COMPARATIVE EFFECTS OF A SERIES OF PROLACTIN INHIBITORS, 17BETA-ESTRADIOL AND 2ALPHA-METHYLDIHYDROTESTOSTERONE PROPIONATE, ON GROWTH OF 7,12-DIMETHYLBENZ(A)ANTHRACENE-INDUCED RAT MAMMARY CARCINOMAS
- 1 January 1977
- journal article
- research article
- Vol. 37 (11) , 3932-3938
Abstract
Eight ergot alkaloids and ergoline derivatives, effective prolactin inhibitors, were tested for activity against DMBA[7,12-dimethylbenz(a)anthracene]-induced rat mammary carcinomas. Compounds were administered daily, 5 times/week for 4 wk, and rats were observed for an additional 4 wk. Groups treated with androgen and estrogen were used as positive controls. Those ergot compounds and ergolines that proved to be highly effective in reducing tumor size or in inducing regression of tumors to nonpalpability were Deprenon (D-6-methyl-8-ergolin-l-ylacetic acid amide) and ergocriptine, effective to an intermediate degree were Dironyl [N-(D-6-methyl-8-isoergolin-l-yl)-N'',N''-diethylurea], ergocornine, and Lysenyl [N-(D-6-methyl-8-isoergolenyl)-N'',N''-diethylurea]; and effective to a minimal degree were Lergotrile (2-chloro-6-methylergoline-8.beta.-acetonitrile), CB-154 [bromocriptine] and 6605-VUFB (D-6-methyl-8-cyanomethylergolin-1). Remission of many individual carcinomas was brief, and duration of complete regression (all tumors in the rat were nonpalpable) was 10 wk.This publication has 8 references indexed in Scilit:
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