Cardiac resident macrophages: the emerging role in arrhythmogenesis
Jiaqian Zhao, Jun Liu, Ying Zou, Jianhong Li, Ming Lei, Xiaoqiu Tan, Tangting Chen

TL;DR
This paper reviews how heart-resident macrophages contribute to heart rhythm disorders and highlights their unique role compared to other immune cells.
Contribution
The paper introduces cardiac resident macrophages as a novel player in arrhythmogenesis through direct electrophysiological interactions.
Findings
Cardiac resident macrophages (CRMs) differ from bone marrow-derived macrophages in origin and function.
CRMs modulate heart rhythm via ion channels and gap junctions, contributing to arrhythmias.
Advanced techniques reveal complex interactions between CRMs and cardiomyocytes in arrhythmia mechanisms.
Abstract
Arrhythmia is a prevalent complication associated with various cardiovascular diseases. The onset of cardiac disease or injury can impair the normal function of cardiomyocytes, thereby precipitating arrhythmic events. Moreover, non-cardiomyocytes, including immune cells, may also play a contributory role in arrhythmogenesis. For instance, processes such as the infiltration of inflammatory cells that secrete pro-inflammatory mediators, fibroblast-to-myofibroblast transformation, and endothelial-to-mesenchymal transition have all been implicated in this process. Recent investigations have identified a distinct subset of resident macrophages within cardiac tissue that exhibit functional properties differing from those of bone marrow-derived macrophages. Cardiac tissue-resident macrophages (CRMs) are distinguished from bone marrow-derived macrophages by their developmental origin,…
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Taxonomy
TopicsCardiac electrophysiology and arrhythmias · Cardiac Fibrosis and Remodeling · Atrial Fibrillation Management and Outcomes
