Kir2.1-Nav1.5 Channel Complexes Are Differently Regulated than Kir2.1 and Nav1.5 Channels Alone

Cardiac Kir2.1 and Nav1.5 channels generate the inward rectifier K(+) (I(K1)) and the Na(+) (I(Na)) currents, respectively. There is a mutual interplay between the ventricular I(Na) and I(K1) densities, because Nav1.5 and Kir2.1 channels exhibit positive reciprocal modulation. Here we compared some...

Descripción completa

Detalles Bibliográficos
Autores principales: Utrilla, Raquel G., Nieto-Marín, Paloma, Alfayate, Silvia, Tinaquero, David, Matamoros, Marcos, Pérez-Hernández, Marta, Sacristán, Sandra, Ondo, Lorena, de Andrés, Raquel, Díez-Guerra, F. Javier, Tamargo, Juan, Delpón, Eva, Caballero, Ricardo
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2017
Materias:
Physiology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5694551/
https://www.ncbi.nlm.nih.gov/pubmed/29184507
http://dx.doi.org/10.3389/fphys.2017.00903
_version_ 1783280157117644800
author Utrilla, Raquel G.
Nieto-Marín, Paloma
Alfayate, Silvia
Tinaquero, David
Matamoros, Marcos
Pérez-Hernández, Marta
Sacristán, Sandra
Ondo, Lorena
de Andrés, Raquel
Díez-Guerra, F. Javier
Tamargo, Juan
Delpón, Eva
Caballero, Ricardo
author_facet Utrilla, Raquel G.
Nieto-Marín, Paloma
Alfayate, Silvia
Tinaquero, David
Matamoros, Marcos
Pérez-Hernández, Marta
Sacristán, Sandra
Ondo, Lorena
de Andrés, Raquel
Díez-Guerra, F. Javier
Tamargo, Juan
Delpón, Eva
Caballero, Ricardo
author_sort Utrilla, Raquel G.
collection PubMed
description Cardiac Kir2.1 and Nav1.5 channels generate the inward rectifier K(+) (I(K1)) and the Na(+) (I(Na)) currents, respectively. There is a mutual interplay between the ventricular I(Na) and I(K1) densities, because Nav1.5 and Kir2.1 channels exhibit positive reciprocal modulation. Here we compared some of the biological properties of Nav1.5 and Kir2.1 channels when they are expressed together or separately to get further insights regarding their putative interaction. First we demonstrated by proximity ligation assays (PLAs) that in the membrane of ventricular myocytes Nav1.5 and Kir2.1 proteins are in close proximity to each other (<40 nm apart). Furthermore, intracellular dialysis with anti-Nav1.5 and anti-Kir2.1 antibodies suggested that these channels form complexes. Patch-clamp experiments in heterologous transfection systems demonstrated that the inhibition of the Ca(2+)/calmodulin-dependent protein kinase II (CaMKII) decreased the I(Na) and the I(K1) generated by Nav1.5 and Kir2.1 channels when they were coexpressed, but not the I(K1) generated by Kir2.1 channels alone, suggesting that complexes, but not Kir2.1 channels, are a substrate of CaMKII. Furthermore, inhibition of CaMKII precluded the interaction between Nav1.5 and Kir2.1 channels. Inhibition of 14-3-3 proteins did not modify the I(Na) and I(K1) densities generated by each channel separately, whereas it decreased the I(Na) and I(K1) generated when they were coexpressed. However, inhibition of 14-3-3 proteins did not abolish the Nav1.5-Kir2.1 interaction. Inhibition of dynamin-dependent endocytosis reduced the internalization of Kir2.1 but not of Nav1.5 or Kir2.1-Nav1.5 complexes. Inhibition of cytoskeleton-dependent vesicular trafficking via the dynein/dynactin motor increased the I(K1), but reduced the I(Na), thus suggesting that the dynein/dynactin motor is preferentially involved in the backward and forward traffic of Kir2.1 and Nav1.5, respectively. Conversely, the dynein/dynactin motor participated in the forward movement of Kir2.1-Nav1.5 complexes. Ubiquitination by Nedd4-2 ubiquitin-protein ligase promoted the Nav1.5 degradation by the proteasome, but not that of Kir2.1 channels. Importantly, the Kir2.1-Nav1.5 complexes were degraded following this route as demonstrated by the overexpression of Nedd4-2 and the inhibition of the proteasome with MG132. These results suggested that Kir2.1 and Nav1.5 channels closely interact with each other leading to the formation of a pool of complexed channels whose biology is similar to that of the Nav1.5 channels.
format Online
Article
Text
id pubmed-5694551
institution National Center for Biotechnology Information
language English
publishDate 2017
publisher Frontiers Media S.A.
record_format MEDLINE/PubMed
spelling pubmed-56945512017-11-28 Kir2.1-Nav1.5 Channel Complexes Are Differently Regulated than Kir2.1 and Nav1.5 Channels Alone Utrilla, Raquel G. Nieto-Marín, Paloma Alfayate, Silvia Tinaquero, David Matamoros, Marcos Pérez-Hernández, Marta Sacristán, Sandra Ondo, Lorena de Andrés, Raquel Díez-Guerra, F. Javier Tamargo, Juan Delpón, Eva Caballero, Ricardo Front Physiol Physiology Cardiac Kir2.1 and Nav1.5 channels generate the inward rectifier K(+) (I(K1)) and the Na(+) (I(Na)) currents, respectively. There is a mutual interplay between the ventricular I(Na) and I(K1) densities, because Nav1.5 and Kir2.1 channels exhibit positive reciprocal modulation. Here we compared some of the biological properties of Nav1.5 and Kir2.1 channels when they are expressed together or separately to get further insights regarding their putative interaction. First we demonstrated by proximity ligation assays (PLAs) that in the membrane of ventricular myocytes Nav1.5 and Kir2.1 proteins are in close proximity to each other (<40 nm apart). Furthermore, intracellular dialysis with anti-Nav1.5 and anti-Kir2.1 antibodies suggested that these channels form complexes. Patch-clamp experiments in heterologous transfection systems demonstrated that the inhibition of the Ca(2+)/calmodulin-dependent protein kinase II (CaMKII) decreased the I(Na) and the I(K1) generated by Nav1.5 and Kir2.1 channels when they were coexpressed, but not the I(K1) generated by Kir2.1 channels alone, suggesting that complexes, but not Kir2.1 channels, are a substrate of CaMKII. Furthermore, inhibition of CaMKII precluded the interaction between Nav1.5 and Kir2.1 channels. Inhibition of 14-3-3 proteins did not modify the I(Na) and I(K1) densities generated by each channel separately, whereas it decreased the I(Na) and I(K1) generated when they were coexpressed. However, inhibition of 14-3-3 proteins did not abolish the Nav1.5-Kir2.1 interaction. Inhibition of dynamin-dependent endocytosis reduced the internalization of Kir2.1 but not of Nav1.5 or Kir2.1-Nav1.5 complexes. Inhibition of cytoskeleton-dependent vesicular trafficking via the dynein/dynactin motor increased the I(K1), but reduced the I(Na), thus suggesting that the dynein/dynactin motor is preferentially involved in the backward and forward traffic of Kir2.1 and Nav1.5, respectively. Conversely, the dynein/dynactin motor participated in the forward movement of Kir2.1-Nav1.5 complexes. Ubiquitination by Nedd4-2 ubiquitin-protein ligase promoted the Nav1.5 degradation by the proteasome, but not that of Kir2.1 channels. Importantly, the Kir2.1-Nav1.5 complexes were degraded following this route as demonstrated by the overexpression of Nedd4-2 and the inhibition of the proteasome with MG132. These results suggested that Kir2.1 and Nav1.5 channels closely interact with each other leading to the formation of a pool of complexed channels whose biology is similar to that of the Nav1.5 channels. Frontiers Media S.A. 2017-11-14 /pmc/articles/PMC5694551/ /pubmed/29184507 http://dx.doi.org/10.3389/fphys.2017.00903 Text en Copyright © 2017 Utrilla, Nieto-Marín, Alfayate, Tinaquero, Matamoros, Pérez-Hernández, Sacristán, Ondo, de Andrés, Díez-Guerra, Tamargo, Delpón and Caballero. http://creativecommons.org/licenses/by/4.0/ 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
Utrilla, Raquel G.
Nieto-Marín, Paloma
Alfayate, Silvia
Tinaquero, David
Matamoros, Marcos
Pérez-Hernández, Marta
Sacristán, Sandra
Ondo, Lorena
de Andrés, Raquel
Díez-Guerra, F. Javier
Tamargo, Juan
Delpón, Eva
Caballero, Ricardo
Kir2.1-Nav1.5 Channel Complexes Are Differently Regulated than Kir2.1 and Nav1.5 Channels Alone
title Kir2.1-Nav1.5 Channel Complexes Are Differently Regulated than Kir2.1 and Nav1.5 Channels Alone
title_full Kir2.1-Nav1.5 Channel Complexes Are Differently Regulated than Kir2.1 and Nav1.5 Channels Alone
title_fullStr Kir2.1-Nav1.5 Channel Complexes Are Differently Regulated than Kir2.1 and Nav1.5 Channels Alone
title_full_unstemmed Kir2.1-Nav1.5 Channel Complexes Are Differently Regulated than Kir2.1 and Nav1.5 Channels Alone
title_short Kir2.1-Nav1.5 Channel Complexes Are Differently Regulated than Kir2.1 and Nav1.5 Channels Alone
title_sort kir2.1-nav1.5 channel complexes are differently regulated than kir2.1 and nav1.5 channels alone
topic Physiology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5694551/
https://www.ncbi.nlm.nih.gov/pubmed/29184507
http://dx.doi.org/10.3389/fphys.2017.00903
work_keys_str_mv AT utrillaraquelg kir21nav15channelcomplexesaredifferentlyregulatedthankir21andnav15channelsalone
AT nietomarinpaloma kir21nav15channelcomplexesaredifferentlyregulatedthankir21andnav15channelsalone
AT alfayatesilvia kir21nav15channelcomplexesaredifferentlyregulatedthankir21andnav15channelsalone
AT tinaquerodavid kir21nav15channelcomplexesaredifferentlyregulatedthankir21andnav15channelsalone
AT matamorosmarcos kir21nav15channelcomplexesaredifferentlyregulatedthankir21andnav15channelsalone
AT perezhernandezmarta kir21nav15channelcomplexesaredifferentlyregulatedthankir21andnav15channelsalone
AT sacristansandra kir21nav15channelcomplexesaredifferentlyregulatedthankir21andnav15channelsalone
AT ondolorena kir21nav15channelcomplexesaredifferentlyregulatedthankir21andnav15channelsalone
AT deandresraquel kir21nav15channelcomplexesaredifferentlyregulatedthankir21andnav15channelsalone
AT diezguerrafjavier kir21nav15channelcomplexesaredifferentlyregulatedthankir21andnav15channelsalone
AT tamargojuan kir21nav15channelcomplexesaredifferentlyregulatedthankir21andnav15channelsalone
AT delponeva kir21nav15channelcomplexesaredifferentlyregulatedthankir21andnav15channelsalone
AT caballeroricardo kir21nav15channelcomplexesaredifferentlyregulatedthankir21andnav15channelsalone

Ejemplares similares