CDC-like kinase 4 deficiency contributes to pathological cardiac hypertrophy by modulating NEXN phosphorylation.
Jian HuangLuxin WangYunli ShenShengqi ZhangYaqun ZhouJimin DuXiue MaYi LiuDandan LiangDan ShiHonghui MaLi LiQi ZhangYi-Han ChenPublished in: Nature communications (2022)
Kinase-catalyzed phosphorylation plays a crucial role in pathological cardiac hypertrophy. Here, we show that CDC-like kinase 4 (CLK4) is a critical regulator of cardiomyocyte hypertrophy and heart failure. Knockdown of Clk4 leads to pathological cardiomyocyte hypertrophy, while overexpression of Clk4 confers resistance to phenylephrine-induced cardiomyocyte hypertrophy. Cardiac-specific Clk4-knockout mice manifest pathological myocardial hypertrophy with progressive left ventricular systolic dysfunction and heart dilation. Further investigation identifies nexilin (NEXN) as the direct substrate of CLK4, and overexpression of a phosphorylation-mimic mutant of NEXN is sufficient to reverse the hypertrophic growth of cardiomyocytes induced by Clk4 knockdown. Importantly, restoring phosphorylation of NEXN ameliorates myocardial hypertrophy in mice with cardiac-specific Clk4 deletion. We conclude that CLK4 regulates cardiac function through phosphorylation of NEXN, and its deficiency may lead to pathological cardiac hypertrophy. CLK4 is a potential intervention target for the prevention and treatment of heart failure.
Keyphrases
- left ventricular
- heart failure
- protein kinase
- high glucose
- cardiac resynchronization therapy
- hypertrophic cardiomyopathy
- acute myocardial infarction
- randomized controlled trial
- mitral valve
- angiotensin ii
- cell proliferation
- transcription factor
- left atrial
- multiple sclerosis
- aortic stenosis
- type diabetes
- adipose tissue
- blood pressure
- genome wide
- cell cycle
- tyrosine kinase
- oxidative stress
- skeletal muscle
- signaling pathway
- dna methylation
- coronary artery disease
- room temperature
- insulin resistance
- stress induced