心室
心力衰竭
补体系统
医学
心脏病学
替代补体途径
内科学
免疫学
免疫系统
作者
Shogo Ito,Hisayuki Hashimoto,Hiroyuki Yamakawa,Dai Kusumoto,Yohei Akiba,Takahiro Nakamura,Mizuki Momoi,Jin Komuro,Toshiomi Katsuki,Mai Kimura,Yoshikazu Kishino,Shin Kashimura,Akira Kunitomi,Mark Lachmann,Masaya Shimojima,Gakuto Yozu,Chikaaki Motoda,Tomohisa Seki,Tsunehisa Yamamoto,Yoshiki Shinya
标识
DOI:10.1038/s41467-022-33152-9
摘要
Failure of the right ventricle plays a critical role in any type of heart failure. However, the mechanism remains unclear, and there is no specific therapy. Here, we show that the right ventricle predominantly expresses alternative complement pathway-related genes, including Cfd and C3aR1. Complement 3 (C3)-knockout attenuates right ventricular dysfunction and fibrosis in a mouse model of right ventricular failure. C3a is produced from C3 by the C3 convertase complex, which includes the essential component complement factor D (Cfd). Cfd-knockout mice also show attenuation of right ventricular failure. Moreover, the plasma concentration of CFD correlates with the severity of right ventricular failure in patients with chronic right ventricular failure. A C3a receptor (C3aR) antagonist dramatically improves right ventricular dysfunction in mice. In summary, we demonstrate the crucial role of the C3-Cfd-C3aR axis in right ventricular failure and highlight potential therapeutic targets for right ventricular failure.
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