Endothelin, sex and hypertension

11 December 2007

journal article
review article
Published by Portland Press Ltd. in Clinical Science

Vol. 114 (2) , 85-97
https://doi.org/10.1042/cs20070169

Abstract

The ETs (endothelins) comprise a family of three 21-amino-acid peptides (ET-1, ET-2 and ET-3) and 31-amino-acid ETs (ET-11–31, ET-21–31 and ET-31–31). ET-1 is synthesized from a biologically inactive precursor, big ET-1, by ECEs (ET-converting enzymes). The actions of ET-1 are mediated through activation of the G-protein-coupled ETA and ETB receptors, which are found in a variety of cells in the cardiovascular and renal systems. ET-1 has potent vasoconstrictor, mitogenic, pro-inflammatory and antinatriuretic properties, which have been implicated in the pathophysiology of a number of cardiovascular diseases. Overexpression of ET-1 has been consistently described in salt-sensitive models of hypertension and in models of renal failure, and has been associated with disease progression. Sex differences are observed in many aspects of mammalian cardiovascular function and pathology. Hypertension, as well as other cardiovascular diseases, is more common in men than in women of similar age. In experimental models of hypertension, males develop an earlier and more severe form of hypertension than do females. Although the reasons for these differences are not well established, the effects of gonadal hormones on arterial, neural and renal mechanisms that control blood pressure are considered contributing factors. Sex differences in the ET-1 pathway, with males displaying higher ET-1 levels, greater ET-1-mediated vasoconstrictor and enhanced pressor responses in comparison with females, are addressed in the present review. Sex-associated differences in the number and function of ETB receptors appear to be particularly important in the specific characteristics of hypertension between females and males. Although the gonadal hormones modulate some of the differences in the ET pathway in the cardiovascular system, a better understanding of the exact mechanisms involved in sex-related differences in this peptidergic system is needed. With further insights into these differences, we may learn that men and women could require different antihypertensive regimens.

Keywords

This publication has 116 references indexed in Scilit:

Deletion of Endothelial Cell Endothelin B Receptors Does Not Affect Blood Pressure or Sensitivity to Salt
Hypertension, 2006
Endothelium-Restricted Overexpression of Human Endothelin-1 Causes Vascular Remodeling and Endothelial Dysfunction
Circulation, 2004
Ethnic Differences in the Vasoconstrictor Activity of Endogenous Endothelin-1 in Hypertensive Patients
Circulation, 2004
Vascular ECE-1 mRNA expression decreases in response to estrogens
Life Sciences, 2003
Mechanisms of 17β-estradiol on the production of ET-1 in ovariectomized rats
Life Sciences, 2003
Endothelin-1 Increases Vascular Superoxide via Endothelin _A –NADPH Oxidase Pathway in Low-Renin Hypertension
Circulation, 2003
Sexual dimorphism in renal ischemia-reperfusion injury in rats: Possible role of endothelin
Kidney International, 2002
Estrogen Attenuates Endothelin-1 Production by Bovine Endothelial Cells via Estrogen Receptor
Biochemical and Biophysical Research Communications, 1998
Novel 31-Amino-Acid-Length Endothelins Cause Constriction of Vascular Smooth Muscle
Biochemical and Biophysical Research Communications, 1998
Effects of the 3-hydroxy-3-methylglutaryl-CoA reductase inhibitors, atorvastatin and simvastatin, on the expression of endothelin-1 and endothelial nitric oxide synthase in vascular endothelial cells.
Journal of Clinical Investigation, 1998