INHIBITION OF ESTROGEN BIOSYNTHESIS AND ITS CONSEQUENCES ON GONADOTROPIN-SECRETION IN THE MALE

被引：53

作者：

BHATNAGAR, AS ^{[1
]}

MULLER, P ^{[1
]}

SCHENKEL, L ^{[1
]}

TRUNET, PF ^{[1
]}

BEH, I ^{[1
]}

SCHIEWECK, K ^{[1
]}

机构：

[1] CIBA GEIGY AG,DIV PHARMACEUT,DEPT DEV,CH-4002 BASEL,SWITZERLAND

来源：

JOURNAL OF STEROID BIOCHEMISTRY AND MOLECULAR BIOLOGY | 1992年 / 41卷 / 3-8期

关键词：

D O I：

10.1016/0960-0760(92)90369-T

中图分类号：

Q5 [生物化学]; Q7 [分子生物学];

学科分类号：

071010 ; 081704 ;

摘要：

Of the gonadal steroids in the male, testosterone is the most important regulator of gonadotrophin secretion. However, whether testosterone affects gonadotrophin secretion directly or whether it must first be aromatized to estrogens is controversial. We have reported extensively on the endocrine and anti-tumor effects of the non-steroidal aromatase inhibitors CGS 16949A and CGS 20267 in adult female rats. In these animals, both inhibitors potently and selectively inhibit estrogen biosynthesis. Thus these agents can be effectively used in studying estrogen-dependent processes. CGS 16949A was administered for 14 days to adult male rats, over a dose range which in females suppresses estradiol and elevates LH. In male rats a suppression of estradiol was seen, however, there was no significant effect on either serum LH or on the weights of androgen-dependent organs. CGS 16949A, when administered to healthy men at a dose of 1 mg b.i.d. for 10 days, causes a significant fall in plasma estradiol and significant elevations of plasma FSH and testosterone. Dose-dependent suppression of serum estradiol and an increase in serum testosterone and LH are seen after administration of single oral doses of CGS 20267. These results indicate that in the male rat, inhibition of aromatization of testosterone to estrogens does not influence gonadotrophin secretion whereas in men the negative feedback exerted by testosterone on gonadotrophin secretion is dependent on the aromatization of testosterone to estrogens.

引用

页码：437 / 443

页数：7

共 30 条

[1]

AWONIYI C, 1986, J ANDROL, V7, P234

[2]

Bhatnagar A S, 1990, J Enzyme Inhib, V4, P179, DOI 10.3109/14756369009040740

[3] NOVEL AROMATASE INHIBITORS [J].

BHATNAGAR, AS ;

HAUSLER, A ;

SCHIEWECK, K ;

BROWNE, LJ ;

BOWMAN, R ;

STEELE, RE .

JOURNAL OF STEROID BIOCHEMISTRY AND MOLECULAR BIOLOGY, 1990, 37 (03) :363-367

[4] INHIBITORS OF ESTROGEN BIOSYNTHESIS - PRECLINICAL STUDIES WITH CGS 16949A, A NEW NONSTEROIDAL AROMATASE INHIBITOR [J].

BHATNAGAR, AS ;

SCHIEWECK, K ;

HAUSLER, A ;

BROWNE, LJ ;

STEELE, RE .

PROCEEDINGS OF THE ROYAL SOCIETY OF EDINBURGH SECTION B-BIOLOGICAL SCIENCES, 1989, 95 :293-303

[5] HIGHLY SELECTIVE-INHIBITION OF ESTROGEN BIOSYNTHESIS BY CGS-20267, A NEW NONSTEROIDAL AROMATASE INHIBITOR [J].

BHATNAGAR, AS ;

HAUSLER, A ;

SCHIEWECK, K ;

LANG, M ;

BOWMAN, R .

JOURNAL OF STEROID BIOCHEMISTRY AND MOLECULAR BIOLOGY, 1990, 37 (06) :1021-1027

[6]

Bogdanove E M, 1975, Recent Prog Horm Res, V31, P567

[7]

DEPALATIS L, 1978, J REPROD FERTIL, V52, P201, DOI 10.1530/jrf.0.0520201

[8] POTENCY AND SELECTIVITY OF THE NONSTEROIDAL AROMATASE INHIBITOR CGS 16949A IN POSTMENOPAUSAL BREAST-CANCER PATIENTS [J].

DOWSETT, M ;

STEIN, RC ;

MEHTA, A ;

COOMBES, RC .

CLINICAL ENDOCRINOLOGY, 1990, 32 (05) :623-634

[9] INHIBITION OF AROMATIZATION STIMULATES LUTEINIZING-HORMONE AND TESTOSTERONE SECRETION IN ADULT MALE RHESUS-MONKEYS [J].

ELLINWOOD, WE ;

HESS, DL ;

ROSELLI, CE ;

SPIES, HG ;

RESKO, JA .

JOURNAL OF CLINICAL ENDOCRINOLOGY & METABOLISM, 1984, 59 (06) :1088-1096

[10] AROMATASE INHIBITION IN THE DOG .1. EFFECT ON SERUM LH, SERUM TESTOSTERONE CONCENTRATIONS, TESTICULAR SECRETIONS AND SPERMATOGENESIS [J].

JUNIEWICZ, PE ;

OESTERLING, JE ;

WALTERS, JR ;

STEELE, RE ;

NISWENDER, GD ;

COFFEY, DS ;

EWING, LL .

JOURNAL OF UROLOGY, 1988, 139 (04) :827-831

← 1 2 3 →