ET-CORM Mediated Vasorelaxation of Small Mesenteric Arteries: Involvement of Kv7 Potassium Channels

ET-CORM Mediated Vasorelaxation of Small Mesenteric Arteries: Involvement of Kv7 Potassium Channels

Although the vasoactive properties of carbon monoxide (CO) have been extensively studied, the mechanism by which CO mediates vasodilation is not completely understood. Through-out published studies on CO mediated vasodilation there is inconsistency on the type of K+-channels that are activated by CO...

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Main Authors: Danfeng Zhang, Bernhard M. Krause, Hans-Günther Schmalz, Paulus Wohlfart, Benito A. Yard, Rudolf Schubert
Format: Article
Language:English
Published: Frontiers Media S.A. 2021-09-01
Series:Frontiers in Pharmacology
Subjects:
vasorelaxation
carbon monoxide
potassium channels
rat
mesenteric arteries
Online Access:https://www.frontiersin.org/articles/10.3389/fphar.2021.702392/full
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spelling doaj-f86381ab7d1e4e40986c3c53dcb6af132021-09-06T04:23:43ZengFrontiers Media S.A.Frontiers in Pharmacology1663-98122021-09-011210.3389/fphar.2021.702392702392ET-CORM Mediated Vasorelaxation of Small Mesenteric Arteries: Involvement of Kv7 Potassium ChannelsDanfeng Zhang0Danfeng Zhang1Bernhard M. Krause2Hans-Günther Schmalz3Paulus Wohlfart4Benito A. Yard5Benito A. Yard6Rudolf Schubert7Rudolf Schubert8Department of Nephrology, Endocrinology and Rheumatology, Fifth Medical Department of Medicine, Medical Faculty Mannheim, University of Heidelberg, Mannheim, GermanyDepartment of Nephrology, the Second Hospital of Anhui Medical University, Hefei, ChinaDepartment of Chemistry, University of Cologne, Cologne, GermanyDepartment of Chemistry, University of Cologne, Cologne, GermanyDiabetes Research, Sanofi Aventis Deutschland GmbH, Frankfurt, GermanyDepartment of Nephrology, Endocrinology and Rheumatology, Fifth Medical Department of Medicine, Medical Faculty Mannheim, University of Heidelberg, Mannheim, GermanyEuropean Center of Angioscience (ECAS), Research Division Cardiovascular Physiology, Medical Faculty Mannheim, Heidelberg University, Frankfurt, GermanyEuropean Center of Angioscience (ECAS), Research Division Cardiovascular Physiology, Medical Faculty Mannheim, Heidelberg University, Frankfurt, GermanyPhysiology, Institute of Theoretical Medicine, Medical Faculty, University of Augsburg, Augsburg, GermanyAlthough the vasoactive properties of carbon monoxide (CO) have been extensively studied, the mechanism by which CO mediates vasodilation is not completely understood. Through-out published studies on CO mediated vasodilation there is inconsistency on the type of K+-channels that are activated by CO releasing molecules (CORMs). Since the vasorelaxation properties of enzyme triggered CORMs (ET-CORMs) have not been studied thus far, we first assessed if ET-CORMs can mediate vasodilation of small mesenteric arteries and subsequently addressed the role of soluble guanylate cyclase (sGC) and that of K-channels herein. To this end, 3 different types of ET-CORMs that either contain acetate (rac-1 and rac-4) or pivalate (rac-8) as ester functionality, were tested ex vivo on methoxamine pre-contracted small rat mesenteric arteries in a myograph setting. Pre-contracted mesenteric arteries strongly dilated upon treatment with both types of acetate containing ET-CORMs (rac-1 and rac-4), while treatment with the pivalate containing ET-CORM (rac-8) resulted in no vasodilation. Pre-treatment of mesenteric arteries with the sGC inhibitor ODQ abolished rac-4 mediated vasodilation, similar as for the known sGC activator SNP. Likewise, rac-4 mediated vasodilation did not occur in KCL pretreated mesenteric arteries. Although mesenteric arteries abundantly expressed a variety of K+-channels only Kv7 channels were found to be of functional relevance for rac-4 mediated vasodilation. In conclusion the current results identified Kv7 channels as the main channel by which rac-4 mediates vasodilation. In keeping with the central role of Kv7 in the control of vascular tone and peripheral resistance these promising ex-vivo data warrant further in vivo studies, particularly in models of primary hypertension or cardiac diseases, to assess the potential use of ET-CORMs in these diseases.https://www.frontiersin.org/articles/10.3389/fphar.2021.702392/fullvasorelaxationcarbon monoxidepotassium channelsratmesenteric arteries
collection DOAJ
language English
format Article
sources DOAJ
author Danfeng Zhang
Danfeng Zhang
Bernhard M. Krause
Hans-Günther Schmalz
Paulus Wohlfart
Benito A. Yard
Benito A. Yard
Rudolf Schubert
Rudolf Schubert
spellingShingle Danfeng Zhang
Danfeng Zhang
Bernhard M. Krause
Hans-Günther Schmalz
Paulus Wohlfart
Benito A. Yard
Benito A. Yard
Rudolf Schubert
Rudolf Schubert
ET-CORM Mediated Vasorelaxation of Small Mesenteric Arteries: Involvement of Kv7 Potassium Channels
Frontiers in Pharmacology
vasorelaxation
carbon monoxide
potassium channels
rat
mesenteric arteries
author_facet Danfeng Zhang
Danfeng Zhang
Bernhard M. Krause
Hans-Günther Schmalz
Paulus Wohlfart
Benito A. Yard
Benito A. Yard
Rudolf Schubert
Rudolf Schubert
author_sort Danfeng Zhang
title ET-CORM Mediated Vasorelaxation of Small Mesenteric Arteries: Involvement of Kv7 Potassium Channels
title_short ET-CORM Mediated Vasorelaxation of Small Mesenteric Arteries: Involvement of Kv7 Potassium Channels
title_full ET-CORM Mediated Vasorelaxation of Small Mesenteric Arteries: Involvement of Kv7 Potassium Channels
title_fullStr ET-CORM Mediated Vasorelaxation of Small Mesenteric Arteries: Involvement of Kv7 Potassium Channels
title_full_unstemmed ET-CORM Mediated Vasorelaxation of Small Mesenteric Arteries: Involvement of Kv7 Potassium Channels
title_sort et-corm mediated vasorelaxation of small mesenteric arteries: involvement of kv7 potassium channels
publisher Frontiers Media S.A.
series Frontiers in Pharmacology
issn 1663-9812
publishDate 2021-09-01
description Although the vasoactive properties of carbon monoxide (CO) have been extensively studied, the mechanism by which CO mediates vasodilation is not completely understood. Through-out published studies on CO mediated vasodilation there is inconsistency on the type of K+-channels that are activated by CO releasing molecules (CORMs). Since the vasorelaxation properties of enzyme triggered CORMs (ET-CORMs) have not been studied thus far, we first assessed if ET-CORMs can mediate vasodilation of small mesenteric arteries and subsequently addressed the role of soluble guanylate cyclase (sGC) and that of K-channels herein. To this end, 3 different types of ET-CORMs that either contain acetate (rac-1 and rac-4) or pivalate (rac-8) as ester functionality, were tested ex vivo on methoxamine pre-contracted small rat mesenteric arteries in a myograph setting. Pre-contracted mesenteric arteries strongly dilated upon treatment with both types of acetate containing ET-CORMs (rac-1 and rac-4), while treatment with the pivalate containing ET-CORM (rac-8) resulted in no vasodilation. Pre-treatment of mesenteric arteries with the sGC inhibitor ODQ abolished rac-4 mediated vasodilation, similar as for the known sGC activator SNP. Likewise, rac-4 mediated vasodilation did not occur in KCL pretreated mesenteric arteries. Although mesenteric arteries abundantly expressed a variety of K+-channels only Kv7 channels were found to be of functional relevance for rac-4 mediated vasodilation. In conclusion the current results identified Kv7 channels as the main channel by which rac-4 mediates vasodilation. In keeping with the central role of Kv7 in the control of vascular tone and peripheral resistance these promising ex-vivo data warrant further in vivo studies, particularly in models of primary hypertension or cardiac diseases, to assess the potential use of ET-CORMs in these diseases.
topic vasorelaxation
carbon monoxide
potassium channels
rat
mesenteric arteries
url https://www.frontiersin.org/articles/10.3389/fphar.2021.702392/full
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