.001 and 0.1% by weight.

 The medicinal and cosmetic compositions according to the invention can contain inert additives or even pharmacodynamically or cosmetically active and in particular: hydrating agents such as thiamorpholinone and its derivatives or urea; antiseborrhoeic agents, such as S-carboxymethylcysteine, S-benzyl-cysteamine and their derivatives, tioxolone; anti-acne agents such as benzoyl peroxide; antibiotics such as erythromycin and its esters, neomycin, tetracy turkeys or polymethylene-4,5 isotiazolinones-3; agents promoting hair regrowth, such as "Minoxidil" (diamino-2,4-piperidino-6-pyridinine oxide-3) and its derivatives, Diazoxide (chloromethyl-3 benzothiadiazine-1,2,4 dioxide- l, l) and Phenytoln (5,5-diphenyl imidazolidinedione-2,4) or dsoxapropanium iodide; steroidal and nonsteroidal anti-inflammatory agents; carotenoids and, in particular, ss-carotene; anti-psoriatic agents such as anthralin and its derivatives and the acids eicosatetraynoSque-5,8,11,14 and triynoIque-5,8,11 and their esters and amides.

 The compositions according to the invention can also contain flavor-enhancing agents, preserving agents, stabilizing agents, humidity-regulating agents, pH-regulating agents, agents for modifying osmotic pressure, emulsifying agents, UV-A and UV-B filters, antioxidants such as α-tocopherol, butylhydroxy-anisole or butylhydroxy-toluene.

 We will now give, by way of illustration and without any limiting character, several examples of preparation of the active compounds of formula (I) according to the invention as well as examples of compositions containing them.

EXAMPLE I
Preparation of [(tetrahydro-5,6,7,8 tetramethyl-5,5,8,8 naphthyl) carbonyl-6 methyl naphthalene carboxylate 2.

(Compound of formula II with R1 = R2 = R3 = R4 = -CH3 and R5 -COOCH3)
To a suspension of 1.5 g (11.2 mmol) of anhydrous aluminum chloride in 10 cm 3 of anhydrous dichloromethane, a solution of 1.88 g (10 mmol) of 1,2-tetrahydro is added dropwise, 3.4 tetramethyl-1,1,4,4 naphthalene and 2.49 g (10 mmol) of chloride of 6-methoxycarbonyl acid-2-naphthalene carboxylic-2 in 60 cm3 of anhydrous dichloromethane. The mixture is stirred for 4 hours at room temperature, then poured into 100 cm3 of acidulated iced water. The organic phase is decanted. The aqueous phase is extracted once again using 100 cm × of dichloromethane. The methylene chloride phases are combined, washed with sodium bicarbonate, dried over sodium sulfate and then concentrated. 3.9 g of a yellow liquid are obtained, which crystallizes at ordinary temperature. This solid is washed with methanol and then recrystallized from 70 cm> dtisopropanol.

 2.1 g of C (tetrahydro-5> 6s7 8 tetramethyl-5,5,8,8 naphthyl) -g carbonyl-6 methyl-2-naphthalene carboxylate are obtained.

 The isopropanol is evaporated, the solid obtained is washed with a minimum of methanol and then recrystallized from this solvent. A second fraction of 0.7 g of expected product is thus isolated, identical to that obtained previously in the form of white crystals, the melting point of which is 134 C.

 The R.M.N.1H 60 HHz spectrum conforms to the expected structure.

Elementary analysis: C27 H28 3
Cal. % C: 80.97 H: 7.05 0: 11.98
Tr. Z 80.85 7.00 12.02
EXAMPLE II
Preparation of acid C (tetrahydro-5,6,7,8 tetramethyl-5,5,8,8 naphthyl) -22 carbonyl-6 naphthalene carboxylic-2 (Compound of formula II with R1R2 = R3 = R4 = -CH3 1 2 and R5 = -COOH)
A suspension of 2.5 of [(tetrahydro-5,6,7,8 tetramethyl-5,5,8,8 naphthyl) -2] carbonyl-6 methyl-2 naphthalene carboxylate obtained in the example
I is stirred for three hours in a mixture of 30 cm3 of methanol and 30 cm9 of 6N aqueous potassium hydroxide at a temperature between 50 and 600C and then left overnight at ordinary temperature. After adding 40 cm3 of water, the methanol is removed by evaporation under vacuum. The aqueous phase-thus obtained is cooled to 0 to 50C, then acidified to pH # 1 by addition of 6N hydrochloric acid. The precipitate obtained is then drained, washed with water, dried at 800C on potassium hydroxide.

 After two recrystallizations, one in 40 cm 3 of isopropanol, the other in 100 cm 3 of methanol, 1.7 g of acid C (tetrahydro-5,6,7,8 tetramethyl-5,5,8,8 naphthyl) - 7 carbonyl-6 naphthalene carboxylic-2 is isolated in the form of white crystals with a melting point of 2240 C.

 The spectrum of R.M.N. H 250 MHz conforms to the expected structure.

Elementary analysis: C26 H26 03
Calc. % C: 80.80 H: 6.78 O: 12.42
Tr.% 80.57 6.93 12.50
EXAMPLE III
Preparation of N-ethyl (tetrahydro-5,6,7,8 tetramethyl-5,5,8,8 naphthyl) -2} carbonyl-6 naphthalene carboxamide-2
(Compound of formula II with R1 = R2 = R3 = R4 = -CH3 and R = -CONHC2H5)
To a suspension of Ig (2.5 mmol) of acid (tetrahydro-5,6,7,8 tetramethyl-5,5,8,8 naphthyl) -2i1 carbonyl-6 naphthalene carboxylic-6, obtained in the example II, in 10 cm3 of anhydrous dichloromethane, 0.49 g (3 mmol) of N, N'carbonyl diimidazole is added with stirring at room temperature.

 Carbon dioxide is released. After one hour of stirring 0.17 cm3 (2.6 mmol) of anhydrous ethylamine are added. One hour later, the starting acid is completely transformed into the corresponding amide.

 The reaction medium is then diluted with 20 cm3 of dichloromethane, washed with 20 cm3 of normal sodium hydroxide, then with a batten until the pH of the washing waters is neutral, dried over sodium sulfate and concentrated to dryness.

 1 g of beige solid is obtained which is recrystallized from an isopropyl ether-acetonitrile mixture. Is thus isolated, after draining and drying the crystals, 0.65 g of N-ethyl C (tetrahydro-5,6,7,8 tetramethyl-5,5,8,8 naphthyl) -2] carbonyl-6 naphthalene carboxamide -2, in the form of white crystals with a melting point of 1550 C.

 The R.M.N1H and infrared spectra correspond to the expected structure.

Elementary analysis: C28 H31 NO2
Calc.%: C: 81.32 H: 7.56 N: 3.39 0: 7.74
Tr. Z: 81.33 7.53 3.30 7.72
EXAMPLE IV
Preparation of (methano-5,8 tetrahydro-5,6,7,8 naphthyl) - carbonyl-6 methyl-2-naphthalene carboxylate
(Compound of formula III with R6 OCH3)
A suspension of 1.08 g (7.5 mmol) of 1,4-methano-1,2,3,4-tetrahydro naphthalene and 2 g (8 mmol) of chloride of 6-methoxycarbonyl acid-2 naphthalene carboxylic-2 in 30 cm3 of anhydrous 1,2-dichloroethane, 1.3 g (9.75 mmol) of anhydrous aluminum chloride are added in portions over 45 min. The mixture is stirred for 5 hours at room temperature then poured into 80 cm3 of acidulated iced water. The organic phase is decanted. The aqueous phase is extracted once again using 60 cm9 of 1,2-dichloroethane. The 1,2-dichloroethane phases are combined, washed with sodium bicarbonate, dried over sodium sulfate and then concentrated. The solid obtained is dried under vacuum at 600C and then recrystallized first from ethyl acetate then from isopropanol. 1 g [(methano-5.8 tetrahydro-5,6,7,8 naphthyl) -2 carbonyl-6 methyl naphthalene carboxylate-2 is thus obtained in the form of white crystals with a melting point of 119 "C.

 The 1H 60MHz NMR spectrum conforms to the expected structure.

Elementary analysis: C24 H20 03
Calc. ZC: 80.87 H: 5.66 W: 13.47
Tr.% 80.82 5.69 13.25
EXAMPLE V
Preparation of 5,8-gethano-5,6,7,8 naphthyl tetrahydro) - 6-carbonyl-2-naphthalene carboxylic-2
(Compound of formula III with R6 = OH)
A suspension of 0.88 g (2.46 mmol) of (methano-5,8 tetrahydro-5,6,7,8 naphthyl) -2 carbonyl-6 methyl-naphthalene carboxylate-2 obtained in Example IV is stirred for two hours in a mixture of 15 cm3 of alcohol and 15 cm3 of 6N aqueous potassium hydroxide heated to reflux. After adding 60 cm9 of water, the alcohol is removed by evaporation under vacuum. The aqueous phase thus obtained is cooled to 0 to 50C and then acidified by adding 15 cm3 of 12N hydrochloric acid. The precipitate obtained is drained, washed with water, dried at 800C on potassium hydroxide.

 After recrystallization from 110 cm9 of methanol, 0.62 g of white crystals of acid 1 (5,8-methano-5,6,7,8 naphthyl) - 6-carbonyl-2-naphthalene-carboxylic-2 are obtained, the point of which is fusion is 243 "C.

 The spectra of R.M.N. 1H 250 MHz and 13C conform to the expected structure.

Elementary analysis: C23 H18 03
Calc. % C: 80.68 H: 5.30 0: 14.02
Tr. 7O 80.83 5.43 13.71
EXAMPLE VI
Preparation of [(tetrahydro-5,6,7,8 napRhtyl) -22 carbonyl-6 methyl naphthalene carboxylate-2 (Compound of formula II with R 1 = R2 = R3 = R4 = H and R5 = -COOCH3)
To a suspension of 1.59 g (12 mmol) of 1,2,3,4-tetrahrdro-naphthalene and 3 g (12.05 mmol) of 6-methoeycnrbonyl acid chloride-2 naphthalene carboxylic acid in 60 cm3 of dichlor 1.2 anhydrous ethane, 2.4 g (18 mmol) of anhydrous aluminum chloride are added in portions. The mixture is stirred for 6 hours at room temperature and then poured into 100 cm3 of acidulated ice water. The organic phase is decanted. The aqueous phase is extracted once again using 100 cm3 of 1,2-dicsaloroethane. The dichloroethane phases are combined, layered with sodium bicarbonate, dried over sodium sulfate and then concentrated to dryness. t1 crude ester obtained is rapidly purified by chromatography on silica gel with an 8/2 hexane / ether mixture, then recrystallized from isopropanol. 2 g of white crystals of [(tetrahydro-5,6,7,8 naphthyl) -2] carbonyl-6-2-naphthalene carboxylate-2 are thus obtained, the melting point of which is 1710 C.

 The spectrum of R.M.N. H 60 MHz conforms to the expected structure.

Elemental analysis: C23 H20 O3
Cal. % C: 80.21 H: 5.85 0: 13.94
Tr.% 80.16 5.91 13.85
EXAMPLE VII
Preparation of [(tetrahydro-5,6,7,8 naphthyl) - 6-carbonyl-naphthalene carboxylic-2 acid
(Compound formula II with R1 = R2 = R3 = R4 = H and R5 = -COOH)
A suspension of 1.50 g (4.35 mmol) of (tetrahydro-5,6,7,8 naphthyl-2) carbonyl-6 methyl naphthalene carboxylate 2 obtained in Example VI, is stirred for three hours in a mixture 25 cm3 of alcohol and 25 cm3 of 6 N aqueous potassium hydroxide heated to reflux. After adding 50 cm3 of water, the alcohol is removed by evaporation under vacuum. The aqueous phase thus obtained is diluted to 500 cm3 to completely dissolve the carboxylate and then acidified by addition of 25 cm3 of 12N hydrochloric acid. obtained is drained, washed with water, dried at 80 ° C. on potassium hydroxide.

 After recrystallization first from isopropanol and then from a methanol / acetone mixture 8/2, 1.1 g of white crystals of acid are obtained ((tetrahydro-5,6,7,8 naphthyl carbonyl-6 naphthalene carboxylic-2). with a melting point of 267 C.

 The spectra of R.M.N. H 250 MHz and 13C conform to the expected structure.

Elementary analysis
C22 H18 O3
Cal. % C: 79.98 H: 5.49 O: 14.53
Tr.% 80.18 5.52 14.24
EXAMPLE VIII
Preparation of N-ethyl [(tetrahydro-5,6,7,8 naphthyl) -2] carbonyl-6 naphthalene carboxamide-2
(Compound of formula II with R1 = R2 = R3 = R4 = H and R5 = -CONR C2H5)
A suspension of 165 g (0.5 mmol) of acid [(tetradydro-5,6,7,8 naphthyl) -2 carbonyl-6 naphthalene carboxylic-2, obtained in 11 Example VII, and of 97.5 mg (0 , 6 mmol) of N, N'-carbonyldiimidazole in 5 cm 3 of dry dichloromethane is stirred for 2 hours at room temperature. 0.04 cm3 (0.6 mmol) of anhydrous ethylamine is then added to the solution obtained. After 30 minutes of stirring, the reaction medium is diluted with 10 cm9 of water, washed successively with 10 cm3 of normal sodium hydroxide, 2 times 10 cm9 of water, 10 cm3 of hydrochloric acid N, and 10 cm3 of water. The dichloromethane phase is dried over sodium sulfate and then evaporated to dryness. The crude amide is dried under vacuum at 600C and then recrystallized from isopropyl ether containing a little methanol. 130 mg of pale yellow N-ethyl needles [(tetrahydro-5,6,7,8 naphthyl) - carbonyl-6 naphthalene carboxamide-2 are obtained, the melting point of which is 1370 C.

 The R.M.N. 1H 250 MHz and 13C spectra conform to the expected structure.

Elementary analysis:: C24 H23 NO2
Cal. % C: 80.64 H: 6.49 N: 3.92 O: 8.95
Tr.% 80.49 6.55 3.86 8.75
EXAMPLE IX
Preparation of (tetrahydro-5,6,8,8 tetramethyl-5,5,8,8 naphthyl) -2 / carbonyl-6 naphthalene carboxaldehyde-2 (Compound of formula II with R1 = R2 = R3 = RçCH3 and R5 = - CH = O)
This compound is prepared in two stages from the acid [(tetrahydro-5,6,7,8 tetramethyl-5,5,8,8 naphthyl) -27 carbonyl-6 naphthalene-carboxylic-2 prepared in Example II . In a first step the carbonyl and carboxylic acid functions are reduced to alcohol. In a second step the (tetrahydro-5,6,7,8 tetramethyl-5,5,8,8 naphthyl) - -1
(6-hydroxymethyl naphthyl) -2 -1 methanol is oxidized to the expected aldehyde.

 a) Preparation of C ([(tetrahydro-5,6,7,8 tetramethyl-5,5,8,8 naphthyl) -21-l p (hydroxymethyl-6 naphthyl) -2d -1 methanol.

 To a suspension of 225 mg (6 mmol) of lithium aluminum hydride in 10 cm 3 of anhydrous tetrahydrofuran stirred with OOC, 1.16 g (3 mmol) of acid prepared according to Example II are added at once. After one hour, the medium is stirred at ordinary temperature, the reaction being followed by C.C.M.

When all of the starting material is transformed, 100 cm3 of 0.1N hydrochloric acid is slowly added, then the mixture is extracted 4 times with 25 cm3 of ethyl ether. The ethereal phases are decanted, dried over sodium sulfate and the solvent is removed by evaporation under vacuum.

 The crude diol obtained is purified by passage over a column of silica gel and eluted with an acetic acid-dioxane-toluene mixture (2-8-90).

 After evaporation of the eluent, 0.9 g of p (tetrahydro-5,6,7,8 tetramethyl-5,5,8,8 naphthyl) -2c 0 (hydroxymethyl-6 naphthyl) -g-1 methanol is isolated. form of white crystals with a melting point of 1570C.

 The R.M.N1H 60 MHz spectrum conforms to the expected structure.

b) Oxidation of the previous diol
To a solution of the diol prepared above 0.8 g (2.1 mmol) in 20 cm 3 of anhydrous dichloromethane, stirred at room temperature, 0.55 g (2.5 mmol) of pyridinium chlorochromate is added. After 45 min, 30 g of silica gel are added and the whole is filtered through Celite. The filter is washed with dichloromethane and the solution is concentrated under reduced pressure. The product obtained is purified by chromatography on silica gel and eluted with an acetic acid-dioxane-toluene mixture (2/8/90). After concentrating the elution phases, then recrystallization from hexane, 0.52 g of (tetrahydro-5,6,7,8 tetramethyl-5,5,8,8 naphthyl) -2 carbonyl-6 naphthalene carboxaldehyde is obtained. 2 in the form of white crystals with a melting point of 1310C.

 The R.M.N. 1H 250 MHz conforms to the expected structure.

Elementary analysis: C26H2602
Calc. % C: 84.29 H: 7.07 0: 8.64
Tr.% 84.21 6.96 8.46
EXAMPLE X
Preparation of (tetramethyl-5,5,8,8 tetrahydro-5, 6,7,8 naphthyl) -i
6-carbonyl-2-hydroxymethyl-naphthalene.

(Compound of formula II with R 1 = R2 = R3 = R4 = -CH3 and R5 = -CH2OH)
To a solution of 0.3 g of 85% potassium hydroxide in 10 cm 3 of methanol,
stirred at 600C, 0.6g (1.6mmol) of t (tetramethyl-5,5,8,8) is added
tetrahydro-5,6,7,8 naphthyl) -43 carbonyl-6 formyl-2 naphthalene and 0.16 cm3
(1.9 mmoles) of formaldehyde in 37% aqueous solution. After 2 hours of agitation at
60-700C, methanol is distilled under normal pressure. We then add 10cm3
of water to the hot residue and cools to room temperature. The precipitate formed
is extracted with four times 25cm of ethyl ether. The ethereal phases are
washed with water then dried over sodium sulphate and evaporated to dryness under
reduced pressure The crude product is purified by chromatography on
silica 60 in the eluent mixture acetic acid / dioxane / toluene 2/8/90 followed
recrystallization from a hexane / acetone mixture. After drying,
obtains 140 mg of white crystals of tetramethyl-5,5,8,8 tetrahydro-5,6,7,8 naphthyl) -g carbonyl-6 hydroxymethyl-2 naphthalene whose melting point is 1620C. The NMR spectrum corresponds to the expected structure.

EXAMPLE XI
Preparation of 2-hydroxy-ethoxyethyl [(tetramethyl-5,5,8,8
tetrahydro-5,6,7,8 naphthyl) -i carbonyl-6 naphthalene carboxamide-2.

(compound of formula II with R1 = R2 = R3 = R4 = -CH3 and R5 = -CONH (CH2) 20- (CH2) 2-OH)
To a suspension of 0.9 g (2.33 mmol) of [tetramethyl-5,5,8,8 acid
tetrahydro-5,6,7,8 naphthyl-2carbonyl-6 naphthalene carboxylic-2 in 9cm9
of anhydrous dichloromethane, 490 mg (3.03 mmol) of
N, N'-carboxyldiimidazole. After 1 hour of stirring at room temperature, 0.27 cm 9 (2.57 mmol) of 2-hydroxyethoxy-ethylamine is added to the solution.
obtained. The reaction medium is stirred for 3 h at room temperature then diluted with 25 cm of dichloromethane and washed with water and dilute hydrochloric acid.

The dichloromethane phase is dried over sodium sulfate and then evaporated to dryness.

The crude amide is purified by chromatography on silica gel 60 in the eluent mixture dichloromethane / tetrahydrofuran 70/30. After evaporation and
drying, 0.65 g of white crystals of N-hydroxyethoxy-2 ethyl [(tetramethyl-5,5,8,8 tetrahydro-5,6,7,8 naphthyl-2 carbonyl-6 naphthalene) are obtained
carboxamide-2 of 800.

 The R.M.N. 1H 250 MHz spectrum conforms to the expected structure.

Elementary analysis: C30H35N04
Calc. C 76.08 H 7.45 N 2.96 O 13.51
Tr. 76.04 7.52 3.00 13.62
EXAMPLE XII
Preparation of Np-hydroxyphenyl (tetramethyl-5,5,8,8 tetrahydro-5,6,7,8 naphthyl-2) carbonyl-6 naphthalene carboxamide-2.

(compound of formula II with R1 = R2 = R3 = R4 = -CH3 and R5 = -CONH C6H4 p OH)
To a suspension of 0.9 g (2.33 mmol) of acid (tetramethyl-5,5,8,8 tetrahydro-5,6,7,8 naphthyl-2) carbonyl-6 naphthalene carboxylic-2 in 9cm9 of anhydrous dichloromethane , add 490mg (3.03mmol) of
N, N'-carbonyldiimidazole. After 1 hour of stirring at room temperature, lcm3 of pure N, N-dimethylformamide 0.31 g (2.8 mmol) of p-aminophenol is added to the solution obtained. The reaction medium is stirred overnight at room temperature. The starting acid not having completely reacted, O, lg of
N, N'-carbonyldiimidazole then 0.1 g of p-aminophenol and stirred for 2 h at room temperature. The reaction medium is then diluted with 50 cm 3 of dichloromethane washed with dilute hydrochloric acid and then with water until neutral. The dichloromethane phase is dried over sodium sulfate and then concentrated under reduced pressure. The crude amide is purified by chromatography on silica gel 60 in a toluene / dichloromethane / ethyl acetate 5/3/2 mixture. By recrystallization from an isopropyl ether / acetone mixture, 0.33 g of white crystals of Np-hydroxyphenyl (tetramethyl-5,5,8,8 tetrahydro-5,6,7,8 naphthyl-2) -carbonyl-6 naphthalene carboxamide are obtained. -2 with a melting point of 268-9 C.

 The R.M.N. 1H 250 MHz spectrum conforms to the expected structure.

Elementary analysis:: CH NO
32 32 3
Calc. C 80.47 H 6.54 N 2.93
Tr. 80.55 6.27 2.89
During the chromatography on silica, a second product is also isolated which, by recrystallization from an acetone / methanol mixture, provides 0.3 g of white crystals of N, O-bis (tetramethyl-5,5,8,8 tetrahydro-5, 6,7.8 naphthyl) -2 dicarbonyl-2,6 naphthyl amino-4 phenol with a melting point of 239-2400C.

 The R.M.N. H 250 MHz conforms to the structure described.

Elementary analysis:: CH NO
58 55 5
Calc. C 82.33 H 6.55 N 1.66 O 9.45
Tr. 82.13 6.73 1.65 9.25
This uncondensed product is saponified with 6N potassium hydroxide in an alcoholic medium for 5 hours at 500C. After dilution with water, evaporation of the alcohol under reduced pressure, and acidification with hydrochloric acid
concentrated, an equimolecular mixture of Np-hydroxyphenyl is obtained
(tetramethyl-5,5,8,8 tetrahydro-5,6,7,8 naphthyl-2) carbonyl-6 naphthalene
carboxamide-2 and acid (tetramethyl-5,5,8,8 tetrahydro-5,6,7,8 naphthyl-2)
carbonyl-6 naphthalene carboxylic-2. By chromatography on silica 60 in
a toluene / dichloromethane / ethyl acetate 5/3/2 mixture, thus isolating a
second fraction of 0.11 g of Np-hydroxyphenyl (tetramethyl-5,5,8,8
tetrahydro-5,6,7,8 naphthyl-2) carbonyl-6 naphthalene carboxamide-2 whose
melting point is identical to the previous one.

EXAMPLE XIII
Preparation of N- (ethoxycarbonyl-1 methylthio-3 propyl) [(tetramethyl-5,5,8,8 tetrahydro-5,6,7,8 naphthyl) -20 carbonyl-6 naphthalene
carboxamide-2.

(compound of formula II with R1 = R2 "R3 = R4 = -CH3 and R5 = -CONH-Cll- (CH2) 2-5-CH3)
C02C2H5
Stirred for 1 h 30 at 40-500C, a solution of 1.2 g (3, lmmoles) of Wtetramethyl-5,5,8,8 tetrahydro-5,6,7,8 naphthyl-2) carbonyl-6 naphthalene
carboxylic-2 and 605mg (3.72mmol) of N, N'-carbonyldiimidazole in 15cm3
anhydrous N, N-dimethyl formamide. Cool to 200C and add 730mg
(3.41 mmol) of hydrochloride of the ethyl ester of L-methionine then
0.48 cm3 (3.41 mmol) of triethylamine. After 1 hour of stirring at 200C then 2 hours at
40-500C, the reaction medium is poured onto 100cm9 of acidulated water.
15 minutes then filter the precipitate which is then washed thoroughly with acid
hydrochloric diluted then with water. After drying under vacuum at 700C, it is purified
by chromatography on silica 60 in a mixture
toluene / dichloromethane / ethyl acetate 5/3/2. After evaporation, we obtain
0.8g N- (1-carbethoxy-3-methylthio propyl) (tetramethyl5,5,8,8
tetrahydro-5,6,7,8 naphthyl) -2 carbonyl-6 naphthalene carboxamide-2 under the
form of a thick oil which turns into a glassy product after drying
extended under vacuum to 70-80 C.

 The R.M.N.1H 60MHz spectrum corresponds to the expected structure.

EXAMPLE XIV
Preparation of N- (carboxy-1 methylthio-3 propyl)
rtetramethyl-5,5,8,8 tetrahydro-5,6,7,8 naphthyl) - carbonyl-6 naphthalene
carboxamide-2.

(compound of formula II with R1 = R2 = R3 = R4 = -CH3 and
R5 = -CONH-CH- (CH2) 2-S-CH3)
CO2H
A suspension of 0.58 g (immole) of N- (ethoxycarbonyl-1 methylthio-3
propyl) (tetramethyl-5,5,8,8 tetrahydro-5,6,7,8 naphthyl) - carbonyl-6
Naphthalene carboxamide-2 obtained in Example XIII is stirred for 30 minutes in a mixture of 5 cm 3 of alcohol and 5 cm 3 of aqueous 6N potassium hydroxide heated to 500 C.

After adding 50 cm3, 11 alcohol is removed by evaporation under reduced pressure at 40-450C. The aqueous phase is then acidified with 3cm3 of 12N hydrochloric acid. The precipitate obtained is drained, washed with copious amounts of water and dried over potassium hydroxide at 700C and then taken up in lukewarm isorpopylic ether. After cooling, filtration and drying under vacuum at 700C, 0.4g of white crystals of N- (1-carboxy-3-methylthio-propyl) tetramethyl-5,5,8,8 tetrahydro-5,6,7,8 naphthyl is obtained. ) -2 carbonyl-6 naphthalene carboxamide-2 with a melting point of 171-20C.

The 1 H NMR 250 MHz spectrum conforms to the expected structure
Elemental analysis: C31H35NO4S 0.5H20
Calc. C 70.69 H 6.89 N 2.66 O 13.67 S 6.08
Tr. 70.95 6.87 2.59 13.55 5.98
EXAMPLES OF COMPOSITIONS:
A - ORAL ROUTE
Example 1 - 0.2 g tablet
Compound of Example II 0.001 g
Starch 0.114 g
Dicalcium phosphate 0.020 g
Silica 0.020 g
Lactose 0.030 g
Talc 0.010 g
Magnesium stearate 0.005 g
Example 2 - 0.2g tablet
Compound of Example V 0.005 g
Starch 0.114 g
Dicalcium phosphate 0.020 g
Silica 0.020 g
Lactose 0.030 g
Talc 0.010 g
Magnesium stearate 0.005 g
Example 3 - Oral suspension
in 5ml ampoules
Compound of Example III 0.001 g
Glycerin 0.500 g
Sorbitol 70% 0.500 g
Sodium saccharin 0.010 g
Methyl parahydroxybenzoate 0.040 g
Aroma qs

QSP purified water 5,000 ml
B - TOPICAL ROUTE
Example 4 - Ointment
Compound of Example I 0.020 g
Isopropyl myristate 81,700 g
Fluid petroleum jelly 9,100 g
Silica sold by the company
Disgusted under the name of
"Aerosil 200" 9.180 g
EXAMPLE 5 Anionic Oil-in-Water Cream
Compound of Example II 0.010 g
Dodecyl sodium sulfate 0.800 g
Glycerol 2,000 g
Stearyl alcohol 20,000 g
Capric acid triglycerides /
caprylic sold by the Company
Dynamit Nobel under the name of
"Miglyol 812" 20,000 g
Preservatives qs
Demineralized water 100,000 g
Example 6 - Gel
Compound of example V 0.050 g
Hydroxy-propyl cellulose sold
by the company Hercules under the
name of "Klucel HF" 2,000 g
Water / ethanol (50:50) QSP 100,000 g

Claims (16)

 1. Keto-naphthodifferins, characterized in that they correspond to the following general formula

 in which  R1, R2, R3 and R4, identical or different, represent a hydrogen atom olS a lower alkyl radical having from 1 to 6 carbon atoms,  or R1 and R3 taken together form a methylene or dimethylene bridge,  R5 represents a lower alkyl radical, the radical -CH2OH or the radical -COR6, R6 representing a hydrogen atom, the radical -OR7 or

 representing a hydrogen atom, an alkyl radical having from 1 to 20 carbon atoms, a monohydroxyalkyl or polyhydroxyalkyl radical, an aryl or aralkyl radical optionally substituted), or a residue of a sugar, or the radical

 p being 1,2 or 3,  r 'and r ", identical or different, representing a hydrogen atom, a lower alkyl radical, a monohydroxyalkyl or polyhydroxyalkyl radical optionally interrupted by a heteroatom, an optionally substituted aryl radical or an amino acid residue, amino ester or amino sugar, or taken together form a heterocycle, substituted or not, and the salts of said keto-naphthalene derivatives of formula (I).  2. Compounds according to claim 1, characterized in that the alkyl radical having from 1 to 20 carbon atoms is a methyl, ethyl, propyl, ethyl-2-hexyl, octyl, dodecyl, hexadecyl or octadecyl radical.  3. Compounds according to Claim 1, characterized in that the monohydroxyalkyl radical is a 2-hydroxy-ethyl 2-hydroxypropyl or 2-hydroxyethoxyethyl radical.  4. Compounds according to claim 1, characterized in that the polyhydroxyalkyl radical is a 2,3-dihydroxypropyl, 1,3-dihydroxy-2-propyl radical or the rest of pentaerythritol.  5. Compounds according to claim 1, characterized in that the remainder of a sugar is a residue derived from glucose, mannitol or erythritol.  6. Compounds according to claim 1, characterized in that the remainder of an amino sugar is a residue derived from glucosamine, galactosamine or mannosamine.  7. Compounds according to Claim 1, characterized in that the radicals r 'and r ", taken together, form a heterocycle taken from the group consisting of a piperidino, piperazino, morpholino pyrrolidino and (2-hydroxyethyl) -4 radical piperazino.  8. Compounds according to any one of claims 1 to 7, characterized in that they correspond to the following formula

 in which  R1, R2, R3 and R4, identical, represent a hydrogen atom or unradical -CH3, R5 represents the radical -CH2OH or the radical -COR6 R6 representing a hydrogen atom, the radical -OR7

 R7 representing a hydrogen atom or an alkyl radical having from 1 to 6 carbon atoms,  and r 'or r "representing a hydrogen atom, a lower alkyl radical hydroxy-4 phenyl, hydroxy-2 ethoxyethyl or carboxy-1 methylthio-3 propyl.  10. Compounds according to any one of Claims 1 to 7, characterized in that they correspond to the following formula:

  in which R6 represents -OR7 or

 R7 representing a hydrogen atom or an alkyl radical having from 1 to 6 carbon atoms,  and r 'or r "representing a hydrogen atom or a lower alkyl radical.  11. Compounds according to any one of claims 1 to 10, characterized in that they are taken from the group consisting of  acid 0 (tetrahydro-5,6,7,8 tetramethyl-5,5,8,8 naphthyl) -2 carbonyl-6 naphthalene carboxylic-2 and its methyl ester,  N-ethyl [(tetrahydro-5,6,7,8 tetramethyl-5,5,8,8 naphthyl) -2 carbonyl-6 naphthalene carboxamide-2, [- (tetrahydro-5,6,7,8 tetramethyl -5,5,8,8 naphthyl) -2 carbonyl-6 naphthalene carboxaldehyde-2,  (tetramethyl-5,5,8,8 tetrahydro-5,6,7,8 naphthyl) -2 carbonyl-6 hydroxymethyl-2 naphthalene,  N-hydroxy-2 ethoxyethyl [(tetramethyl-5,5,8,8 tetrahydro-5,6,7,8 naphthyl) -2] carbonyl-6 naphthalene, carboxamide-2,  N-p-hydroxyphenyl L (tetramethyl-5,5,8,8 tetrahydro-5,6,7,8 naphthyl-2)] carbonyl-6 naphthalene carboxamide-2,  N- (ethoxycarbonyl-1 methylthio-3 propyl) C (tetramethyl-5ss5s8,8 tetrahydro-5,6,7,8 naphthyl) -2] carbonyl-6 naphthalene carboxamide-2,  N- (carboxy-1-methylthio-propyl) [tetramethyl-5,5,8,8 tetrahydro-5,6,7,8 naphthyl) -20 carbonyl-6 naphthalene carboxamide-2,  E (methano-5,8 tetrahydro-5,6,7,8 naphthyl) -2J carbonyl-6 naphthalene carboxylic-2 acid and its methyl ester,  (tetrahydro-5,6,7,8 naphthyl) -3 carbonyl-6 naphthalene carboxylic-2 and its methyl ester,  N-ethyl (5,6,7,8 naphthyl) (naphthyl) - 6-carbonyl-naphthalene-carboxamide-2,  12. Process for the preparation of the compounds according to any one of claims 1 to 11, characterized in that it consists in condensing, under the conditions of the FRIEDEL-CRAFTS reaction, a naphthalenic acid halide of formula

 on tetrahydro-1,2,3,4 naphthalene optionally substituted in the 1,4-position of formula

 formulas in which:  X represents a halogen, preferably a chlorine atom,  R1, R2, R3, R4 and R; having the same meanings as those given in claim 1.  13. The method of claim 12, characterized in that the condensation reaction is carried out at room temperature in a chlorinated solvent such as dichlorometlane or 1,2-dichloroethane.  14. Medicine characterized in that it is an active compound of formula (I) or one of its salts according to any one of claims 1 to it or obtained according to any one of claims 12 or 13.  15. Pharmaceutical composition characterized in that it contains, in a vehicle suitable for administration by the enteral, parenteral, topical or ocular route, at least one active compound of formula (I) or one of its salts, according to any one of claims 1 to 11 or obtained according to any one of claims 12 or 13.  16. Pharmaceutical composition according to claim 15 characterized in that the active compound is present at a concentration between 0.0001 and 5 Z by weight and preferably between 0.001 and 1 Z by weight.  17. Use of a compound of formula (I) or of a salt thereof according to any one of claims 1 to 11 for the preparation of a pharmaceutical composition intended for the treatment of dermatological, rheumatic, respiratory ailments, tumors , as well as the treatment of ophthalmological conditions.  18. Cosmetic composition for body and hair hygiene, characterized in that it contains, in an appropriate cosmetic vehicle, at least one active compound of formula (I) or one of its salts according to any one of claims 1 to 11 or obtained according to any one of claims 12 or 13.  19. Cosmetic composition according to claim 18, characterized in that it contains from 0.0001 to 2%, and preferably from 0.001 to 0.1% by weight of the active compound.