Angiotensin AT(1) – α(2C)-Adrenoceptor Interaction Disturbs α(2A)-auto-Inhibition of Catecholamine Release in Hypertensive Rats

α(2)-Adrenoceptors lower central sympathetic output and peripheral catecholamine release, and thus may prevent sympathetic hyperactivity and hypertension. α(2)AR also influence vascular tension. These α(2)AR are malfunctioning in spontaneously hypertensive rats (SHR). Here I tested if an interaction...

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Autor principal: Berg, Torill
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2013
Materias:
Neuroscience
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3677154/
https://www.ncbi.nlm.nih.gov/pubmed/23772221
http://dx.doi.org/10.3389/fneur.2013.00070
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author Berg, Torill
author_facet Berg, Torill
author_sort Berg, Torill
collection PubMed
description α(2)-Adrenoceptors lower central sympathetic output and peripheral catecholamine release, and thus may prevent sympathetic hyperactivity and hypertension. α(2)AR also influence vascular tension. These α(2)AR are malfunctioning in spontaneously hypertensive rats (SHR). Here I tested if an interaction between α(2)AR subtypes and the angiotensin AT1 receptor (AT(1)R) precipitated these disorders. Blood pressure was monitored through a femoral artery catheter and cardiac output by ascending aorta flow in anesthetized rats. Catecholamine concentrations were determined in plasma collected at the end of a 15-min tyramine-infusion. Tyramine stimulates norepinephrine release through the re-uptake transporter, thus preventing re-uptake. Presynaptic control of vesicular release is therefore reflected as differences in overflow to plasma. Previous experiments showed surgical stress to activate some secretion of epinephrine, also subjected to α(2)AR-auto-inhibition. Normotensive rats (WKY) and SHR were pre-treated with (1) vehicle or α(2)AR-antagonist (L-659,066), followed by fadolmidine (α(2C>B>A) + α(1)AR-agonist), ST-91 (α(2non-A)-selective agonist), or m-nitrobiphenyline (α(2C)AR-agonist + α(2A+B)-antagonist), or (2) AT1R-antagonist losartan, losartan + L-659,066, or losartan + clonidine. In WKY, L-659,066 alone, L-659,066 + agonist or losartan + L-659,066 increased catecholamine overflow to plasma after tyramine and eliminated the norepinephrine-induced rise in total peripheral vascular resistance (TPR). In SHR, L-659,066 + fadolmidine/ST-91/m-nitrobiphenyline and losartan + L-659,066 greatly increased, and losartan + clonidine reduced, catecholamine concentrations, and L-659,066 + ST-91, losartan + L-659,066 and losartan + clonidine eliminated the tyramine-induced rise in TPR. Separately, these drugs had no effect in SHR. In conclusion, peripheral α(2C)AR-stimulation or AT(1)R-inhibition restored failing α(2A)AR-mediated auto-inhibition of norepinephrine and epinephrine release and control of TPR in SHR.
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spelling pubmed-36771542013-06-14 Angiotensin AT(1) – α(2C)-Adrenoceptor Interaction Disturbs α(2A)-auto-Inhibition of Catecholamine Release in Hypertensive Rats Berg, Torill Front Neurol Neuroscience α(2)-Adrenoceptors lower central sympathetic output and peripheral catecholamine release, and thus may prevent sympathetic hyperactivity and hypertension. α(2)AR also influence vascular tension. These α(2)AR are malfunctioning in spontaneously hypertensive rats (SHR). Here I tested if an interaction between α(2)AR subtypes and the angiotensin AT1 receptor (AT(1)R) precipitated these disorders. Blood pressure was monitored through a femoral artery catheter and cardiac output by ascending aorta flow in anesthetized rats. Catecholamine concentrations were determined in plasma collected at the end of a 15-min tyramine-infusion. Tyramine stimulates norepinephrine release through the re-uptake transporter, thus preventing re-uptake. Presynaptic control of vesicular release is therefore reflected as differences in overflow to plasma. Previous experiments showed surgical stress to activate some secretion of epinephrine, also subjected to α(2)AR-auto-inhibition. Normotensive rats (WKY) and SHR were pre-treated with (1) vehicle or α(2)AR-antagonist (L-659,066), followed by fadolmidine (α(2C>B>A) + α(1)AR-agonist), ST-91 (α(2non-A)-selective agonist), or m-nitrobiphenyline (α(2C)AR-agonist + α(2A+B)-antagonist), or (2) AT1R-antagonist losartan, losartan + L-659,066, or losartan + clonidine. In WKY, L-659,066 alone, L-659,066 + agonist or losartan + L-659,066 increased catecholamine overflow to plasma after tyramine and eliminated the norepinephrine-induced rise in total peripheral vascular resistance (TPR). In SHR, L-659,066 + fadolmidine/ST-91/m-nitrobiphenyline and losartan + L-659,066 greatly increased, and losartan + clonidine reduced, catecholamine concentrations, and L-659,066 + ST-91, losartan + L-659,066 and losartan + clonidine eliminated the tyramine-induced rise in TPR. Separately, these drugs had no effect in SHR. In conclusion, peripheral α(2C)AR-stimulation or AT(1)R-inhibition restored failing α(2A)AR-mediated auto-inhibition of norepinephrine and epinephrine release and control of TPR in SHR. Frontiers Media S.A. 2013-06-10 /pmc/articles/PMC3677154/ /pubmed/23772221 http://dx.doi.org/10.3389/fneur.2013.00070 Text en Copyright © 2013 Berg. http://creativecommons.org/licenses/by/3.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits use, distribution and reproduction in other forums, provided the original authors and source are credited and subject to any copyright notices concerning any third-party graphics etc.
spellingShingle Neuroscience
Berg, Torill
Angiotensin AT(1) – α(2C)-Adrenoceptor Interaction Disturbs α(2A)-auto-Inhibition of Catecholamine Release in Hypertensive Rats
title Angiotensin AT(1) – α(2C)-Adrenoceptor Interaction Disturbs α(2A)-auto-Inhibition of Catecholamine Release in Hypertensive Rats
title_full Angiotensin AT(1) – α(2C)-Adrenoceptor Interaction Disturbs α(2A)-auto-Inhibition of Catecholamine Release in Hypertensive Rats
title_fullStr Angiotensin AT(1) – α(2C)-Adrenoceptor Interaction Disturbs α(2A)-auto-Inhibition of Catecholamine Release in Hypertensive Rats
title_full_unstemmed Angiotensin AT(1) – α(2C)-Adrenoceptor Interaction Disturbs α(2A)-auto-Inhibition of Catecholamine Release in Hypertensive Rats
title_short Angiotensin AT(1) – α(2C)-Adrenoceptor Interaction Disturbs α(2A)-auto-Inhibition of Catecholamine Release in Hypertensive Rats
title_sort angiotensin at(1) – α(2c)-adrenoceptor interaction disturbs α(2a)-auto-inhibition of catecholamine release in hypertensive rats
topic Neuroscience
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3677154/
https://www.ncbi.nlm.nih.gov/pubmed/23772221
http://dx.doi.org/10.3389/fneur.2013.00070
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