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Metabolite ligands of estrogen receptor-beta reduce primate coronary hyperreactivity.

Rajesh G Mishra, Frank Z Stanczyk, Kenneth A Burry, Suzanne Oparil, Benita S Katzenellenbogen, Michele L Nealen, John A Katzenellenbogen, R Kent Hermsmeyer

American journal of physiology. Heart and circulatory physiology 2006 Jan


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    Previous reports showed that 17beta-estradiol implants attenuate in vivo coronary hyperreactivity (CH), characterized by long-duration vasoconstrictions (in coronary angiographic experiments), in menopausal rhesus monkeys. Prolonged Ca2+ contraction signals that correspond with CH in coronary vascular muscle cells (VMC) to the same dual-constrictor stimulus, serotonin + the thromboxane analog U-46619, in estrogen-deprived VMC were suppressed by >72 h in 17beta-estradiol. The purpose of this study was to test whether an endogenous estrogen metabolite with estrogen receptor-beta (ER-beta) binding activity, estriol (E3), suppresses in vivo and in vitro CH. E3 treatment in vivo for 4 wk significantly attenuated the angiographically evaluated vasoconstrictor response to intracoronary serotonin + U-46619 challenge. In vitro treatment of rhesus coronary VMC for >72 h with nanomolar E3 attenuated late Ca2+ signals. This reduction of late Ca2+ signals also appeared after >72 h of treatment with subnanomolar 5alpha-androstane-3beta,17beta-diol (3beta-Adiol), an endogenous dihydrotestosterone metabolite with ER-beta binding activity. R,R-tetrahydrochrysene, a selective ER-beta antagonist, significantly blocked the E3- and 3beta-Adiol-mediated attenuation of late Ca2+ signal increases. ER-beta and thromboxane-prostanoid receptor (TPR) were coexpressed in coronary arteries and aorta. In vivo E3 treatment attenuated aortic TPR expression. Furthermore, in vitro treatment with E3 or 3beta-Adiol downregulated TPR expression in VMC, which was blocked for both agonists by pretreatment with R,R-tetrahydrochrysene. E3- and 3beta-Adiol-mediated reduction in persistent Ca2+ signals is associated with ER-beta-mediated attenuation of TPR expression and may partly explain estrogen benefits in coronary vascular muscle.

    Citation

    Rajesh G Mishra, Frank Z Stanczyk, Kenneth A Burry, Suzanne Oparil, Benita S Katzenellenbogen, Michele L Nealen, John A Katzenellenbogen, R Kent Hermsmeyer. Metabolite ligands of estrogen receptor-beta reduce primate coronary hyperreactivity. American journal of physiology. Heart and circulatory physiology. 2006 Jan;290(1):H295-303

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    PMID: 16199482

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