Novel insights into the electrophysiology of murine cardiac macrophages: relevance of voltage-gated potassium channels

AIMS: Macrophages (MΦ), known for immunological roles, such as phagocytosis and antigen presentation, have been found to electrotonically couple to cardiomyocytes (CM) of the atrioventricular node via Cx43, affecting cardiac conduction in isolated mouse hearts. Here, we characterize passive and acti...

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Autores principales: Simon-Chica, Ana, Fernández, Marbely C, Wülfers, Eike M, Lother, Achim, Hilgendorf, Ingo, Seemann, Gunnar, Ravens, Ursula, Kohl, Peter, Schneider-Warme, Franziska
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2021
Materias:
Original Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8859634/
https://www.ncbi.nlm.nih.gov/pubmed/33823533
http://dx.doi.org/10.1093/cvr/cvab126
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author Simon-Chica, Ana
Fernández, Marbely C
Wülfers, Eike M
Lother, Achim
Hilgendorf, Ingo
Seemann, Gunnar
Ravens, Ursula
Kohl, Peter
Schneider-Warme, Franziska
author_facet Simon-Chica, Ana
Fernández, Marbely C
Wülfers, Eike M
Lother, Achim
Hilgendorf, Ingo
Seemann, Gunnar
Ravens, Ursula
Kohl, Peter
Schneider-Warme, Franziska
author_sort Simon-Chica, Ana
collection PubMed
description AIMS: Macrophages (MΦ), known for immunological roles, such as phagocytosis and antigen presentation, have been found to electrotonically couple to cardiomyocytes (CM) of the atrioventricular node via Cx43, affecting cardiac conduction in isolated mouse hearts. Here, we characterize passive and active electrophysiological properties of murine cardiac resident MΦ, and model their potential electrophysiological relevance for CM. METHODS AND RESULTS: We combined classic electrophysiological approaches with 3D florescence imaging, RNA-sequencing, pharmacological interventions, and computer simulations. We used Cx(3) [Formula: see text] mice wherein cardiac MΦ are fluorescently labelled. FACS-purified fluorescent MΦ from mouse hearts were studied by whole-cell patch-clamp. MΦ electrophysiological properties include: membrane resistance 2.2±0.1 GΩ (all data mean±SEM), capacitance 18.3±0.1 pF, resting membrane potential −39.6±0.3 mV, and several voltage-activated, outward or inwardly rectifying potassium currents. Using ion channel blockers (barium, TEA, 4-AP, margatoxin, XEN-D0103, and DIDS), flow cytometry, immuno-staining, and RNA-sequencing, we identified Kv1.3, Kv1.5, and Kir2.1 as channels contributing to observed ion currents. MΦ displayed four patterns for outward and two for inward-rectifier potassium currents. Additionally, MΦ showed surface expression of Cx43, a prerequisite for homo- and/or heterotypic electrotonic coupling. Experimental results fed into development of an original computational model to describe cardiac MΦ electrophysiology. Computer simulations to quantitatively assess plausible effects of MΦ on electrotonically coupled CM showed that MΦ can depolarize resting CM, shorten early and prolong late action potential duration, with effects depending on coupling strength and individual MΦ electrophysiological properties, in particular resting membrane potential and presence/absence of Kir2.1. CONCLUSION: Our results provide a first electrophysiological characterization of cardiac resident MΦ, and a computational model to quantitatively explore their relevance in the heterocellular heart. Future work will be focussed at distinguishing electrophysiological effects of MΦ–CM coupling on both cell types during steady-state and in patho-physiological remodelling, when immune cells change their phenotype, proliferate, and/or invade from external sources.
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spelling pubmed-88596342022-02-22 Novel insights into the electrophysiology of murine cardiac macrophages: relevance of voltage-gated potassium channels Simon-Chica, Ana Fernández, Marbely C Wülfers, Eike M Lother, Achim Hilgendorf, Ingo Seemann, Gunnar Ravens, Ursula Kohl, Peter Schneider-Warme, Franziska Cardiovasc Res Original Articles AIMS: Macrophages (MΦ), known for immunological roles, such as phagocytosis and antigen presentation, have been found to electrotonically couple to cardiomyocytes (CM) of the atrioventricular node via Cx43, affecting cardiac conduction in isolated mouse hearts. Here, we characterize passive and active electrophysiological properties of murine cardiac resident MΦ, and model their potential electrophysiological relevance for CM. METHODS AND RESULTS: We combined classic electrophysiological approaches with 3D florescence imaging, RNA-sequencing, pharmacological interventions, and computer simulations. We used Cx(3) [Formula: see text] mice wherein cardiac MΦ are fluorescently labelled. FACS-purified fluorescent MΦ from mouse hearts were studied by whole-cell patch-clamp. MΦ electrophysiological properties include: membrane resistance 2.2±0.1 GΩ (all data mean±SEM), capacitance 18.3±0.1 pF, resting membrane potential −39.6±0.3 mV, and several voltage-activated, outward or inwardly rectifying potassium currents. Using ion channel blockers (barium, TEA, 4-AP, margatoxin, XEN-D0103, and DIDS), flow cytometry, immuno-staining, and RNA-sequencing, we identified Kv1.3, Kv1.5, and Kir2.1 as channels contributing to observed ion currents. MΦ displayed four patterns for outward and two for inward-rectifier potassium currents. Additionally, MΦ showed surface expression of Cx43, a prerequisite for homo- and/or heterotypic electrotonic coupling. Experimental results fed into development of an original computational model to describe cardiac MΦ electrophysiology. Computer simulations to quantitatively assess plausible effects of MΦ on electrotonically coupled CM showed that MΦ can depolarize resting CM, shorten early and prolong late action potential duration, with effects depending on coupling strength and individual MΦ electrophysiological properties, in particular resting membrane potential and presence/absence of Kir2.1. CONCLUSION: Our results provide a first electrophysiological characterization of cardiac resident MΦ, and a computational model to quantitatively explore their relevance in the heterocellular heart. Future work will be focussed at distinguishing electrophysiological effects of MΦ–CM coupling on both cell types during steady-state and in patho-physiological remodelling, when immune cells change their phenotype, proliferate, and/or invade from external sources. Oxford University Press 2021-04-06 /pmc/articles/PMC8859634/ /pubmed/33823533 http://dx.doi.org/10.1093/cvr/cvab126 Text en © The Author(s) 2021. Published by Oxford University Press on behalf of the European Society of Cardiology. https://creativecommons.org/licenses/by-nc/4.0/This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License (https://creativecommons.org/licenses/by-nc/4.0/), which permits non-commercial re-use, distribution, and reproduction in any medium, provided the original work is properly cited. For commercial re-use, please contact journals.permissions@oup.com
spellingShingle Original Articles
Simon-Chica, Ana
Fernández, Marbely C
Wülfers, Eike M
Lother, Achim
Hilgendorf, Ingo
Seemann, Gunnar
Ravens, Ursula
Kohl, Peter
Schneider-Warme, Franziska
Novel insights into the electrophysiology of murine cardiac macrophages: relevance of voltage-gated potassium channels
title Novel insights into the electrophysiology of murine cardiac macrophages: relevance of voltage-gated potassium channels
title_full Novel insights into the electrophysiology of murine cardiac macrophages: relevance of voltage-gated potassium channels
title_fullStr Novel insights into the electrophysiology of murine cardiac macrophages: relevance of voltage-gated potassium channels
title_full_unstemmed Novel insights into the electrophysiology of murine cardiac macrophages: relevance of voltage-gated potassium channels
title_short Novel insights into the electrophysiology of murine cardiac macrophages: relevance of voltage-gated potassium channels
title_sort novel insights into the electrophysiology of murine cardiac macrophages: relevance of voltage-gated potassium channels
topic Original Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8859634/
https://www.ncbi.nlm.nih.gov/pubmed/33823533
http://dx.doi.org/10.1093/cvr/cvab126
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