Synthetic Antigonadotropins. IV. Bromotriphenylethylenes - Journal of

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July 1965

SYNTHETIC ,4NTIGOiTADOTROPINS.

Synthetic Antigonadotropins.

IT’

415

IV. Bromotriphenylethylenes

H. H. FOX,‘J. T. GIBAS,H. L. LEE, AND A. BORIS Besearch Laboratories, H o f m a n n - L a Roche, Inc., S u t l e y , .I-eu; Jersey Receiued February 12, 1966

-2series of bromotriphenylethylene derivatives has been prepared, every member of Thich tested so far has shown marked antigonadotropic and estrogenic activity.

Previous work in this continuing study2 has shown that the antigonadotropic activity of triarylethylenes was closely dependent upon maintaining the integrity of the basic triphenylethylene structure. (C6H5)26=6HC+jHj Activity was lost when (1) a pyridine ring or cycloalkyl group was substituted for one of the phenyl groups a t C-1 ; ( 2 ) the two phenyl groups at C-1 were bridged; ( 3 ) a cyclopropyl group was substituted for the ethylene link; or (4) a nitrogen atom was substituted for C-2. However, the fact that a conipound possessed a triphenylethylene structure was no guarantee of activity since activity was also lost in the presence of certain substituents on the phenyl group^.^ On the basis of earlier work in this field, it was decided that of the various changes which could be made in the triphenylethylene structure pictured above, one that seemed most desirable would be the replacement of the hydrogen a t C-2 with a halogen to produce halotriphenylethylenes. The halogen chosen mas bromine and the present report concerns the synthesis of bromotriphenylethylenes of the following structure.

‘f C= ‘ I

I

c

I

X = F, CF,,CI f = H, OH,CH30,C&CHZO

These compounds were prepared, in general, by treating the appropriate triphenylethylerie in glacial acetic acid solution with 1 molecular equiv. of bromine a t room temperature. After standing for 0.5-1 hr., the reaction mixture was refluxed for 2-3 hr., the solvent was removed, and the solid product was recrystallized froin the appropriate solvent (usually ethanol). The above procedure n as not applicable to those conipounds in which T = OH. htteiiipts to brominate the hydroxylated compounds directly gave anonialous results, probably due to broiiiination of the phenolic ring. To circumvent this difficulty attempts were made to demethylate the inethoxy analogs. lT7heri these attempts also failed, recourse was had to benzyloxy derivatives of the triphenylethylenes. Bromination of the benzyloxy derivatives using acetic acid as a solvent resulted i n considerable decomposition u-ith the odor of benzalde(11 Cyclo Chemical Corp. Los Angeleu, Calif. (2) ( n ) H. H. Fox J. T.Gibas H. L. Lee and 1 L3o11a J . X e d C h m . 7, 506 (1964), (b) H. H. Fox, J. T. Glbas, H. L. Lee, and A. Bans, zbzd., 7 , 790 (1964). ( 3 ) H. H. Fox, .J. T.Gibas, H. L. h e , and 1. Boris, zhzd., 8 , 250 (lq6.5).

hyde much in evidence. Chloroform proved sat isfactory as a solvent in these cases and bromination was carried out by the addition of bromine at the reflux temperature of chloroform followed by debenzylation to give the desired hydroxylated bromo derivatives. This sequence of reactions is illustrated in the following equation.

HO

Q c=c,

The coinpourids of this series exist as cis-trans isomers. I n some instances, both isomeric foriiis were isolated and arbitrarily identified as “a” and “p” forms. S o effort was made to determine their absolute configuration. With the exception of 1,l-diphenyl-2bromo-2- (p-chlorophenyl) et hylene which had previously been prepared by Tadros, et u Z . , ~ all of the coinpounds reported here and listed in Table I are new. Pharmacology.-All of the bromotriphenylethylene derivatives prepared in this study showed marked antigonadotropic and marked estrogenic activity when tested as previously described.*!: I t mas apparent that bromination of the triphenylethylene enhanced both the antigonadotropic and estrogenic activity inasmuch as the brominated derivatives were inany times more active than their unbroniiriated precursors. Indeed, three triphenylethylene derivatives which had no activity, namely, l,l-diphenyl-2-(ni-trifluoromethyIphenyl)ethylene, l-(p-benzyloxphenyl)-l-phenyl-2-(p-fluorophenyl)ethylene, and 1-(p-benzyloxyphenyl)-1-phenyl2-(nz-fluorophenyl)ethylerie, all gave active bromo derivatives. The antigonadotropic and estrogenic activities of the compounds described herein are listed in Table 11. Where the estrogenic dose was 0.1 nig., ovariectomized rats were used. The antigonadotropic activity of thew ( 4 j JV, Tadros, K . Farallst, a n d .J. 31. Robson, J . Ciicm. Soc., 4YY (19.19). ( 5 ) A. Boris and H. H. F o x , .4rr/i. intern. Phurmncodun., 161, 475 (1964).

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