Title of Invention | A PROCESS FOR PRODUCING PHENYLACETIC ACID DERIVATIVES |
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Abstract | The present invention relates to a process for the production of a compound of Formula I, or a pharmaceutically acceptable salt thereof, or a pharmaceutically acceptable prodrug ester thereof, where R is methyl or ethyl; R<sub>1</sub> is chloro or fluore; R<sub>2</sub> is hydrogen or fluoro R<sub>3</sub> is hydrogen, fluoro, chloro, methyl, ethyl, methoxy or hydroxyl; R<sub>4</sub> is hydrogen or fluoro; and R<sub>5</sub> is chloro, fluoro, trifluoromethyl or methyl, provided that R<sub>1</sub>, R<sub>2</sub>, R<sub>4</sub> and R<sub>5</sub> are not all fluoro when R is ethyl and R<sub>3</sub> is H; comprising the steps of: rearrangement and hydrolysis of a compound of formula IX to produce a compound of formula VIII transforming the compound of formula VIII into the compound of formula I. |
Full Text | The present invention relates to processes for the production of 2-phenylamino-5-alkylphenyl acetic acids (the compounds of formula I given below), intermediates therefor and pharmaceutically acceptable salts thereof and pharmaceutically acceptable prodrug esters thereof; wherein R is methyl or ethyl; R1 is chloro or fluoro; R2 is hydrogen or fluoro; R3 is hydrogen, fluoro, chloro, methyl, ethyl, methoxy, ethoxy or hydroxy; R4 is hydrogen or fluoro; and R5 is chloro, fluoro, trifluoromethyl or methyl, provided that Ri, R2, R4 and R5 are not all fluoro when R is ethyl and R3 is H. Accordingly in a first aspect the invention provides a process for the production of a compound of Formula I, or a pharmaceutically acceptable salt thereof, or a pharmaceutically acceptable and physiologically cleavable prodrug ester thereof, comprising cleaving a lactam of formula n wherein the symbols are as defined above with a base. The above processes may include, if desired, temorarily protecting any interfering reactive groups and then isolating the resulting conpound of the invention; and, if desired, converting the free carboxylic acid of the confound of formula I into a pharmaceutically acceptable ester derivative thereof; and/or if desired, converting the free acid of formula I into a salt or a resulting salt into the free acid or into another salt. The above processes may be carried out under conditions known in the art for the hydrolytic cleavage of lactams, preferably with a strong base, such as aqueous sodium hydroxide (e.g. a 30% aqueous solution of NaOH), optionally in the presence of a water miscible organic solvent such as ethanol or methanol, preferably at elevated temperature, e.g. at a temperature in the range from about 50° to 100°C, (for instance as generally described in US Patent 3,558,690). The resultant reaction mixture is conveniently neutralised with an acid, e.g. a mineral acid such as hydrochloric acid to give the free acid product of formula I, which may be recovered by crystallisation, e.g. on cooling of the reaction mixture to ambient temperature, and filtration. Pharmaceutically acceptable prodrug esters are ester derivatives which are convertible by solvolysis or under physiological conditions to the free carboxylic acids of formula I. Such esters are e.g. lower alkyl esters (such as the methyl or ethyl ester), carboxy-lower alkyl esters such as the carboxymethyl ester, nitrooxy-lower alkyl esters (such as the 4-nitrooxybutyl ester), and the like. Pharmaceutically acceptable salts represent metal salts, such as alkaline metal salts, e.g. sodium, potassium, magnesium or calcium salts, as well as ammonium salts, which are formed e.g. with ammonia and mono- or di-alkylamines, such as diethylammonium salts, and with amino acids such as arginine and histidine salts. Preferred confounds of formula I which may be prepared according to the present invention include: 5-methyl-2-(2",4"-dichloro-6"-methylanilino)phenylacetic acid; 5-methyl-2-(2", 3\ 5", 6"-tetrafluoroanilino)phenylacetic acid; 5-methyl-2-(2", 3", 4", 6"-tetrafluoroanilino)phenylacetic acid; 5-methyl-2-(2",6"-dichIoroaiulino)phenyIaceticacid; 5-methyl-2-(2",6"-dichloroanilino)phenylacetic acid, potassium salt; 5-methyl-2-(2",6"-dichloroanilino)phenylacetic acid, sodium salt; 5-methyl-2-(2"-chloro-6"fluoroanilino)phenylaceticacid; 5-methyl-2-(2",6"-dichloro-4"-methylanilino)phenylaceticacid; 5-methyl-2-(2"-chloro-6"-methylanilino)phenylaceticacid; 5-methyl-2-(2",4"-difluro-6"-chloroanilino)phenylaceticacid; 5-methyl-2-(2"-fluoro-4",6"-dichloroanilino)phenylaceticacid; 5-methyl-2-(2"-chloro-4"-fluoro-6"-methylanilino)phenylaceticacid; 5-ethyl-2-(2" -fluoro-6" -chloroanilino)phenylacetic acid; 5-ethyl-2-(2"-chloro-6"-methylanilino)phenylaceticacid; 5-ethyl-2-(2" ,3" ,6"-trifluroanilino)phenylacetic acid; 5-ethyl-2-(2" ,3" ,5" ,6"-tetrafluoro-4"-ethoxyanilino)phenylacetic acid; 5-ethyl-2-(2"-chloro-4",6"-difluroanilino)phenylaceticacid; 5-ethyl-2-(2",4"-dichloro-6"-fluoroanilino)phenylaceticacid; 5-ethyl-2-(2*,4"-dichloro-6"-methylanilino)phenylaceticacid; 5-ethyl-2-(2"-fluoro-4"-cliloro-6"-methylanilino)phenyIaceticacid; 5-ethyl-2-(2",4"-difluoro-6"-methylanilino)phenylaceticacid; 5-ethyl-2-(2"-cWoro-4"-fluoro-6"-methylanilino)phenylaceticacid; 5-methyl-2-(2"-chloro-4"-hydroxy-6"-fluoroamlino)phenylaceticacid; 5-methyl-2-(2"-fluoro-6"-trifluoromethylanilino)phenylacetic acid, and 5-methyl-2-(2",4"-dicWoro-6"-trifluoromethylanilino)phenylaceticacid, and pharmaceutically acceptable salts thereof; and pharmaceutically acceptable prodrug esters thereof. Standard mild oxidation conditions may be used, such as heating with catalytical amounts of palladium on charcoal in a proper solvent, e.g. xylene. The lactam of formula III may be prepared by coupling an aniline derivative of formula IV IV wherein the symbols are as defined above, with a cyclohexanone derivative of formula Va or an amino substituted cyclohexene derivative of formula Vb wherein R is ethyl or methyl and R" is lower alkyl or sunilar. Coupling of IV with Va and Vb typically involves elimination of water or the secondary amine, HNR"2, e.g. under acidic conditions. Vb may be prepared by reaction of the amino substitutes cyclohexene derivative of formula Vb" wherein R and R" are as defined above, with methyl or ethyl glyoxylate. Vb may be converted to Va by hydrolysis, for instance as hereinafter described in the Examles. Alternatively the lactam of formula II is obtained by cyclisation of a compound of formulaVII Particularly preferred compounds of formula I which may be prepared according to the present invention include: 5-methyl-2-(2", 3", 4", 6"-tetrafluoroanilino)phenylacetic acid; 5-methyl-2-(2",6"-dichloroanilino)phenylaceticacid; 5-methyl-2-(2"-chloro-6"fluoroanilino)phenylacetic acid; 5-methyl-2-(2",6"-dichloro-4"-methylanilino)phenylacetic acid; 5-methyl-2-(2"-chloro-6"-methylanilino)phenylacetic acid; 5-methyl-2-(2"-chloro-4"-fluoro-6"-methylanilino)phenylacetic acid; 5-ethyl-2-(2"-fluoro-6"-chloroanilino)phenylaceticacid; 5-ethyl-2-(2"-chloro-6"-methylanilino)phenylaceticacid; 5-ethyl-2-(2",3",6"-trifluroanilino)phenylacetic acid, and 5-ethyl-2-(2",4"-dichloro-6"-methylanilino)phenylaceticacid, and pharmaceutically acceptable salts thereof; and pharmaceutically acceptable prodrug esters thereof. Thus, preferably also the processes of the invention may be used to prepare compounds of formula I in which R is methyl or ethyl; R1, is chloro or fluoro; R2 is hydrogen; R3 is hydrogen, fluoro, chloro, methyl or hydroxy; R4 is hydrogen; R5 is chloro, fluoro or methyl; or a pharmaceutically acceptable salt or a pharmaceutically acceptable prodrug ester thereof. The lactam of formula II may be prepared by oxidation of a lactam of formula III wherein the symbols are as defined above. wherein the symbols are as defined above. The cyclisation process is conveniently carried out under Friedel-Crafts alkylation conditions, e.g. in the presence of a Friedel-Crafts catalyst such as aluminium chloride or ethyl aluminium dichloride, preferably at elevated temperature, e.g. a temperature in the range from about 100° to about 180°C. The cyclisation reaction may be carried out in the presence of an inert solvent such as dichlorobenzene, or preferably a melt of the compound of formula VII is heated with the Friedel-Crafts catalyst. The compound of formula VII is prepared by N-acylation of a diphenylamine of formula Vm wherein the symbols are as defined above with a haloacetyl chloride. For instance, the compound of formula Vni is heated, e.g. to about 80°C, with chloroacetylchloride. The product may be recovered by diluting the reaction mixture with solvent, e.g. 2-propanol, and crystallisation. The compound of formula VII may be obtained by rearrangement and hydrolysis of a compound of formula DC. wherein the symbols are as defined above. Conveniently the compound of formula IX is treated with an organic base, e.g. an alkali metal alkoxide such as sodium methoxide, preferably with heating, e.g. to a ten^erature of at least about 75°C. During this procedure an intermediate product of formula X, wherein the symbols are as defined above, forms as a result of the initial rearrangement reaction, but undergoes direct cleavage under the prevailing reaction conditions to give the diphenylamine compound of formula Vin. Alternatively the diphenylamine compound of formula Vin may be obtained by coupling of the corresponding halobenzene derivative of formula XI where X is a halogen, e.g. I or Br, and the other symbols are as defined above with p-toluidine or 4-ethyl aniline. Such a coupling reaction may be carried out by use of Buchwald chemistry. For example, the compound of formula XI and the p-tohiidine or 4-ethyl aniline are mixed with an organic base, e.g. sodium tertiary butylate, and an appropriate ligand, e.g. BINAP, in an organic solvent such as toluene; a palladium compound or catalyst precursor such as Pd(dba)2 is added and the reaction mixture is heated. After cooling and treatment with acid, e.g. HCl, the diphenylamine product of formula VIII may be recovered from the organic phase of the reaction mixture. In a further alternative, the diphenylamine compound of formula VIII may be obtained by coupling of the corresponding aniline derivative of formula IV as defined above with 4-bromotoluene or l-ethyl-4-bromobenzene. Such a coupling reaction may be carried out similarly by use of Buchwald chemistry. For example, the confound of formula IV and the 4-bromotoluene or l-ethyl-4-bromobenzene are mixed with an organic base, e.g. sodium tertiary butylate in an organic solvent such as toluene; a palladium compound or catalyst precursor e.g. Pd(dba)2, and a ligand, e.g. P(tBu)3, or BINAP, are added to this reaction mixture which is then stirred at elevated temperature, e.g. 110°C, until completion of the reaction, e.g. overnight. Similarly the diphenylamine product of formula VIE may be recovered from the organic phase of the reaction mixture, for instance after cooling and treatment with acid, e.g. HCl. The compound of formula IX may be prepared by alkylation of the corresponding phenol derivative of formula XII wherein the symbols are as defined above, with 2-chloro-N-(4-methylphenyl)acetamide or 2 ch]oro-N-(4-ethylphenyl)acetamide. For instance, the compound of formula XII and 2-chloro-N-(4-methylphenyl)acetaniide or 2-chloro-N-(4-ethylphenyl)acetamide are mixed in an organic solvent such as 2-propanol in the presence of a base, e.g. K2CO3, and the reaction mixture boiled until completion of the reaction, e.g. for about 4 hours. 2-chloro-N-(4-methylphenyl)acetamide and 2-chloro-N-(4-ethylphenyl)acetamide may be prepared, e.g. in situ, by reaction of 4-methyl- or 4-ethylaniline with chloroacetyl chloride. The compound of formula IX may be recovered from the reaction mixture if desired. Preferably, however, the compound of formula IX is not isolated but is converted to the compound of formula VHI, by rearrangement and hydrolysis as described above carried out on the product reaction mixture resulting from the alkylation of the compound of formula Xn. Alternatively the diphenylamine of formula Vni may be prepared by oxidation of the corresponding compound of formula XHI (or tautomer thereof) wherein the symbols are as defined above. The dehydrogenation reaction may be carried out by classical methods, for instance by treatment with iodine, e.g. I2 in THF/AcOH. The compound of formula XIII may be prepared by coupling of l-methoxy-4-methylcyclohexa-l,4-diene or l-methoxy-4-ethylcyclohexa-l,4-diene with an aniline derivative of formula IV as defined above. This coupling reaction may be carried out in the presence of a catalyst such as TiCl4, in organic solvents e.g. THF and chlorobenzene, preferably with cooling, e.g. at about -40°C. l-methoxy-4-inethylcyclohexa-l,4-diene or l-methoxy-4-ethylcyclohexa-l,4-diene may be prepared by partial reduction of 4-methyIanisole or 4-ethylanisole by Birch reduction, e.g. by treatment with Na in liquid ammonia, for instance as described by Subba Rao et al. Australian Journal of Chemistry 1992,45, p. 187-203. Conveniently the confound of formula Xni is not isolated, but the coupling reaction between the conpound of formula IV and the l-methoxy-4-niethylcyclohexa-1,4-diene or l-methoxy-4-ethylcyclohexa-l,4-diene, is followed by oxidation to give the diphenylamine derivative of formula VIII. In starting compounds and intermediates, which are converted to the compounds of formulae I to XDI in a manner as hereinbefore described, functional groups present such as amino, hydroxy and carboxyl groups, are optionally protected by conventional protecting groups that are common in preparative organic chemistry. Protected hydroxy, amino and carboxyl groups are those that can be converted under nuld conditions into free amino, hydroxy and carboxyl groups without other undesirable side reactions taking place. For example, hydroxy protecting groups are preferably benzyl or substituted benzyl groups. Processes for the preparation of the 2-phenylamino-5-alkylphenylacetic acid derivatives as described above are shown schematically on the following page. The processes for the production of the compounds of formulae II, HI, VII, Vin , IX, X and XIII as described above are included within the scope of the present invention. Thys in further aspects the invention includes a process selected from a) A process for the production of the lactam of formula II which comprises oxidizing of a lactam of formula III b) A process for the production of the lactam of formula n as defined above, which conprises cyclisation of a confound of formula VII c) A process for the preparation of a compound of formula ni as defined above comprising coupling an aniline derivative of formula IV with a cyclohexanone derivative of formula Va or an amino substituted cyclohexene derivative of formula Vb wherein R is ethyl or methyl and R" is lower alkyl or similar d) A process for the production of a compound of formula VII which comprises N-acylation of a diphenylamine of formula VIII with a haloacetyl chloride e) A process for the preparation of a compound of formula VIQ which comprises rearrangement and hydrolysis of a compound of formula IX. f) A process for the production of a compound of formula VIII which conprises coupling of a halobenzene derivative of formula XI in which X is halo, with p-toluidine or 4-ethyl-aniline; g) A process for the production of a compound of formula VIII which comprises coupling an aniline derivative of formula IV with 4-bromotoluene or l-ethyl-4- bromobenzene; h) A process for the production of a compound of formula VII which comprises cleavage of a compound of formula X i) A process for the formation of a compound of formula X which comprises rearrangement of a compound of formula DC j) A process for the production of a compound of formula DC which comprises alkylation of a compound of formula XII with 2-chloro-N-(4-methylphenyl)acetamide or 2 chloro-N-(4-ethylphenyl)acetamide k) A process for the production of a compound of formula VIII which con^rises alkylation of a compound of formula XII with 2-chloro-N-(4-methylphenyl)acetamide or 2 chloro-N-(4-ethylphenyl)acetamide followed by rearrangement and cleavage of the intermediate confound of formula DC; 1) A process for the production of a conq)Ound of formula Vin conq)rising oxidation of the corresponding conq)ound of formula XIII (or tautomer thereof) m) A process for the production of a compound of formula Xni which comprises coupling l-methoxy-4-methylcyclohexa-l,4-diene or l-methoxy-4-ethylcyclohexa-l,4-diene with an aniline derivative of formula IV as defined above, and n) A process for the production of a compound of formula VIII comprising coupling l-methoxy-4-methylcyclohexa-l,4-diene or l-methoxy-4-ethylcyclohexa-l,4-diene with an aniline derivative or formula IV, followed by dehydrogenation wherein all symbols used are as defined above. One or more of the processes a) to n) above may be used in appropriate sequence (see the scheme given above) in the preparation of the compound of formula I. Thus the invention further provides a process for the preparation of a compound of formula I wherein the symbols are as defined above, which comprises one or more of processes selected from processes a) to n) as defined above, optionally in combination with aprocess according to the first aspect of the invention. Still yet further the invention provides a compound of formula I, or a pharmaceutically acceptable salt thereof, or a pharmaceutically acceptable prodrug ester thereof, when prepared by a process which comprises one or more of processes a) to n) as defined above, preferably with a process according to the first aspect of the invention. The confounds of formulae II, HI, Vn, VIII, DC, X and XIII are included per se within the scope of the present invention. Thus in yet further aspects the invention provides a compound selected from: a) A compound of formula II b) A comound of formula HI c) A compound of formula VII d) A compound of formula VIII Compounds of formula XII in which at one of R1 or R6 is chlorine and the other is fluorine may be prepared by methods known in the art of chlorination of phenols, preferably in the presence of catalytic amounts of a secondary amine, e.g. diisopropylamine. In a preferred embodiment according to the present invention, the chlorination reaction comprises simultaneous addition of chlorine and phenol to the reaction mixture, preferably using hexane fraction as the solvent. It has been found that simultaneous addition of at least part, preferably the majority, of the chlorine and the phenol to the reaction mixture gives rise to high productivity and selectivity in production of the desired product as compared with the unwanted side products. Furthermore use of hexane fractions permits isolation of the desired phenol product in high purity (e.g. 99%) by crystallisation. The invention is further described by way of illustration only in the following Examples. EXAMPLES The diphenylamine compounds of Formula VIII are prepared by Buchwald chemistry as described below in Examples 1 and 2, either by coupling of an aniline derivative of Formula IV with 4-bromotoluene or l-ethyl-4-bromobenzene as described in Example 1, or by coupling of a halobenzene derivative of Formula XI with p-toluidine or 4-ethylaniline as described in Examples 2. The compounds of Formula Vni thus obtained may be converted into the corresponding compounds of Formula I by procedures as described below. Example la N-(2",3",4",6"-Tetrafluorophenyl)-4-methylaniline A mixture of 2,3,4,6-tetrafluoroaniline (0.72g, 4.4 mmol), 4-bromotoIuene (0.8g, 4.7mmol), toluene (55ml), sodium tert-butoxide (0,8g, 8.3mmol), tri-tert-butylphosphine (IBOmg, 0.64mmol) and bis-dibenzylideneacetone-palladium(O) (125 mg, 0.2mmol) is heated under nitrogen to 85°C for 3h. After cooling, water (50ml), concentrated aqu. HCl (10ml) and hyflo (Ig) is added and stirring is continued for about one hour followed by filtration. The organic phase is washed with water twice, evaporated and the residue is subjected to flash chromatography on silica (45g) using heptane/toluene (2:1) as the eluent to afford N-(2",3",4",6"-Tetrafluorophenyl)-4-methylaniline (0.92g, 3.6 mmol) as an oil which crystallises (mp. 64-65°C). ^H-NMR (400 MHz, DMS0-d6): 2.20 (s, 3H, CH3); 6.63 [d, 8.2Hz, 2H, HC(2), HC(6)]; 6.99 [d, 8.2Hz, 2H, HC(3), HC(5)]; 7.56 [symmetrical m, IH, HC(5")]; 7.84 (s, IH, NH). N,N-Bis-p-tolyl-2,3,4,6-tetrafluoroaniline is isolated as a byproduct, mp: 94.96°C. Example lb: N-(2",3",5",6"-Tetrafluorophenyl)-4-ethylaniline A mixture of 2,3,5,6-tetrafluoroaniline (4.5g, 27.3 mmol), 4-ethylbromobenzene (5.0g, 27mmol), toluene (50ml), sodium tert-butoxide (4.67g, 48nunol), tri-tert-butylphosphin (217mg, 1.07mmol) and bis-dibenzyIideneacetone-pa]ladium(0) (260 mg, 0.45mmol) is heated under nitrogen to 85°"C for 15.5h. The mixture is cooled to room temperatue and water (30ml), concentrated hydrochloric acid (20ml) and hyflo are added. After stirring for 45minutes, the mixture is filtered and the organic phase is washed with water three times. The solvent is evaporated in vacuo and the residue is chromatographed on silica usind hexane/toluene (9:1 to 3:1) affording N-(2",3",5",6"-tetrafluorophenyl)-4-ethylanilin as a liquid. "H-NMR (400MHz, CDCI3): 1.26 (t, 3H, CH3); 2.65 (q, 2H, CH2); 5.65 (s, IH, NH); 6.73 [tt, IH, H-C(4")]; 6.88 [d. 2H, H-C(2,6)]; 7.15 [d, 2H, H-C(3,5)]. MS, m/z: 268 (M-H), 248 (M-HF). Example Ic: N-(2"-Chloro-4"-fluoro-6"-methylphenyl)-4-methylaniline 3.08g (19.3mmol) of 2-chlor-4-fluoro-6-methyl-aniline (prepared from N-acetyl-4-fluoro-2-methylaniline by chlorination followed by hydrolyses), 3.48 g (20.3mmol) of 4-bromotoluene are dissolved in 55ml of toluene and after the addition of 3.43g (36mmol) of sodium tert-butoxide, 166mg (0.82mmol) of tri-tert-butylphosphin and 460mg (O.Smmol) of bis-dibenzylideneacetone-palIadium(0), the mixture is heated with stirring under nitrogen to 90°C for 40 minutes. The usual aqueous acidic workup (50ml water, 10ml cone. HCl, Ig hyflo, filtration, washing the organic phase with water, drying, evaporation) gave 5.5g of the crude product which may be purified by flash-chromatography using silica and heptane as the eluent affording 3.52 g of N-(2"-chloro-4"-fluoro-6"-methylphenyl)-4-methylaniline as an oily substance. "H-NMR (400MHz, DMS0-d6): 2.18 (s, 3H, CH3); 6.37 (d, 2H, H-C(2,6)]; 6.92 [d, 2H, H-C(3,5)]; 7.19 (dd, IH. H-C(5")]; 7.32 (s, IH, NH); 7.35 (dd, IH, HC(3")]. Example Id: N-(2"-Chloro-6"-methylphenyl)-4-methylaniline 1.02g (7.2inmoI) of 2-chloro-6-methylaniline, 1.23g (7.2mmol) 4-bromotoluene, 1.15g (12mmol) sodium tert-butoxide, 160mg (OJmmol) tri-tert-butylphosphine and 130mg (0.23mmol) bis-dibenzylideneacetone-palladium(O) are reacted in 50ml toluene under nitrogen at 90°C for 20 minutes and at 60°C over night. Aqueous workup (3N HCl, with hyflo, washing the organic phase with water) and flash-chromatography on silica using heptan/toluene (4:1) as the eluent affords 1.49g of N-(2"-chloro-6"-methylphenyl)-4-methylaniline. "H-NMR (400MHz, CDCI3): 2.21 (s, 3H, C-6"- CH3); 2.29 (s, 3H. C-4-CH3); 5.61 (s,br, IH, NH); 6.57 [d, 2H, HC(2,6)]; 7.04 [d, 2H, HC(3,5)]; 7.07 [t under signal at 7.04, IH, HC(4")]; 7.16 [d, 2H, H(C5")]; 7.33 [d, IH, H(C3")]. N,N-Bis-p-tolyl-2-chloro-6-methylaniline (9mg) is isolated as a byproduct. Example le: N-(2"-Chloro-6"-methylphenyl)-4-ethylaniline To a solution of 5.2 g (37mmol) of 2-chIoro-6-methylaniline and 6.95 g (37.6 mmol) of 4-ethyl bromobenzene in 50ml of toluene is added 6.5 g (68 mmol) sodium tert-butoxide, 180 mg (0.89 mmol).tri-tert-butylphosphine (dissolved in 2 ml of toluene) and 300 mg (0.52 mmol) of bis-dibenzylideneacetone palladium(0). The mixture is heated unter nitrogen to 90°C for 3 hours and then cooled to room tenq)erature. Hyflo (Ig), water (30ml) and cone, hydrochloric acid (10ml) are added and after stirring for 30 minutes the mixture is filtered. The organic phase is washed with water (30ml) twice and evaporated. The residue is subjected to flash-chromatography on silica (75g) eluting with heptane to afford 5.3g (21.6mniol, 58%) of N-(2"-chloro-6*- methylphenyl)-4-ethyIaniline as an almost colourless liquid. •H-NMR (300MHZ, CDCI3): 1.10 (t, 3H, CH3CH2-); 2.10 [s, 3H, CH3-C(6")]; 2.50 (q, 2H, CH3-QJ2-); 5.54 (s, br, IH, NH); 6.48 [d, 2H, HC(2,6)]; 6.93 ft, 1H,H(C4")]; 6.95 [d. 2H. HC(3,5)]; 7.05 [d. IH, HC(5")]; 7.22 [d, IH, HC(3")]. Example If: N-(2",4"-Dichloro-6"-methylphenyl)-4-ethylaniline The mixture of 2,4-dichloro-6-methylaniline (3.313g, 18.8mmol), 4-ethyl bromobenzene (3.64g, 20mmol), sodium tert-butoxide (3.41g, 35mmol), racemic BINAP (0.274g, 0.44mmol), bis-dibenzylideneacetone-palladium(0) (250mg, 0.43mmol) and toluene (50ml) is refluxed under nitrogen for 22h. The mixture is cooled, treated with water (40ml), conc. HCl (10ml), hyflo (1.7g) stirred for additional 30minutes and filtered. The organic phase is washed with water twice and evaporated. The crude product (6.88g) is purified by flash-chromatography (silica, toluene) to afford 2.93 g of N-(2",4"-dichloro-6"-methylphenyl)-4-ethylaniline. "H-NMR (300MHZ, CDCI3): 1.15 (t, 3H, CHj-CHrAr); 2.08 (s, 3H, C-6"-CH3); 2.50 (q, 2H, CH3-CH2-Ar); 5.42 (s, br.. IH, NH); 6.50 [d, 2H, HC(2,6,)]; 6.96 [d, 2H, HC(3,5)]; 7.10 [s. IH, HC(5")]; 7.25 [s, IH, HC(3")1. The reaction proceeds much faster even at 85°C when BINAP is replaced by tri-tert-butylphosphine; however N,N-di-(4-ethylphenyl)-2",4"-dichloro-6"-methylaniline is formed as a byproduct in considerable amounts when excess of 4-ethyl bronrobenzene is used. This byproduct can be isolated as a solid, rap: 74-75""C; "H-NMR (400MHZ, CDQa): 1.24 (t, 6H, CH2-CH3); 2.09 (s, 3H, C-6"-CH3); 2.61 (q. 4H, CH2-CH3); 6.89 [d. 4H, HC(2,6)]; 7.06 [d. 4H, HC(3,5)]; 7.20 [s, IH. HC(5")]; 7.36 [s, IH, HC(3*)]; MS: 383 (M+), 368 (M-CH3), 354 (M-CH2CH3). Example 2: N-(2",3",6"-Trifluorophenyl)-4-ethylaniIine To a solution of 1.21g of 4-ethylaniline, l.l0g of 2,3,6-trifluoro-bromobeiizene in lOg of toluene is added consecutively 350 mg BINAP and 300 mg of bis-dibenzylideneaceton-palladium (0) [Pd(dba)2) in 3 ml of toluene and 0.9 g of sodium tert.-butoxide in 3 ml toluene. The mixture is flushed with nitrogen and heated for 6 h under reflux. After cooling to room ten5)erature, water (30 ml), concentrated hydrochloric acid (10 ml) and hyflo (1 g) are added and stirring is continued for 1 h. The mixture is filtered and the filtrate is separated into its phases. The organic phase is washed three times with water, dried using magnesium sulfate and evaporated to dryness. The residue can be used as such in the following step or purified by flash chromatography on silica using toluene as the eluent affording 1.13 g of N-(2",3",6"-trifluorophenyl)-4-ethylanilin. "H-NMR (300MHz, CDCU): 1.14 (t, 7.7Hz, 3H, CHa-CH.-Ar): 2.53(q, 7.7Hz, 2H, CH.-CHrAr); 5.29 (br. s, IH, NH); 6.7-6.81 [m, 2H, C-4"-H, HC(5")]; 6.75 [d, 2H. HC(2,6)3; 7.02 [d, 8.5Hz. 2H. HC(3,5)]. Diphenylamine compounds of Formula Vni, for mstance as prepared above in Examples 1 and 2, are converted to the corresponding compounds of Formula VII as described in Example 3 Example 3a N-(2*,3",4",6"-TetrafluorophenyI)-N-chloroacetyl-4- methylaniline The mixture of N-(2",3",4",6"-tetrafluorophenyl)-4-methylanilm (0.82g, 3.2 mmol) and chloro acetylchloride (1.6g) is heated with stirring to 90°C under nitrogen for 1.3 h. To destroy excess of the acid chloride, 2-propanol and water (2 ml each) is added and stirring is continued over night at room tenq)erature. After adding toluene (20ml), the mixture is extracted with sodium bicarbonate and the organic phase is dried with magnesium sulfate and evaporated to dryness. The residue is purified by flash chromatography (silica, toulene) to obtain N-(2",3",4",6"-tetrafluorophenyl)-N-chloroacetyl-4-methylaniline (0.98g, 2.95mmol) as an oil. Example 3b: N-(2" ,3" ,5" ,6" -Tetrafluorophenyl)-N-chloroacetyl-4-ethylanilinc N-(2",3",5",6"-tetrafluorophenyl)-4-ethylanilin (2.05g) and chloro acetylchloride (1.99g) is mixed without solvent and heated with stirring to 90°C under nitrogen for 20 h. Tetrahydrofurane (10ml) and aqueous sodium bicarbonate are added after cooling and stirring is continued for about 1 hour. The organic phase is diluted with toluene and washed with water three times and dried over magnesium sulfate. Evaporation and chromatography of the residue (silica, toluene) gave N-(2",3",5*,6"-tetrafluorophenyl)-N-chloroacetyl-4-ethylaniline (1.84g) as a solid which is recrystallised from heptane, rap.: 72°C "H-NMR (400MHz, DMF-d7, 140°C: 1.25 (t, 3H, CH3); 2.70 (q, 2H, CH2); 4.28 (s, 2H, CH2-CO); 7.35 [d, 2H, HC(3,5)]; 7.43 [d, 2H, HC(2,6)]; 7.65 [tt. IH, HC(4")). Example 3c: N-(2"-Chloro-4"-fluoro-6"-methylphenyl)-N-chloroacetyl-4-methylaniline 1.32g of N-(2"-Chloro-4"-fluoro-6"-methylphenyl)-4-methyIaniline is reacted with chloracetylchloride (1.76g) at 90°C for BOminutes. The cooled mixture is stirred with toluene (20ml) and aqu. sodium carbonate for 30 minutes and the organic phase is evaporated. The residue is purified flash-chromatography on silica using toluene affording 1.04g of N-(2"-chloro-4"-fluoro-6*-methylphenyl)-N-chloroacetyl-4-methylaniline as a solid which is recrystallised from heptane/2-propanol (9:1), mp.: 96-97°C. "H-NMR (400MHZ, DMF-d7, 120°C, all peaks appear broadend or split): 2.43 (s, 3H,CH3); 4.31 (s, 2H, CI-CH2-CO); 7.31 [d, IH, HC(5")]; 7.32 and 7.40 [AB, 4H, C-HC(2,6) and HC(3,5)]; 7.45 [s, IH. HC(3")]. Example 3d: N-(2"-Chloro-6"-methylphenyl)-N-chloroacetyl-4-methylaniline The solution of N-(2"-chloro-6"-methylphenyl)-4-methylaniline (1.4g) in 2.21g chloroacetylchloride is heated to 90°C for 4 h. The mixture is diluted with tohiene (25ml), cooled to room tenq)erature and washed with aqu. sodium carbonate. The organic phase is dried, evaporated and the residue is subjected to flash chromatography [57g silica, toluene and tohiene/ethylacetate (98:2)] to afford 1.45g of N-(2*-Chloro-6"-methylphenyl)-N-chloroacetyl-4-methylaniline which is crystallised from heptane. mp: 113-114°C. Example 3e: N-(2" -Chloro-6" -methylphenyl)-N-chloroacetyl-4-ethylaniline N-(2"-Ch]oro-6"-niethylphenyl)-N-4-ethylani]ine (4.95 g, 20 mmol) is treated with chloro acetylchloride (3.23 g, 28.5 mmol) and the mixture is heated with stirring under nitrogen at 95°C for 40 minutes. After adding 2-propanol (5 ml) and cooling to room ten5)erature, the mixture is diluted with toluene and extracted with aqu. sodium bicarbonate. The organic phase is washed with water and evaporated to dryness. Flash chromatography on silica (55g) using toluene as the eluent affords 5.66 g (17.6mmol, 88%) of N-(2"-chloro-6"-methylphenyl)-N-chloroacetyl-4-ethylaniline as a viscous liquid. "H-NMR (400MHz, DMF-d7, 140°C): 1.22 (t, 3H, CH2-CH2-), 2.32 (s, 3H, CH3-C6"); 2.65 (q, 2H, CH.-CH;-); 4.12,4.18 (AB, 2H, CH2-CI); 7.22 and 7.31 [each d, each 2H, HC(2,6) and HC(3,5)]; 7.3-7.5 [m, 3H, HC(3",4",5")]. Example 3f: N-(2",4"Dichloro-6"-methylphenyl)-N-chloroacetyl-4- ethylaniline N-(2",4"Dichloro-6"-methylphenyl)-4-ethylaniline (4.83g as a mixture with the byproduct N,N-di-(4-ethylphenyl)-2",4"-dichloro-6*-methylaniline) is dissolved in 4. 18g of chloro acetylchlorid and heated to 100°C for 1.5h. The mixture is cooled, diluted with toluene (50ml) and extracted with aqu. sodium bicarbonate. The organic phase is evaporated to dryness and chromatographed on silica (75g) eluting with toluene to afford unreacted N,N-di-(4-ethylphenyl)-2",4"-dichloro-6"-methylaniline and N-(2",4"-dichloro-6"-methylphenyl)-N-chloroacetyl-4-ethylaniline(2.95g). A crystallised sample melts at 83-84°C. "H-NMR (400MHZ, DMF-d7, 140°C): 1.22 (t, 3H, CH2-CH2); 2.31 (s, 3H, C-6"-CH3); 2.56 (q, 2H, CH3-CH2); 4.20 (s, split, 2H, CI-CH2-CO); 7.35, 7.42 [AB, 4H, HC(2,6) and HC(3,5) respectively]; 7.40 [s, br. IH, HC(5")], 7.53 [s, br, IH, HC(3")]. Alternatively compounds of Formula VIII may be prepared by a procedure involving coupling of l-methoxy-4-methylcyclohexa-l,4-dJene or l-methoxy-4-ethylcyclohexa-l,4-diene with an aniline derivative of formula IV as defined above to give an intermediate compound of Formula XIII (or tautomer thereof) which is oxidised without isolation to give the compound of Formula VIQ, as described below in Example 4. Example 4a): N-f2".6"-DichlorophenvlM-methylaniline a) A solution of 4.35 g 2,6-dichloro-aniline in 4 ml of tetrahydrofuran and 35 ml of chlorobenzene is cooled down to -40 to -45°C. At this temperature, 5.09 g of titanium-tetrachloride is added to the solution, followed by the addition of 5.0 g of 1-Methoxy-4-methylcyclohexa-l,4-diene. The reaction mixture is allowed to warm up to approximately -35°C and stirred for 2 hours at this temperature. A solution of 10.18 g of iodine in 20 ml of tetrahydrofuran and 2.3 ml of acetic acid is then added dropwise to the reaction mixture and the temperature was allowed to warm up to 0°C. The mixture was stirred for 1 hour at 0°C and 16 hours at 25°C. Then 3.4 g of iodine is added to the reaction mixture and stirring is continued for additional 24 hours at 25°C. The reaction is finally quenched by pouring the reaction mixture onto a mixture of 250 ml of aqueous Sodium bisulfite (38-40%) and 400 ml of saturated aqueous sodium carbonate. The water phase is extracted with ethyl acetate (1x200 ml and 2x100 ml), the ethyl acetate phases are unified and washed with 1(X) ml of water. The organic phase was dried over anhydrous sodium sulfate and evaporated in vacuo to yield 11.44 g of a dark slurry. The slurry was dissolved in hexane/t-butyl-methylether and the solution was filtered over silica gel to obtain, after evaporation of the solvent, 5.75 g of crude product. The product can be used directly in the next step. Alternatively, it can be purified e.g. by column chromatography on silica gel with hexane/t-butyl-methylether (9:1) as eluent to yield pure N-(2",6"-Dichlorophenyl)-4-methylaniline. "H-NMR(CDCl3, 400 MHz, 300K) 5 2.3l(s, 3H, CH3), 3.6-4.8(broad signal, IH, NH), 6.68(d, J= 8 Hz, 2H, H-C(2) and H-C(6)), 7.02-7.12 (m, 3H, H-C(3), H-C(5) and H-C(4")), 7.38 (d, J= 8 Hz, 2H, H-C(3") and H-C(5")). MS(EI): m/z 251(Nr), 216(M-a)+, 181(M-2C1)+ Example4b): N-(2"-Chloro-6"-fluoro-phenylV4-methylaniline A solution of 3.91 g 2-chloro-6-fluoro-aniline in 4 ml of tetrahydroftiran and 35 ml of chlorobenzene is cooled down to -40 to -45°C. At this temperature, 5.09 g of titanium-tetrachloride is added to the solution, followed by the addition of 5.0 g of 1-Methoxy-4-methylcyclohexa-l,4-diene. The reaction mixture is allowed to warm up to approx. -35°C and stirred for 2 hours at this temperature. A solution of 10.18 g of iodine in 20 ml of tetrahydroftiran and 2.3 ml of acetic acid is then added drop-wise to the reaction mixture and the temperature was allowed to warm up to 0°C. The mixture was stirred for 1 hour at 0°C and 16 hours at 25°C. Then 3.4 g of iodine is added to the reaction mixture and stirring is continued for additional 24 hours at 25°C. The reaction is finally quenched by pouring the reaction mixture onto a mixture of 250 ml of aeq. Sodium bisulfite (38-40%) and 400 ml of saturated aeq. sodium carbonate. The aqueous phase is extracted with ethyl acetate (1x200 ml and 2x100 ml), the ethyl acetate phases are unified and washed with 100 ml of water. The organic phase was dried over anhydrous sodium sulfate and evaporated in vacuo to give a yellow viscous liquid. The liquid was dissolved in hexane/t-butyl-methylether and the solution was filtered over silica gel to obtain, after evaporation of the solvent, 4.33 g of crude product. The product can be used directly in the next step. Alternatively, it can be purified e.g. by column chromatography on silica gel with hexane / t-butyl-methylether (9:1) as ehient to yield pureN-(2"-Chloro-6"-fluoro-phenyl)-4-methylaniline. "H-NMR (DMSO-d6, 500 MHz, 300K) 5 2.17(s. 3H. CH3); 6.53[dd, J = 8.5Hz, JH-F = 1.5Hz, 2H. HC(2) and HC(6)3, 6.94[d, J = 8.0Hz, 2H. HC(3) and HC(5)], 7.16[ddd, J = 8.0Hz, J„.p= 6.0Hz, IH, HC(4")], 7.25[ddd, J = 8.0,1.5Hz, J„.p= 8.0, IH, HC(5")]; 7.34[ddd, J = 8.0,1.5Hz, J„.F= 1.5, IH, HC(3")]; 7.63(s, IH, NH). MS(EI) m/z 235 (100, M+, 200 (35, (M-Cl+, 185 (55) Example 4c): N-(2"-Chloro-6"-methyl-phcnvlV4-ethvlaniline A solution of 3.0 g 2-Cliloro-6-methyl-aniline in 3.5 ml of tetrahydrofuran and 31 ml of chlorobenzene is cooled down to -40 to -45°C. At this temperature, 4.01 g of titanium-tetrachloride is added to the solution, followed by the addition of 6.18 g of 1-Methoxy-4-ethylcyclohexa-l,4-diene. The reaction mixture is allowed to warm up to approx. -35°C and stirred for 3 hours at this ten:q)erature. A solution of 8.06 g of iodine in 16.4 ml of tetrahydrofuran and 1.8 ml of acetic acid is added to the reaction mixture and the ten^rature is allowed to warm up to 0°C. The mixture is stirred for 30 minutes at 0°C and 2 hours at 25""C. Then 2.68 g of iodine is added to the reaction mixture and stirring is continued for additional 24 hours at 25°C. Again, 2.68 g of iodine is added and stirring is continued for additional 72 hours at 25°C. The reaction is finaUy quenched by pouring the reaction mixture onto a mixture of 250 ml of aqueous sodium bisulfite (38-40%) and 450 ml of saturated aqueous sodium carbonate. The water phase is extracted with ethyl acetate (1x200 ml and 2x100 ml), the ethyl acetate phases are unified and washed with 100 ml of brine. The organic phase was dried over anhydrous sodium sulfate and evaporated in vacuo to give a dark viscous liquid. The liquid was dissolved in heptane / toluene and the solution was filtered over silicagel to obtain, after evaporation of the solvent, 2.0 g of crude product. The product can be used directly in the next step. Alternatively, it can be purified e.g. by column chromatography on silica gel with heptane / toluene (7:3) as eluent to yield pure N-(2-Chloro-6-methyl-phenyl)-4-ethylaniline. "H-NMR(CDCl3, 400 MHz, 300K) 6 1.24 (t, J= 7.5 Hz, 3H, H3C(8)), 2.22 (s, 3H, H3C-C(2")), 2.61 (q, J= 7.5 Hz, 2H, H2C(7)), 4.0-5.5 (broad signal, IH, NH). 6.60 (d-like, J= 8 Hz, 2H, H-C(2) and H-C(6)), 7.02-7.10 (m, 3H, H-C(3), H-C(5) and H-C(4")), 7.10-7.20 (m, IH, H-C(3")). 7.33 (d-like, J= 9 Hz, IH, H-C(5")). MS: m/z 245(M*). 230, 214, 194,180. The l-Methoxy-4-methylcyclohexa-l,4-diene and l-Methoxy-4-ethylcyclohexa-l,4-diene starting materials for Example 4 are prepared according to a known literature procedure. l-Methoxy-4-methylcyclohexa-l ,4-diene ( Preparation according to a known literature procedure: G.S.R. Subba Rao, D. K. Banerjee, L. Uma Devi and Uma Sheriff, Australian Journal of Chemistry 1992,45, p. 187-203 1 -Methoxy-4-ethylcyclohexa-1,4-diene Conpound 4 was prepared according to the same literature procedure given above for 1 -methoxy-4-methyIcyclohexa-1,4-diene. The products of Examples 4 are converted into the corresponding compounds of Formula VII for instance as described in Exaamples 3 above and 5 below Example 5: N-(2\6"-Dichlorophenyl")-N-chloroacetyl-4-methy1ani]tne N-(2",6"-Dichlorophenyl)-4-methylaniline (4.86g) is reacted with chloroacetylchloride (3.92g) at 90°C for 2h. After dilution with toluene, the mixture is washed with aqueous sodiumcarbonate twice, 40% aqu. sodium bisulfite and water. The organic phase is dried (MgSOt) and evaporated. The residue is recrystallised from ethanol (12g) to obtain N-(2",6*-Dichlorophenyl)-N-chloroacetyl-4-methylaniline (2.83g), rap: 129.5-130°C. In a yet further alternative compounds of Formula VII may be prepared by a procedure involving a Smiles type rearrangement of a compound of Formula DC to give an intermediate product of Formula VIII as defined above which is converted without being isolated to the compound of Formula VII as described in Example below. Example 6a): N-(2".6"-dichloro-4"-methylphenyl)-N-chloroacetvl-4- methylaniline. 12g (67 mmol) of 2,6-dichloro-4-methylphenol are dissolved in 25 ml of 2-propanol followed by the addition of 10.5g (76 mmol) of potassium carbonate and 12.8g (70 mmol) of 2-chloro-N-(4-methylphenyl)acetamide. The mixture is refluxed for 4h. At this time, the formation of A: 2-(2",6"-dichloro-4"-methy^henoxy)-N-(4-methylphenyl)acetamide is completed. 13.6ml of sodium methylate solution 30% in methanol are slowly added and the temerature is increased to about 8S°C by distilling 25ml of solvent. The mixture is stirred 2h more to conplete the formation of g. 25ml of water are added at 70°C to obtain a 2 phases solution. The lower layer is discarded. The upper layer is diluted with 20 ml of heptane-fraction and washed with 2x 20 ml of water. The organic phase is separated and concentrated in vacuo to obtain N-(2",6"-dichloro-4"-methylphenyl)-4-methylaniline as a crude oil. GC/MS: 265(100,M*), 195(130). This oil is heated to 90°C and treated with 6.5ml of chloroacetylchloride. After 2h the mixture is diluted with 60nil of 2-propanol, cooled to about 20°C and seeded. The precipitated suspension is cooled to 0°C. The crystals are isolated by filtration, washed with cold 2-propanol and dried to obtain N-(2",6"-dichloro-4"-methylphenyl)-N-chloroacetyl-4-methylaniIine. Mp: 140-14rC. •H-NMR (DMF-d7, 413K, 400Mz) 2.33 (s, 3H, CHj); 2.40(s, 3H, CH3); 4.18(s, 2H. CH2); 7.22[d, 2H, HC(5) and HC(3)]; 7.38[d, 2H, HC(2) and HC(6)]; 7.42[s, 2H, HC(3")and HC(5")]. Example 6b): N-(2"-chloro-6"-fluorophenyl)-N-chloroacetyl-4-methylaniline Same procedure as example 6a, starting from 2-chloro-6-fluorophenol Mp: 80-82°C. "H-NMR (DMF-d7, 393K, 400Mz) 2.4(s, 3H, CH3); 4.3(s, 2H, CH2); 7.35[d, 2H, HC(3) and HC(5)]; 7.43[ddd, IH, HC(5")]; 7.48[d, 2H, HC(2) and HC(6)]; 7.55[d, IH, HC(3")]; 7.6[ddd, IH, HC(4")]. Example 6c): N-("2\3\6" -trifluorophenyl)-N-chloroacetyl-4-ethylaniline Same procedure as example 6a, starting from 2,3,6-trifluorophenol and 2-chloro-N-(4-ethylphenyl)acetamide. The crude intermediate N-(2",3",6"-trifluorophenyl)-4-ethylaniline was roughly purified by filtration on silica using toluene as eluent, Mp: 49-50°C. *H-NMR(DMF-d7, 413K, 400MHz) 1.24(t, 3H, CH3); 2.70(q, 2H. CH2-CH3); 4.25(s, 2H, CHz-Q); 7.20[m, IH, HC(5")]; 7.34[d, 2H, HC(3) and HC(5)]; 7.42[d, 2H, HC(2) and HC(6)]; 7.46[m, IH, HC(4")]. Example 6d): N-(2*-chloro-6"-fluorophenylVN-chloroacety|-4-ethy1ani1ine Same procedure as example 6a starting from 2-chloro-6-fluorophenol and 2-chloro-N- (4-ethylphenyl)acetamide. Mp: 67-68°C. "H-NMR (DMF-d7, 413K, 500MHz) 1.23(t, 3H, CH3); 2.68(q, 2H, CH2-CH3); 4.20(s, 2H, CH2-CI); 7.29[d, 2H, HC(3) and HC(5)]; 7.34[m, IH, HC(5")]; 7.43[d, 2H, HC(2) and HC(6)]; 7.48[m, 2H, HC(3") and HC(4")]. Example 6e): N-(2".6"-dichlorophenyl)-N-chloroacetvl-4-methy1anilinft Same procedure as example 6a starting from 2,6-dichlorophenol and 2-chloro-N-(4-methylphenyl)acetamide. At the end of the acetylation reaction the mixture was diluted with a small amount of toluene (0.2 part) to prevent solidification. Mp: 129-130°C. "H-NMR(DMF-d7, 393K, 500Mz) 2.40(s, 3H, CH3); 4.28(s, 2H, CH2-CI); 7.30[d, 2H, HC(3) and HC(5)]; 7.46[d, 2H, HC(2) and HC(6)]; 7.54[m, IH, HC(4")]; 7.67[d, 2H, HC(3") and HC(5")]. Compounds of Formula VII are cyclised to give lactams of Formula II as described in Example 7 Example): N-(2".6"-dichloro-4"-methylphenvlV5-methyloxindole A mixture of 6.85g (20 mmol) of N-(2",6"-dichloro-4"-methylphenyl)-N-chloroacetyl-4-methylaniline and 3.36g (26 mmol) of aluminium chloride was heated slowly to 160-170°C and held at this temperature for 3-4h. During this time, nitrogen was continuously bubbled into the melt. The mixture was diluted with 20 ml of toluene and added on 20 ml of warm water. The organic layer was separated, washed with water and evaporated. The residue was crystallised from 20 ml of 2-propanol giving N-(2",6"-dichloro-4"-methyIphenyl)-5-methyloxindole. Mp: 153-154°C. "H-NMR (DMS0-d6, 500Mz, 300K) 2.29 [s, 3H, CH3-CS)]; 2.41 [s, 3H, CH3-C(4")]; 3.81(s, 2H, CH2); 6.27 [d, IH, HC(7)]; 7.00 [d. IH, HC(6)1; 7.19 [s, IH, HC(4)]; 7.58 [s, 2H, HC(3") and HC(5")]. Example 7b): N-(2"-chloro-6"-fluorophenyl)-5-methyloxindole Same procedure as example 7a Mp:137-138°C."H-NMR (DMSO-d6, 500MHz, 300K) 2.27(s, 3H, CH3); 3.83(s, 2H, CH2) 6.35[d, IH, HC(7)]; 7.01[ d, IH, HC(6)]; 7.19 [s, IH, HC(4)]; 7.52 [d, IH, HC(5")]; 7.60 [d, IH, HC(3")], 7.63 [d, IH, HC(4")]. Example 7c): N-(2".3".6"-trifluorophenylV5-ethvloxindole Same procedure as example 7a. After 4h reaction, 10% more aluminium chloride was added, Overall reaction time: 6h. Mp: 171-172°C.1H-NMR (DMS0-d6, 500Mz, 300K) 1.18 (t, 3H, CH3); 2.60[q, 2H, CH2-CH3]; 3.89[s, 2H, CH2-CO]; 6.62 [d, IH, HC(7)]; 7.09[d, IH, HC(6)]; 7.25 [s. IH, HC(4)]; 7.46 [m, IH, HC(5")]; 7.76 [m, IH, HC(4")]. Exan^le7d): N-(2"-chloro-6*-fluorophenyl)-5-ethyloxindole Same procedure as example7c. Mp: 129-130""C. "H-NMR (DMSO- d6, BOOK. 500Mz) 1.18 (t, 3H, CH3); 2.59 [q, 2H, CH2-CH3]; 3.86 (s, 2H. CH2-C0 ); 6.39 [d, IH, HC(7)]; 7.05 [d, IH, HC(6)]; 7.24 [s, IH, HC(4)], 7.59 [m, IH, HC(5")]; 7.64 [m, 2H, HC(3") and HC(4")]. Example 7e): N-(2,6-dichlorophenvn-S-methvloxindole Same procedure as 7a H-NMR (DMS0-d6, 500MHz, 300K) 2.30 (s. 3H, CH3); 3.85 (s, 2H, CH2); 6.29 [d. IH, HC(7)]; 7.02 [d, IH, HC(6)]; 7.22 [s, IH, HC(4)], 7.62 [t, IH, HC(4")]; 7.76 [d, 2H, HC(3") and HC(5")]. Example 7f): N-f2".3*.4".6"-TetrafluorophenvlV5-methyloxindole The solution of N-(2",3",4",6"-tetrafluorophenyl)-N-chloroacetyl-4-methylaniline (0.97g, 2.97mmol) in chlorobenzene (2.5g) is treated with aluminum trichloride (1.05g, 7.8mmol) and the mixture is heated with stirring in an oil bath (155°C) for 5h while flushing the flask with nitrogen. Toluene (30ml) and water (20ml) are added and stirring is continued for 30 minutes at room temperature. The phases are separated and the organic phase is washed with hydrochloric acid (2N) and water. Evaporation under reduced pressure affords a solid (0.84g, 2.85mmol) which is recrystallised from 2-propanol to afford pure N-(2",3",4",6"-tetrafluorophenyl)-5-methyloxindole, mp. 172-173""C. IH-NMR (300MHz, 300K, CDCI3): 2.28 (s, 3H, CH3); 3.65 [s, 2H, H2C(3)]; 6.39 [d, 7.5Hz, IH, HC(7)]; 6.85-7.0 [m, IH, HC(5")]; 6.98 ttd, 7.5H2, IH, HC(6)]; 7.09 [s. IH, HC(4)]. Exan^le7g): N-f2"-Chloro-6"-methvlphenylV5-ethyloxindole In a flask are mixed N-(2"-chloro-6"-methylphenyl)-N-chloroacetyl-4-ethylaniline (2.08g) are mixed with aluminum trichloride (1.16g) and the mixture is flushed with nitrogen. The flask is introduced into an oil bath (155-160°C) and the mixture is stirred under a stream of nitrogen for 4.5 hours. The mixture is slightly cooled to about 100°C, treated with toluene (30ml) and IN HCl (20ml) and stirred for 30 minutes whUe the temperature decreases gradually. After phase separation, the organic phase is washed with IN HCl and water, dried (magnesium sulfate) and evaporated. The residue is chromatographed on silica (86g) using toluene containing 5-20% isopropyl acetate as eluent affording the title product. Mp: 125-126°C In a yet farther alternative lactams of Formula n are prepared by oxidation of an unsaturated lactam of Formula HI which may be prepared, for instance as described in Example 8. Example 8: (5-Ethy]-2-morpholin-4-yl-cycIohex-2-enylidene)-acetic acid ethyl ester 91.6 g of 4-Ethyl-cyclohexanone, 73.6 g of morpholine and 2 g of p-toluene-sulfonic acid monohydrate are dissolved in 400 ml of toluene. The mixture is heated to reflux and the water formed is removed by a water separator. After reacting for about 24h, the reaction mixture is cooled to 100°C and 2 g of p-tohiene-sulfonic acid are added, followed by the addition of 157.22 g of glyoxylic acid ethyl ester during 30 minutes. The mixture is again heated to reflux for 5 hours and allowed to cool down to 22°C. The solvent is evaporated in vacuo and the crude product is distilled in vacuo at 140-150°C/9.5-^mbar. "H-NMR(CDCl3, 500 MHz, 277K) 6 0.896 ppm (t, J= 7 Hz, 3H, H3CCH)), 1.277 (t, J= 7 Hz, 3H, HaC(lO)), 1.20-1.45 (m. 2H, H2C(16)), 1.50-1.62 (m, IH. H-C(4)), 1.876 (ddd, Ji= 18 Hz, J2= 9 Hz, J3= 3 Hz, IH, H-C(3)), 2.13 (m, IH, H-C(5)), 2.35 (dt, J,= 17 Hz, h= 5 Hz. IH, H-C(3)). 2.55-2.65 (m, 2H, H-C(12) and H-C(15)). 2.72-2.80 (m. 2H. H-C(12) and H-C(15)), 3.55 (dm. J= 15Hz. IH, H-C(5)). 3.74 (m. 4H, H2C(13) and H2C(14)). 4.152 (q. J= 7 Hz. 2H, H2C(9)). 5.46 (dd. J,= 5Hz, h= 3Hz, IH. H-C(2)), 6.17 (broad s. IH, H-C(7)). Assignments according to numbers given on the formula. IR(film): strong absorptions at 2960,1710,1624. 1609,1191, 1156 and 1120 cm"". MS(EI): m/z 279(ivr), 250(M-C2H5)^ 234, 206(M-CO2C2H5)^ 176, 164, 135, 84. b). Synthesis of (5-Ethyl-2-oxo-cycIohexylidene)-acetic acid ethyl ester 10 g of [5-Ethyl-2-morpholin-4-yl-cyclohex-2-enylidene]-acetic acid ethyl ester are dissolved in 20 ml of toluene. 12 ml of 6M HCl are added dropwise under rigorous stirring and the reaction mixture is stirred for additional 60 minutes at 22°C. The organic layer is separated and washed with 25 ml of water twice. The combined water layers are extracted with 25 nd of toluene. The combined toluene layers are dried over anhydrous sodium sulfate and the solvent is evaporated in vacuo to yield 6.72 g of [5-ethyl-2-oxo-cyclohexylidene]-acetic acid ethyl ester as an oil. "H-NMR (CDCl3, 500MHz, 277K) 5 0.935 ppm (t, J= 7 Hz. 3H, H3C(12)), 1.259 (t, J= 7 Hz, 3H, HjQlO)), 1.31-1.45 (m. 2H, H2C(11)), 1.46-1.55 (m, IH, H-C(5)). 1.59-1.69 (m, IH, H-C(4)). 1.97-2.04 (m, IH, H-C(5)), 2.296 (ddd, J= 17 Hz, II Hz and 3Hz, IH, H-C(3)), 2.383 (m, IH. H-C(6)), 2.615 (dt, J= 17 and 4 Hz, IH, H-C(6)), 3.57 (dm, J= 17 Hz. IH, H-C(3)), 4.17 (q, J= 7 Hz, 2H, H2C(9)), 6.42 (m, IH, H-C(7)). Assignments according to numbers given on the formula. IR(film): strong absorptions at 1719,1698 and 1200 cm"". MS (EI): m/z 210(M+, 164(M-C2H50Hr, 135. c). Synthesis of l-(2-Chloro-6-methyl-phenyl)-5-ethyl-l,4,5,6-tetrahydro-mdol-2-one 3.45 g of 2-Chloro-6-methyl-aniline are dissolved in 26 ml of toluene. 0.227 g of p-toluene-sulfonic acid (mono hydrate) are added and the mixture is heated to reflux. A solution of 5.0 g of (5-Ethyl-2-oxo-cyclohexylidene)-acetic acid ethyl ester in 13 ml of toluene is added drop-wise during 75 minutes and the water formed is collected by the means of a water separator. The reaction mixture is heated to reflux for 15 hours, during which time the condensing solvent is frequently removed and replaced by fresh toluene. For work-up, the mixture is cooled to 22°C and is treated with 70 ml of saturated aqueous sodium bicarbonate solution under rigorous stirring. The layers are separated and the toluene phase is washed with a 5% aqueous solution of citric acid and finally with a 10% solution of sodium chloride in water. The aqueous phases are extracted with 70 ml of toluene and the toluene phases are combined. The solvent is evaporated in vacuo to yield 7.1 g of the crude product as a highly viscous oil. An analytical sanple of the crude product can be purified by chromatography on silica gel using toluene/ethyl acetate (9:1) as eluent to yield pure l-(2-Chloro-6-methyl-phenyl)-5-ethyl-1,4,5,6-tetrahydro-indol-2-one. "H-NMR (dfi-DMSO, 400MHz, BOOK) 5 0.894 ppm (t, J= 7Hz, 3H, HsQl 1)), 1.34-1.43 (m. 2H, HzQlO)), 1.70-1.82 (m, IH, H-C(5)), 1.90-2.02 (m, IH. H-C(6)), 2.038 (s, 3H. H3C(6")), 2.28-2.40 (m, 2H, H-C(4) and H-C(6)), 2.87 (dd, J,= 17Hz and J2= 4 Hz, IH, H-C(4)), 5.14 (m, IH, H-C(7)). 5.96 (broad s, IH, H-C(3)), 7.3-7.5 (m, 3H. H-QB"), H-C(4"), H-C(5")). Assignments according to the numbers given on the formula. IR (film): strong absorptions at 1703, 1660 and 1476 cm"". MS (EI): m/z 287 (M+), 272 (M.CHs)+ 258 (M-C2H5)+, 252 (M-Cl)+ d): Synthesis of N-(2-Chloro-6-methyl-phenyl)-5-ethyl-oxindole 1 -(2-Chloro-6-methyl-phenyl)-5-ethyl-1,4,5,6-tetrahydro-indol-2-one can be oxidized by classical methods, e.g. with 10% Pd-C in refluxing xylene to yield N-(2-Chloro-6-methyl-phenyl)-5-ethyl-oxindole. "H-NMR and MS spectra see example 7g. Lactams of Formula n as defined above are converted to compounds of Formula I as defined above, for instance as described in Example 9 below. Exan^le 9 a): 5-MethyI-2-(2".6"-dichloro-4"-methylanilino)phenylacetic acid A mixture of 1.5g of N-(2",6"-dichloro-4"-methylphenyl)-5-methyloxindole, 18ml of ethanol and 1ml of water is heated to reflux. 1.9g of a 30% sodium hydroxide solution is slowly added and reflux is continued for 4-5h. The solution is cooled to about 40°C and treated slowly with a solution of 1.5g of concentrated hydrochloric acid in 12ml of water up to a pH of 3-4. The obtained suspension is cooled to 20°C. The crystals are collected by filtration, washed with water and dried giving 5-Methyl-2-(2",6"-dichloro-4"-methylanilino)phenylacetic acid. Mp: 179-182°C. "H-NMR (DMSO-d6, 300K, 500Mz) 2.22[s, 3H, CH3-C(5)]; 2.32[s, 3H, CH3-C(4")]; 3.67(s, 2H, CHa); 6.18[d, IH, HC(3)], 6.87[s, d, IH, HC(4)]; 6.97(s, IH, NH); 7.02[s, IH, HC(6)]; 7.36[s, 2H, HC(3") and HC(5")]; 12.68(br.s, IH, COOH). Example 9b): 5-Methyl-2-(2"-chloro-6"-fluoroanilino)phenylacetic acid Same procedure as 9a. Mp: 152-154°C "H-NMR(DMS0-d6, 500MHz, 300K) 6 2.21(s, 3H, CHj), 3.64(s, 2H, CHj); 6.42[dd, IH, HC(3)], 6.90[dd, IH, HC(4)], 7.01 [d, IH, HC(6)], 7.09(s, IH, NH), 7.09[ddd, IH, HC(4")]. 7.23[ddd, IH, HC(5")], 7.34[ddd, IH, HC(3")], 12.67(s, IH, COOH). Example 9c): 5-Methyl-2-f2".3".4".6"-tetrafluoroanilinoVphenylaceticacid The suspension of 350 mg of N-(2",3",4",6"-tetrafluorophenyl)-5-methyloxindole in 20ml of ethanol and 5 ml of water is degassed by passing through nitrogen for 1.5h. Then 260mg of 30% aqueous sodium hydroxide is added and the mixture is heated to reflux for 6.5 hours. Most of the ethanol is then removed by distillation the mbcture is cooled to room temperature followed by the slow addition of IN hydrochloric acid (1.05g) to reach a pH of about 3. The precipitate is then filtered, washed with ethanol/water (1:1) and dried in vacuo at room temperature affording the title product. Mp: 145-146°C. IH-NMR (300MHz, DMS0-d6): 2.23 (s, 3H. CH3); 3.65 (s, 2H, CH2-COO); 6.55 [s, IH, HC(3)]; 6.92 [d, IH, HC(4)]; 7.00 [s, IH, HC86)]; 7.20 (s, IH, NH); 7.50 [m, IH, HC(5")]. Similarly other lactams of formula II are converted to conq)ounds of Formula I substantially as described above. WE CLAIM; 1. A process for the production of a compound of Formula I, or a pharmaceutically acceptable salt thereof, or a pharmaceutically acceptable prodrug ester thereof, wherein R is methyl or ethyl; R1 is chloro or fluoro; R2 is hydrogen or fluoro; R3 is hydrogen, fluoro, chloro, methyl, ethyl, methoxy, ethoxy or hydroxy; R4 is hydrogen or fluoro; and R5 is chloro, fluoro, trifluoromethyl or methyl, provided that R1, R2, R4 and R5 are not all fluoro when R is ethyl and R3 is H; comprising the steps of: rearrangement and hydrolysis of a compound of formula IX to produce a compound of formula VIII transforming the compound of formula VIII into the compound of formula I. 2. The process as claimed in claim 1, wherein any interfering reactive groups are temporarily protected and then the resulting compound is isolated . 3. The process as claimed in claim 1, wherein the free carboxylic acid of the compound of formula I is converted into a pharmaceutically acceptable ester derivative thereof 4. The process as claimed in claim 1, wherein the free acid of formula I is converted into a salt or a resulting salt into the free acid or into another salt. 5. The process as claimed in claim 1, wherein the transforming of the compound of formula VIII into the compound of formula I comprises (a) N-acylation of the compound of formula VIII with a haloacetyl chloride to produce a compound of formula VII (b) cyclisation of the compound of formula VII to produce a lactam of formula and (c) cleaving the lactam with a base. 6. A process for the preparation of a compound of formula VIII which comprises rearrangement and hydrolysis of a compound of formula IX. 7. The process as claimed in any one of claims 1 to 4 for the preparation of a compound selected from: 5-methyl-2-(2",4"-dichloro-6"-methylanilino)phenylaceticacid; 5-methyl-2-(2", 3", 5", 6"-tetrafluoroanilino)phenylacetic acid; 5-methyl-2-(2", 3", 4", 6"-tetrafluoroanilino)phenylacetic acid; 5-methyl-2-(2",6"-dichloroanilino)phenylaceticacid; 5-methyl-2-(2",6"-dichloroanilino)phenylacetic acid, potassium salt; 5-methyl-2-(2",6"-dichloroanilino)phenyIacetic acid, sodium salt; 5 -methyl-2-(2" -chloro-6" fluoroanilino)phenylacetic acid; 5-methyl-2-(2",6"-dichloro-4"-methylanilino)phenylaceticacid; 5-methyl-2-(2"-chloro-6"-methylanilino)phenylaceticacid; 5-methyl-2-(2" ,4"-difluro-6" -chloroanilino)phenylacetic acid; 5-methyl-2-(2"-fluoro-4",6"-dichloroanilino)phenylacetic acid; 5-methyl-2-(2"-chloro-4"-fluoro-6"-methylanilino)phenylacetic acid; 5-ethyl-2-(2"-fluoro-6"-chloroanilino)phenylaceticacid; 5 -ethyl-2-(2" -chloro-6" -methylanilino)phenylacetic acid; 5-ethyl-2-(2",3",6"-trifluroanilino)phenylacetic acid; 5-ethyl-2-(2",3",5",6"-tetrafluoro-4"-ethoxyanilino)phenylacetic acid; 5-ethyl-2-(2"-chloro-4",6"-difluroanilino)phenylacetic acid; 5-ethyl-2-(2",4"-dichloro-6"-fluoroanilino)phenylacetic acid; 5-ethyl-2-(2",4"-dichloro-6"-methylanilino)phenylacetic acid; 5-ethyl-2-(2"-fluoro-4"-chloro-6"-methylaniiino)phenylacetic acid; 5-ethyl-2-(2",4"-difluoro-6"-methylanilino)phenylacetic acid; 5-ethyl-2-(2"-chloro-4"-fluoro-6"-methylanilino)phenylacetic acid; 5-methyl-2-(2"-chloro-4"-hydroxy-6"-fluoroanilino)phenylacetic acid; 5-methyl-2-(2"-fluoro-6"-trifluoromethylanilino)phenylacetic acid; 5-methyI-2-(2" ,4"-dichloro-6"-trifluoromethylanilino)phenylacetic acid; 5-methyl-2-(2", 3", 4", 6"-tetrafluoroanilino)phenylacetic acid; 5-methyl-2-(2",6"-dichIoroanilino)phenylacetic acid; 5-methyl-2-(2"-chloro-6" fluoroanilino)phenylacetic acid; 5-methyl-2-(2",6"-dichloro-4"-methylanilino)phenylaceticacid; 5 -methyl -2 -(2" -chloro-6" -methylanilino)phenylacetic acid; 5-methyl-2-(2"-chloro-4"-fluoro-6"-methylanilino)phenylacetic acid; 5-ethyl-2-(2"-fluoro-6"-chloroanilino)phenylacetic acid; 5-ethyl-2-(2"-chloro-6"-methylanilino)phenylacetic acid; 5-ethyl-2-(2",3",6"-trifluroanilino)phenylacetic acid, and 5-ethyl-2-(2" ,4"-dichloro-6"-methylanilino)phenylacetic acid, and pharmaceutically acceptable salts thereof; and pharmaceutically acceptable prodrug esters thereof. 8. The process as claimed in any one of the preceding claims wherein: R is methyl; Rl is chloro; R2, R3 and R4 are hydrogen and R5 is fluoro. 9. A compound of formula I prepared by a process as claimed in any one of claims 1 to 4. |
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in-pct-2002-0411-che abstract-duplicate.pdf
in-pct-2002-0411-che claims-duplicate.pdf
in-pct-2002-0411-che claims.pdf
in-pct-2002-0411-che correspondence-others.pdf
in-pct-2002-0411-che correspondence-po.pdf
in-pct-2002-0411-che description(complete)-duplicate.pdf
in-pct-2002-0411-che description(complete).pdf
in-pct-2002-0411-che form-1.pdf
in-pct-2002-0411-che form-13.pdf
in-pct-2002-0411-che form-19.pdf
in-pct-2002-0411-che form-26.pdf
in-pct-2002-0411-che form-3.pdf
in-pct-2002-0411-che form-5.pdf
Patent Number | 214149 | ||||||||||||||||||||||||
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Indian Patent Application Number | IN/PCT/2002/411/CHE | ||||||||||||||||||||||||
PG Journal Number | 13/2008 | ||||||||||||||||||||||||
Publication Date | 31-Mar-2008 | ||||||||||||||||||||||||
Grant Date | 05-Feb-2008 | ||||||||||||||||||||||||
Date of Filing | 18-Mar-2002 | ||||||||||||||||||||||||
Name of Patentee | NOVARTIS AG | ||||||||||||||||||||||||
Applicant Address | Schwarzwaldallee 215, 4058 Basel, | ||||||||||||||||||||||||
Inventors:
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PCT International Classification Number | C07C 211/52 | ||||||||||||||||||||||||
PCT International Application Number | PCT/EP2000/009346 | ||||||||||||||||||||||||
PCT International Filing date | 2000-09-25 | ||||||||||||||||||||||||
PCT Conventions:
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