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Am J Physiol Regul Integr Comp Physiol 292: R794-R799, 2007. First published September 21, 2006; doi:10.1152/ajpregu.00424.2006
0363-6119/07 $8.00
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Sex Differences in Renal and Cardiovascular Function: Physiology and Pathophysiology

Effect of sex hormones on renal estrogen and angiotensin type 1 receptors in female and male rats

Jennifer L. Rogers,1,* Adam R. Mitchell,1,* Christine Maric,1,2,3 Kathryn Sandberg,1,2,3 Adam Myers,1,3 and Susan E. Mulroney1,3

Departments of 1Physiology and Biophysics and 2Medicine and 3Center for the Study of Sex Differences in Health, Aging and Disease, Georgetown University School of Medicine, Washington, DC

Submitted 6 June 2006 ; accepted in final form 19 September 2006

Although the mechanisms are not understood, evidence suggests that 17beta-estradiol (E2) confers protection from cardiovascular and renal complications in many diseases. We have reported that E2 decreases angiotensin type 1 receptors (AT1Rs) in different tissues and hypothesize that E2 exerts tonic inhibition on AT1Rs, reducing effects of ANG II. This study determined the effects of E2 and dihydrotestosterone (DHT) on cortical estrogen receptors (ERs) and glomerular AT1R binding in rats. Animals underwent sham operation, ovariectomy (Ovx) or orchidectomy (Cas) and were treated (Ovx ± E2; Cas ± DHT) for 3 wk. Cortical ER{alpha} protein was 2.5 times greater, and ERbeta was 80% less in females vs. males (P < 0.01). Glomerular AT1R binding was lower in females than males [4,657 ± 838 vs. 7,457 ± 467 counts per minute (cpm), P < 0.01]. Ovx reduced ER{alpha} protein by 50%, whereas E2 increased ER{alpha} expression after Ovx. The decrease in cortical ER{alpha} in Ovx rats was associated with a significant increase in AT1R binding (6,908 ± 609 cpm), and E2 prevented this increase. There was no change in ER{alpha} or AT1R binding following Cas ± DHT (25 mg) treatment, although Cas did elevate cortical ERbeta (P < 0.01). Interestingly, the high dose DHT (200 mg) elevated ER{alpha} 150% above intact levels and profoundly decreased AT1R binding (1,824 ± 705 cpm, P < 0.001 vs. intact male). This indicates that under normal conditions, glomerular AT1R binding is significantly greater in male than female animals, which may be important in development of cardiovascular and renal disease in males. Furthermore, E2 regulates ER{alpha} and is inversely associated with glomerular AT1R binding, supporting our hypothesis that E2 tonically suppresses AT1Rs and suggesting a potential mechanism for the protective effects of estrogen.

kidney; 17beta-estradiol; dihydrotestosterone; testosterone; ovariectomy; castration; angiotensin II



Address for reprint requests and other correspondence: S. E. Mulroney, Georgetown Univ. Medical Center, Box 571640, Washington, DC 20057 (e-mail: mulrones{at}georgetown.edu)




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