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VPAC1 receptors play a dominant role in PACAP-induced vasorelaxation in female mice

BACKGROUND: PACAP and VIP are closely related neuropeptides with wide distribution and potent effect in the vasculature. We previously reported vasomotor activity in peripheral vasculature of male wild type (WT) and PACAP-deficient (KO) mice. However, female vascular responses are still unexplored....

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Autores principales: Ivic, Ivan, Balasko, Marta, Fulop, Balazs D., Hashimoto, Hitoshi, Toth, Gabor, Tamas, Andrea, Juhasz, Tamas, Koller, Akos, Reglodi, Dora, Solymár, Margit
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2019
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6347420/
https://www.ncbi.nlm.nih.gov/pubmed/30682157
http://dx.doi.org/10.1371/journal.pone.0211433
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author Ivic, Ivan
Balasko, Marta
Fulop, Balazs D.
Hashimoto, Hitoshi
Toth, Gabor
Tamas, Andrea
Juhasz, Tamas
Koller, Akos
Reglodi, Dora
Solymár, Margit
author_facet Ivic, Ivan
Balasko, Marta
Fulop, Balazs D.
Hashimoto, Hitoshi
Toth, Gabor
Tamas, Andrea
Juhasz, Tamas
Koller, Akos
Reglodi, Dora
Solymár, Margit
author_sort Ivic, Ivan
collection PubMed
description BACKGROUND: PACAP and VIP are closely related neuropeptides with wide distribution and potent effect in the vasculature. We previously reported vasomotor activity in peripheral vasculature of male wild type (WT) and PACAP-deficient (KO) mice. However, female vascular responses are still unexplored. We hypothesized that PACAP-like activity is maintained in female PACAP KO mice and the mechanism through which it is regulated differs from that of male PACAP KO animals. METHODS: We investigated the vasomotor effects of VIP and PACAP isoforms and their selective blockers in WT and PACAP KO female mice in carotid and femoral arteries. The expression and level of different PACAP receptors in the vessels were measured by RT-PCR and Western blot. RESULTS: In both carotid and femoral arteries of WT mice, PACAP1-38, PACAP1-27 or VIP induced relaxation, without pronounced differences between them. Reduced relaxation was recorded only in the carotid arteries of KO mice as compared to their WT controls. The specific VPAC1R antagonist completely blocked the PACAP/VIP-induced relaxation in both arteries of all mice, while PAC1R antagonist affected relaxation only in their femoral arteries. CONCLUSION: In female WT mice, VPAC1 receptors appear to play a dominant role in PACAP-induced vasorelaxation both in carotid and in femoral arteries. In the PACAP KO group PAC1R activation exerts vasorelaxation in the femoral arteries but in carotid arteries there is no significant effect of the activation of this receptor. In the background of this regional difference, decreased PAC1R and increased VPAC1R availability in the carotid arteries was found.
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spelling pubmed-63474202019-02-15 VPAC1 receptors play a dominant role in PACAP-induced vasorelaxation in female mice Ivic, Ivan Balasko, Marta Fulop, Balazs D. Hashimoto, Hitoshi Toth, Gabor Tamas, Andrea Juhasz, Tamas Koller, Akos Reglodi, Dora Solymár, Margit PLoS One Research Article BACKGROUND: PACAP and VIP are closely related neuropeptides with wide distribution and potent effect in the vasculature. We previously reported vasomotor activity in peripheral vasculature of male wild type (WT) and PACAP-deficient (KO) mice. However, female vascular responses are still unexplored. We hypothesized that PACAP-like activity is maintained in female PACAP KO mice and the mechanism through which it is regulated differs from that of male PACAP KO animals. METHODS: We investigated the vasomotor effects of VIP and PACAP isoforms and their selective blockers in WT and PACAP KO female mice in carotid and femoral arteries. The expression and level of different PACAP receptors in the vessels were measured by RT-PCR and Western blot. RESULTS: In both carotid and femoral arteries of WT mice, PACAP1-38, PACAP1-27 or VIP induced relaxation, without pronounced differences between them. Reduced relaxation was recorded only in the carotid arteries of KO mice as compared to their WT controls. The specific VPAC1R antagonist completely blocked the PACAP/VIP-induced relaxation in both arteries of all mice, while PAC1R antagonist affected relaxation only in their femoral arteries. CONCLUSION: In female WT mice, VPAC1 receptors appear to play a dominant role in PACAP-induced vasorelaxation both in carotid and in femoral arteries. In the PACAP KO group PAC1R activation exerts vasorelaxation in the femoral arteries but in carotid arteries there is no significant effect of the activation of this receptor. In the background of this regional difference, decreased PAC1R and increased VPAC1R availability in the carotid arteries was found. Public Library of Science 2019-01-25 /pmc/articles/PMC6347420/ /pubmed/30682157 http://dx.doi.org/10.1371/journal.pone.0211433 Text en © 2019 Ivic et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Ivic, Ivan
Balasko, Marta
Fulop, Balazs D.
Hashimoto, Hitoshi
Toth, Gabor
Tamas, Andrea
Juhasz, Tamas
Koller, Akos
Reglodi, Dora
Solymár, Margit
VPAC1 receptors play a dominant role in PACAP-induced vasorelaxation in female mice
title VPAC1 receptors play a dominant role in PACAP-induced vasorelaxation in female mice
title_full VPAC1 receptors play a dominant role in PACAP-induced vasorelaxation in female mice
title_fullStr VPAC1 receptors play a dominant role in PACAP-induced vasorelaxation in female mice
title_full_unstemmed VPAC1 receptors play a dominant role in PACAP-induced vasorelaxation in female mice
title_short VPAC1 receptors play a dominant role in PACAP-induced vasorelaxation in female mice
title_sort vpac1 receptors play a dominant role in pacap-induced vasorelaxation in female mice
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6347420/
https://www.ncbi.nlm.nih.gov/pubmed/30682157
http://dx.doi.org/10.1371/journal.pone.0211433
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