Functional effects of KCNQ K(+) channels in airway smooth muscle

KCNQ (K(v)7) channels underlie a voltage-gated K(+) current best known for control of neuronal excitability, and its inhibition by G(q/11)-coupled, muscarinic signaling. Studies have indicated expression of KCNQ channels in airway smooth muscle (ASM), a tissue that is predominantly regulated by musc...

Descripción completa

Detalles Bibliográficos
Autores principales: Evseev, Alexey I., Semenov, Iurii, Archer, Crystal R., Medina, Jorge L., Dube, Peter H., Shapiro, Mark S., Brenner, Robert
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2013
Materias:
Physiology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3791379/
https://www.ncbi.nlm.nih.gov/pubmed/24109455
http://dx.doi.org/10.3389/fphys.2013.00277
_version_ 1782286709045592064
author Evseev, Alexey I.
Semenov, Iurii
Archer, Crystal R.
Medina, Jorge L.
Dube, Peter H.
Shapiro, Mark S.
Brenner, Robert
author_facet Evseev, Alexey I.
Semenov, Iurii
Archer, Crystal R.
Medina, Jorge L.
Dube, Peter H.
Shapiro, Mark S.
Brenner, Robert
author_sort Evseev, Alexey I.
collection PubMed
description KCNQ (K(v)7) channels underlie a voltage-gated K(+) current best known for control of neuronal excitability, and its inhibition by G(q/11)-coupled, muscarinic signaling. Studies have indicated expression of KCNQ channels in airway smooth muscle (ASM), a tissue that is predominantly regulated by muscarinic receptor signaling. Therefore, we investigated the function of KCNQ channels in rodent ASM and their interplay with G(q/11)-coupled M(3) muscarinic receptors. Perforated-patch clamp of dissociated ASM cells detected a K(+) current inhibited by the KCNQ antagonist, XE991, and augmented by the specific agonist, flupirtine. KCNQ channels begin to activate at voltages near resting potentials for ASM cells, and indeed XE991 depolarized resting membrane potentials. Muscarinic receptor activation inhibited KCNQ current weakly (~20%) at concentrations half-maximal for contractions. Thus, we were surprised to see that KCNQ had no affect on membrane voltage or muscle contractility following muscarinic activation. Further, M(3) receptor-specific antagonist J104129 fumarate alone did not reveal KCNQ effects on muscarinic evoked depolarization or contractility. However, a role for KCNQ channels was revealed when BK-K(+) channel activities are reduced. While KCNQ channels do control resting potentials, they appear to play a redundant role with BK calcium-activated K(+) channels during ASM muscarinic signaling. In contrast to effect of antagonist, we observe that KCNQ agonist flupirtine caused a significant hyperpolarization and reduced contraction in vitro irrespective of muscarinic activation. Using non-invasive whole animal plethysmography, the clinically approved KCNQ agonist retigabine caused a transient reduction in indexes of airway resistance in both wild type and BK β1 knockout (KO) mice treated with the muscarinic agonist. These findings indicate that KCNQ channels can be recruited via agonists to oppose muscarinic evoked contractions and may be of therapeutic value as bronchodilators.
format Online
Article
Text
id pubmed-3791379
institution National Center for Biotechnology Information
language English
publishDate 2013
publisher Frontiers Media S.A.
record_format MEDLINE/PubMed
spelling pubmed-37913792013-10-09 Functional effects of KCNQ K(+) channels in airway smooth muscle Evseev, Alexey I. Semenov, Iurii Archer, Crystal R. Medina, Jorge L. Dube, Peter H. Shapiro, Mark S. Brenner, Robert Front Physiol Physiology KCNQ (K(v)7) channels underlie a voltage-gated K(+) current best known for control of neuronal excitability, and its inhibition by G(q/11)-coupled, muscarinic signaling. Studies have indicated expression of KCNQ channels in airway smooth muscle (ASM), a tissue that is predominantly regulated by muscarinic receptor signaling. Therefore, we investigated the function of KCNQ channels in rodent ASM and their interplay with G(q/11)-coupled M(3) muscarinic receptors. Perforated-patch clamp of dissociated ASM cells detected a K(+) current inhibited by the KCNQ antagonist, XE991, and augmented by the specific agonist, flupirtine. KCNQ channels begin to activate at voltages near resting potentials for ASM cells, and indeed XE991 depolarized resting membrane potentials. Muscarinic receptor activation inhibited KCNQ current weakly (~20%) at concentrations half-maximal for contractions. Thus, we were surprised to see that KCNQ had no affect on membrane voltage or muscle contractility following muscarinic activation. Further, M(3) receptor-specific antagonist J104129 fumarate alone did not reveal KCNQ effects on muscarinic evoked depolarization or contractility. However, a role for KCNQ channels was revealed when BK-K(+) channel activities are reduced. While KCNQ channels do control resting potentials, they appear to play a redundant role with BK calcium-activated K(+) channels during ASM muscarinic signaling. In contrast to effect of antagonist, we observe that KCNQ agonist flupirtine caused a significant hyperpolarization and reduced contraction in vitro irrespective of muscarinic activation. Using non-invasive whole animal plethysmography, the clinically approved KCNQ agonist retigabine caused a transient reduction in indexes of airway resistance in both wild type and BK β1 knockout (KO) mice treated with the muscarinic agonist. These findings indicate that KCNQ channels can be recruited via agonists to oppose muscarinic evoked contractions and may be of therapeutic value as bronchodilators. Frontiers Media S.A. 2013-10-07 /pmc/articles/PMC3791379/ /pubmed/24109455 http://dx.doi.org/10.3389/fphys.2013.00277 Text en Copyright © 2013 Evseev, Semenov, Archer, Medina, Dube, Shapiro and Brenner. http://creativecommons.org/licenses/by/3.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) or licensor are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Physiology
Evseev, Alexey I.
Semenov, Iurii
Archer, Crystal R.
Medina, Jorge L.
Dube, Peter H.
Shapiro, Mark S.
Brenner, Robert
Functional effects of KCNQ K(+) channels in airway smooth muscle
title Functional effects of KCNQ K(+) channels in airway smooth muscle
title_full Functional effects of KCNQ K(+) channels in airway smooth muscle
title_fullStr Functional effects of KCNQ K(+) channels in airway smooth muscle
title_full_unstemmed Functional effects of KCNQ K(+) channels in airway smooth muscle
title_short Functional effects of KCNQ K(+) channels in airway smooth muscle
title_sort functional effects of kcnq k(+) channels in airway smooth muscle
topic Physiology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3791379/
https://www.ncbi.nlm.nih.gov/pubmed/24109455
http://dx.doi.org/10.3389/fphys.2013.00277
work_keys_str_mv AT evseevalexeyi functionaleffectsofkcnqkchannelsinairwaysmoothmuscle
AT semenoviurii functionaleffectsofkcnqkchannelsinairwaysmoothmuscle
AT archercrystalr functionaleffectsofkcnqkchannelsinairwaysmoothmuscle
AT medinajorgel functionaleffectsofkcnqkchannelsinairwaysmoothmuscle
AT dubepeterh functionaleffectsofkcnqkchannelsinairwaysmoothmuscle
AT shapiromarks functionaleffectsofkcnqkchannelsinairwaysmoothmuscle
AT brennerrobert functionaleffectsofkcnqkchannelsinairwaysmoothmuscle

Ejemplares similares