| Literature DB >> 33771995 |
Junichi Sugita1, Katsuhito Fujiu2,3,4, Yukiteru Nakayama1, Takumi Matsubara1, Jun Matsuda1, Tsukasa Oshima1, Yuxiang Liu1, Yujin Maru1, Eriko Hasumi1, Toshiya Kojima1, Hiroshi Seno5, Keisuke Asano5, Ayumu Ishijima5, Naoki Tomii5, Masatoshi Yamazaki5, Fujimi Kudo6, Ichiro Sakuma5, Ryozo Nagai7, Ichiro Manabe8, Issei Komuro1.
Abstract
Cardiac arrhythmias are a primary contributor to sudden cardiac death, a major unmet medical need. Because right ventricular (RV) dysfunction increases the risk for sudden cardiac death, we examined responses to RV stress in mice. Among immune cells accumulated in the RV after pressure overload-induced by pulmonary artery banding, interfering with macrophages caused sudden death from severe arrhythmias. We show that cardiac macrophages crucially maintain cardiac impulse conduction by facilitating myocardial intercellular communication through gap junctions. Amphiregulin (AREG) produced by cardiac macrophages is a key mediator that controls connexin 43 phosphorylation and translocation in cardiomyocytes. Deletion of Areg from macrophages led to disorganization of gap junctions and, in turn, lethal arrhythmias during acute stresses, including RV pressure overload and β-adrenergic receptor stimulation. These results suggest that AREG from cardiac resident macrophages is a critical regulator of cardiac impulse conduction and may be a useful therapeutic target for the prevention of sudden death.Entities:
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Year: 2021 PMID: 33771995 DOI: 10.1038/s41467-021-22178-0
Source DB: PubMed Journal: Nat Commun ISSN: 2041-1723 Impact factor: 14.919