THE ACUTE ESTROGENIC DILATION OF RAT AORTA IS MEDIATED SOLELY BY SELECTIVE ESTROGEN RECEPTOR-{alpha}AGONISTS AND IS ABOLISHED BY ESTROGEN DEPRIVATION

doi:10.1124/jpet.104.082867

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First published on February 18, 2005; DOI: 10.1124/jpet.104.082867

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Received for publication December 27, 2004.
Revised February 15, 2005.
Accepted for publication February 15, 2005.

THE ACUTE ESTROGENIC DILATION OF RAT AORTA IS MEDIATED SOLELY BY SELECTIVE ESTROGEN RECEPTOR- ${alpha}$ AGONISTS AND IS ABOLISHED BY ESTROGEN DEPRIVATION

Chiara Bolego ¹, Andrea Cignarella ¹^*, Paola Sanvito ¹, Valeria Pelosi ¹, Fabio Pellegatta ¹, Lina Puglisi ¹, Christian Pinna ¹

¹ University of Milan

^* Address correspondence to: E-mail: andrea.cignarella{at}unimi.it

Abstract

Estrogen is known to induce rapid vasodilatory response in isolatedarteries. Because estrogen is a non-selective receptor agonist,the involvement of estrogen receptor (ER) subtypes in acuteestrogenic responses has remained elusive. Acute administrationof the selective ER ${alpha}$ agonist 4,4',4''-(4-propyl- [¹H]-pyrazole-1,3,5-triyl)tris-phenol (PPT) to precontracted aortic rings from intactfemale rats dose-dependently induced an ER-dependent vascularrelaxation fully overlapping to that induced by 17 ${beta}$ -estradiol.By contrast, the selective ER ${beta}$ agonist 2,3-bis(4-hydroxyphenyl)-propionitrile(DPN) had no acute effect on vasomotion. This short-term vasorelaxantaction of PPT was abolished by the NO synthase inhibitor L-NAMEand by endothelium removal. In aortic tissues from ovariectomized(OVX) rats, however, neither 17 ${beta}$ -estradiol nor PPT induced acutevascular relaxation. The effect of PPT was restored in preparationsfrom estrogen-replaced OVX rats while DPN remained ineffectiveeven after estrogen replacement. PPT acted through an ER-dependentmechanism, as shown by impaired response in the presence ofthe anti-estrogen ICI 182,780. Accordingly, isolated rat aorticendothelial cells expressed both ER ${alpha}$ and ER ${beta}$ . These data showthat selective ER ${alpha}$ but not ER ${beta}$ agonists reproduced the acute vasodilationof estrogen via a receptor-mediated pathway in the aorta fromintact as well as 17 ${beta}$ -estradiol-replaced OVX rats. This beneficialeffect was undetectable in tissues from OVX rats. Selectivepharmacological targeting of ER subtypes may thus representa novel and promising approach in the treatment of vasculardisease.

Key words: aorta, endothelium, estrogen, ovariectomy, selective estrogen receptor agonists, vasodilation

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THE ACUTE ESTROGENIC DILATION OF RAT AORTA IS MEDIATED SOLELY BY SELECTIVE ESTROGEN RECEPTOR-AGONISTS AND IS ABOLISHED BY ESTROGEN DEPRIVATION

THE ACUTE ESTROGENIC DILATION OF RAT AORTA IS MEDIATED SOLELY BY SELECTIVE ESTROGEN RECEPTOR- ${alpha}$ AGONISTS AND IS ABOLISHED BY ESTROGEN DEPRIVATION