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Sex‐specific alterations in NOS regulation of vascular function in aorta and mesenteric arteries from spontaneously hypertensive rats compared to Wistar Kyoto rats
Author(s) -
Loria Analia S.,
Brinson Krystal N.,
Fox Brandon M.,
Sullivan Jennifer C.
Publication year - 2014
Publication title -
physiological reports
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.918
H-Index - 39
ISSN - 2051-817X
DOI - 10.14814/phy2.12125
Subject(s) - mesenteric arteries , vasoconstriction , medicine , endocrinology , phenylephrine , aorta , nitric oxide synthase , contraction (grammar) , vasodilation , nitric oxide , blood pressure , artery
The present study tested the hypothesis that spontaneously hypertensive rats ( SHR ) have impaired nitric oxide synthase ( NOS )‐mediated regulation of vascular function versus Wistar‐Kyoto rats ( WKY ). Aorta and small mesenteric arteries were studied from male and female SHR (M SHR and F SHR ) and WKY (M WKY and F WKY ). Phenylephrine ( PE )‐induced vasoconstriction was greater in aorta of M SHR versus all others ( P  < 0.05); there were neither sex nor strain differences in PE contraction in mesenteric arteries. The NOS inhibitor l ‐Nitro‐Arginine Methyl Ester ( l ‐ NAME ) increased PE ‐induced vasoconstriction in all rats, although the increase was the least in male SHR ( P  < 0.05), revealing a blunted vasoconstrictor buffering capacity of NOS . l ‐ NAME increased sensitivity to PE ‐induced constriction only in mesenteric arteries of SHR , although, the maximal percent increase in contraction was comparable among groups. ACh‐induced relaxation was also less in aorta from M SHR versus all others ( P  < 0.05). ACh relaxation was comparable among groups in mesenteric arteries, although SHR exhibited a greater NOS component to ACh‐induced relaxation than WKY . To gain mechanistic insight into sex and strain differences in vascular function, NOS activity and NOS 3 protein expression were measured. Aortic NOS activity was comparable between groups and M SHR had greater NOS 3 expression than M WKY . In contrast, although vascular function was largely maintained in mesenteric arteries of SHR , NOS activity was less in SHR versus WKY . In conclusion, M SHR exhibit a decrease in NOS regulation of vascular function compared to F SHR and WKY , although this is not mediated by decreases in NOS activity and/or expression.

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