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A New Perspective on Intercalated Disc Organization: Implications for Heart Disease

机译:插片组织的新观点:对心脏病的影响

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Adherens junctions and desmosomes are intercellular adhesive junctions and essential for the morphogenesis, differentiation, and maintenance of tissues that are subjected to high mechanical stress, including heart and skin. The different junction complexes are organized at the termini of the cardiomyocyte called the intercalated disc. Disruption of adhesive integrity via mutations in genes encoding desmosomal proteins causes an inherited heart disease, arrhythmogenic right ventricular cardiomyopathy (ARVC). Besides plakoglobin, which is shared by adherens junctions and desmosomes, other desmosomal components, desmoglein-2, desmocollin-2, plakophilin-2, and desmoplakin are also present in ultrastructurally defined fascia adherens junctions of heart muscle, but not other tissues. This mixed-type of junctional structure is termed hybrid adhering junction or area composita. Desmosomal plakophilin-2 directly interacts with adherens junction protein alphaT-catenin, providing a new molecular link between the cadherin-catenin complex and desmosome. The area composita only exists in the cardiac intercalated disc of mammalian species suggesting that it evolved to strengthen mechanical coupling in the heart of higher vertebrates. The cross-talk among different junctions and their implication in the pathogenesis of ARVC are discussed in this review.
机译:粘附连接和桥粒是细胞间的粘附连接,对于经受高机械应力(包括心脏和皮肤)的组织的形态发生,分化和维持至关重要。不同的连接复合物组织在称为插入盘的心肌细胞末端。通过编码桥粒蛋白的基因中的突变破坏粘附完整性会导致遗传性心脏病,即心律失常性右室心肌病(ARVC)。除了粘附连接和桥粒共享的珠光蛋白外,其他超链体成分,desmoglein-2,desmocollin-2,plakophilin-2和desmoplakin也存在于超微结构定义的筋膜粘附心肌的连接处,但不存在于其他组织。这种混合类型的接合结构被称为混合粘附接合或区域复合材料。 Desmosomal plakophilin-2与粘附连接蛋白αT-catenin直接相互作用,从而在钙粘蛋白-catenin复合物和桥粒之间提供了新的分子连接。复合材料区域仅存在于哺乳动物物种的心脏插层盘中,这表明它已进化为增强高等脊椎动物心脏中的机械耦合。本文综述了不同连接点之间的串扰及其在ARVC发病机理中的意义。

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