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Estrogen receptor antagonism uncovers gender-dimorphic suppression of whole body fat oxidation in humans: differential effects of tamoxifen on the GH and gonadal axes

Abstract

CONTEXT: Tamoxifen, a selective estrogen receptor modulator, suppresses GH secretion in women but not in men. It increases testosterone levels in men. As GH and testosterone stimulate fat metabolism, the metabolic consequences of tamoxifen may be greater in women than in men. OBJECTIVE: To determine whether tamoxifen suppresses fat oxidation (Fox) to a greater degree in women than in men. DESIGN: An open-label study of ten healthy postmenopausal women and ten healthy men receiving 2-week treatment with tamoxifen (20 mg/day). ENDPOINT MEASURES: GH response to arginine stimulation, serum levels of IGF1, testosterone and LH (men only), sex hormone binding globulin (SHBG) and whole body basal and postprandial Fox. RESULTS: In women, tamoxifen significantly reduced the mean GH response to arginine stimulation (Delta -87%, P<0.05) and circulating IGF1 levels (Delta -23.5+/-5.4%, P<0.01). Tamoxifen reduced postprandial Fox in women (Delta -34.6+/-10.3%; P<0.05). In men, tamoxifen did not affect the GH response to arginine stimulation but significantly reduced mean IGF1 levels (Delta -24.8+/-6.1%, P<0.01). Tamoxifen increased mean testosterone levels (Delta 52+/-14.2%; P<0.01). Fox was not significantly affected by tamoxifen in men. CONCLUSION: Tamoxifen attenuated the GH response to stimulation and reduced postprandial Fox in women but not in men. We conclude that at a therapeutic dose, the suppressive effect of tamoxifen on fat metabolism is gender-dependent. Higher testosterone levels may mitigate the suppression of GH secretion and Fox during tamoxifen treatment in men.

Type Journal
ISBN 1479-683X (Electronic) 0804-4643 (Linking)
Authors Birzniece, V. ; Ho, K. K.;
Responsible Garvan Author (missing name)
Publisher Name EUROPEAN JOURNAL OF ENDOCRINOLOGY
Published Date 2015-01-01
Published Volume 173
Published Issue 4
Published Pages 479-87
Status Published in-print
URL link to publisher's version http://www.ncbi.nlm.nih.gov/pubmed/26199431