表观遗传重编程以预防遗传性心肌病。
Epigenetic reprogramming to prevent genetic cardiomyopathy.
出版信息
J Clin Invest. 2021 Jan 4;131(1). doi: 10.1172/JCI143684.
Abstract
Mutations in the gene that codes for lamin A/C (LMNA) are a common cause of adult-onset cardiomyopathy and heart failure. In this issue of the JCI, Guénantin and Jebeniani et al. identify impaired cardiomyocyte development and maturation as a prenatal feature in a model of laminopathy. Cardiomyocytes carrying the Lmna point mutation H222P misexpressed genes involved in the epithelial-mesenchymal transition and showed decreased methylation at the fourth lysine of histone H3 (H3K4). Notably, inhibiting lysine-specific demethylase 1 in the LMNA H222P mouse model treated this congenital form of cardiomyopathy and improved survival in utero. These data highlight early epigenomic modifications in lamin A/C-mediated pathology and indicate a unique therapeutic strategy for cardiomyopathy.
摘要
编码核纤层蛋白 A/C(LMNA)的基因突变是成人发病型心肌病和心力衰竭的常见原因。在本期 JCI 中,Guénantin 和 Jebeniani 等人发现,在 laminopathy 模型中,心肌细胞发育和成熟受损是一种产前特征。携带 Lmna H222P 点突变的心肌细胞异常表达涉及上皮-间充质转化的基因,并显示组蛋白 H3 第四赖氨酸(H3K4)的甲基化减少。值得注意的是,在 LMNA H222P 小鼠模型中抑制赖氨酸特异性去甲基酶 1 可治疗这种先天性心肌病,并改善子宫内的存活率。这些数据突出了核纤层蛋白 A/C 介导的病理中的早期表观遗传修饰,并为心肌病提供了一种独特的治疗策略。
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