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(Pro)renin receptor accelerates development of sarcopenia via activation of Wnt/YAP signaling axis

Wnt信号通路 肌萎缩 生物 骨骼肌 内分泌学 内科学 祖细胞 C2C12型 信号转导 心肌细胞 连环蛋白 丹麦克朗 WNT3A型 转基因小鼠 受体 细胞生物学 转基因 干细胞 医学 肌发生 生物化学 基因
作者
Naohiro Yoshida,Jin Endo,Kenichiro Kinouchi,Hiroki Kitakata,Hidenori Moriyama,Masaharu Kataoka,Tsunehisa Yamamoto,Kohsuke Shirakawa,Satoshi Morimoto,Akira Nishiyama,Akihiro Hashiguchi,Itsuro Higuchi,Keiichi Fukuda,Atsuhiro Ichihara,Motoaki Sano
出处
期刊:Aging Cell [Wiley]
卷期号:18 (5) 被引量:23
标识
DOI:10.1111/acel.12991
摘要

Abstract To extend life expectancy and ensure healthy aging, it is crucial to prevent and minimize age‐induced skeletal muscle atrophy, also known as sarcopenia. However, the disease's molecular mechanism remains unclear. The age‐related Wnt/β‐catenin signaling pathway has been recently shown to be activated by the (pro)renin receptor ((P)RR). We report here that (P)RR expression was increased in the atrophied skeletal muscles of aged mice and humans. Therefore, we developed a gain‐of‐function model of age‐related sarcopenia via transgenic expression of (P)RR under control of the CAG promoter. Consistent with our hypothesis, (P)RR‐Tg mice died early and exhibited muscle atrophy with histological features of sarcopenia. Moreover, Wnt/β‐catenin signaling was activated and the regenerative capacity of muscle progenitor cells after cardiotoxin injury was impaired due to cell fusion failure in (P)RR‐Tg mice. In vitro forced expression of (P)RR protein in C2C12 myoblast cells suppressed myotube formation by activating Wnt/β‐catenin signaling. Administration of Dickkopf‐related protein 1, an inhibitor of Wnt/β‐catenin signaling, and anti‐(P)RR neutralizing antibody, which inhibits binding of (P)RR to the Wnt receptor, significantly improved sarcopenia in (P)RR‐Tg mice. Furthermore, the use of anti‐(P)RR neutralizing antibodies significantly improved the regenerative ability of skeletal muscle in aged mice. Finally, we show that Yes‐associated protein (YAP) signaling, which is coordinately regulated by Wnt/β‐catenin, contributed to the development of (P)RR‐induced sarcopenia. The present study demonstrates the use of (P)RR‐Tg mice as a novel sarcopenia model, and shows that (P)RR‐Wnt‐YAP signaling plays a pivotal role in the pathogenesis of this disease.

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