泛素连接酶
泛素
病态的
下调和上调
心力衰竭
心肌肥大
医学
肌肉肥大
内科学
基因敲除
血管紧张素II
磷酸化
心脏病学
内分泌学
基因剔除小鼠
收缩
心室重构
泛素蛋白连接酶类
肾素-血管紧张素系统
癌症研究
激酶
心肌细胞
作者
Risheng Zhao,Xiaoli Cui,Huizhu Du,Zhuoqun Wang,Chang Liu,Linxin Zhang,Jianing Qi,Di Yang,Hui Yu,Shuang Yan,Wei Liu,Haiming Sun,Mengyang Wang
标识
DOI:10.1002/advs.202521337
摘要
Pathological cardiac hypertrophy is a major predisposing factor for heart failure (HF). This study investigates the role of the E3 ubiquitin ligase Tripartite Motif-Containing 40 (TRIM40) in cardiac hypertrophy. Using TRIM40 knockout (TRIM40-/-), cardiac-specific knockdown and overexpressing mice, pathological hypertrophy was induced by angiotensin II (Ang II) infusion or transverse aortic constriction (TAC). Results showed that TRIM40 expression was upregulated in hypertrophic hearts. TRIM40 deficiency attenuated cardiac hypertrophy and dysfunction, whereas its overexpression exacerbated pathological remodeling. Mechanistically, TRIM40 binds PKN2 via its B-box domain and, in a manner requiring its C29-dependent E3 ligase activity, promotes K63-linked ubiquitination of PKN2. This leads to enhanced PKN2 phosphorylation at Ser815 and activation of downstream signaling. Pharmacological inhibition of PKN2 attenuated cardiac remodeling induced by TRIM40 overexpression. These findings reveal that TRIM40 drives cardiac hypertrophy through K63-linked ubiquitination and activation of PKN2, identifying TRIM40 as a promising candidate for therapeutic intervention in HF.
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