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Equilin displays similar endothelium-independent vasodilator potential to 17β-estradiol regardless of lower potential to inhibit calcium entry.

Authors :
Filgueira FP
Lobato NS
Nascimento DL
Ceravolo GS
Giachini FRC
Lima VV
Dantas AP
Fortes ZB
Webb RC
Tostes RC
Carvalho MHC
Source :
Steroids [Steroids] 2019 Jan; Vol. 141, pp. 46-54. Date of Electronic Publication: 2018 Nov 17.
Publication Year :
2019

Abstract

Conjugated equine estrogens (CEE) have been widely used by women who seek to relieve symptoms of menopause. Despite evidence describing protective effects against risk factors for cardiovascular diseases by naturally occurring estrogens, little is known about the vascular effects of equilin, one of the main components of CEE and not physiologically present in women. In this regard, the present study aims to compare the vascular effects of equilin in an experimental model of hypertension with those induced by 17β-estradiol. Resistance mesenteric arteries from female spontaneously hypertensive rats (SHR) were used for recording isometric tension in a small vessel myograph. As effectively as 17β-estradiol, equilin evoked a concentration-dependent relaxation in mesenteric arteries from female SHRs contracted with KCl, U46619, PDBu or ET-1. Equilin-induced vasodilation does not involve classical estrogen receptor activation, since the estrogen receptor antagonist (ICI 182,780) failed to inhibit relaxation in U46619-precontracted mesenteric arteries. Vasorelaxation was not affected by either endothelium removal or by inhibiting the release or action of endothelium-derived factors. Incubation with L-NAME (NOS inhibitor), ODQ (guanylyl cyclase inhibitor) or KT5823 (inhibitor of protein kinase G) did not affect equilin-induced relaxation. Similarly, indomethacin (COX inhibitor) or blockage of potassium channels with tetraethylammonium, glibenclamide, 4-aminopyridine, or ouabain did not affect equilin-induced relaxation. Inhibitors of adenylyl cyclase SQ22536 or protein kinase A (KT5720) also had no effects on equilin-induced relaxation. While 17β-estradiol inhibited calcium (Ca <superscript>2+</superscript> ) -induced contractions in high-K <superscript>+</superscript> depolarization medium in a concentration-dependent manner, equilin induced a slight rightward-shift in the contractile responses to Ca <superscript>2+</superscript> . Comparable pattern of responses were observed in the concentration-response curves to (S)-(-)-Bay K 8644, a L-type Ca <superscript>2+</superscript> channel activator. Equilin was unable to block the transitory contraction produced by caffeine-induced Ca <superscript>2+</superscript> release from intracellular stores. In conclusion, equilin blocks L-type Ca <superscript>2+</superscript> channels less effectively than 17β-estradiol. Despite its lower effectiveness, equilin equally relaxes resistance mesenteric arteries by blocking Ca <superscript>2+</superscript> entry on smooth muscle.<br /> (Copyright © 2018. Published by Elsevier Inc.)

Subjects

Subjects :
Animals
Endoplasmic Reticulum metabolism
Female
Rats
Rats, Inbred SHR
Calcium metabolism
Endoplasmic Reticulum drug effects
Equilin pharmacology
Estradiol pharmacology
Vasodilation drug effects
Vasodilator Agents pharmacology

Details

Language :
English
ISSN :
1878-5867
Volume :
141
Database :
MEDLINE
Journal :
Steroids
Publication Type :
Academic Journal
Accession number :
30458188
Full Text :
https://doi.org/10.1016/j.steroids.2018.11.006
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