MacRae Calum A, Birchmeier Walter, Thierfelder Ludwig
Cardiovascular Research Center, Massachusetts General Hospital and Harvard Medical School, Boston, Massachusetts, USA.
J Clin Invest. 2006 Jul;116(7):1825-8. doi: 10.1172/JCI29174.
Mutations in genes encoding desmosomal proteins have been identified as the major cause of arrhythmogenic right ventricular dysplasia/cardiomyopathy (ARVC), in which the right ventricle is "replaced" by fibrofatty tissue, resulting in lethal arrhythmias. In this issue of the JCI, Garcia-Gras et al. demonstrate that cardiac-specific loss of the desmosomal protein desmoplakin is sufficient to cause nuclear translocation of plakoglobin, upregulation of adipogenic genes in vitro, and a shift from a cardiomyocyte to an adipocyte cell fate in vivo (see the related article beginning on page 2012). This evidence for potential Wnt/beta-catenin signaling defects sets the scene for a comprehensive exploration of the contributions of this pathway to the pathophysiology of ARVC, not only through perturbation of cardiac patterning and development, but also through effects on myocardial differentiation and physiology.
编码桥粒蛋白的基因突变已被确认为致心律失常性右室发育不良/心肌病(ARVC)的主要病因,在这种疾病中,右心室被纤维脂肪组织“取代”,从而导致致命性心律失常。在本期《临床研究杂志》中,加西亚 - 格拉斯等人证明,桥粒蛋白桥粒斑蛋白在心脏中的特异性缺失足以导致 plakoglobin 的核转位、体外脂肪生成基因的上调以及体内心肌细胞向脂肪细胞命运的转变(见第 2012 页开始的相关文章)。这种潜在的 Wnt/β-连环蛋白信号缺陷的证据为全面探索该信号通路对 ARVC 病理生理学的贡献奠定了基础,这不仅是通过干扰心脏的模式形成和发育,还通过对心肌分化和生理的影响来实现的。
