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首页> 外文期刊>European Journal of Cell Biology: Journal of Deutsche Gesellschaft fur Elektronenmikroskopie: Journal of Deutsche Gesellschaft fur Zellbiologie >The area composita of adhering junctions connecting heart muscle cells of vertebrates. V. The importance of plakophilin-2 demonstrated by small interference RNA-mediated knockdown in cultured rat cardiomyocytes.
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The area composita of adhering junctions connecting heart muscle cells of vertebrates. V. The importance of plakophilin-2 demonstrated by small interference RNA-mediated knockdown in cultured rat cardiomyocytes.

机译:连接脊椎动物的心肌细胞的附着连接区的复合物。 V.在培养的大鼠心肌细胞中,小干扰RNA介导的敲低证明了plakophilin-2的重要性。

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摘要

In the adult mammalian heart, the cardiomyocytes are connected by large polar arrays of closely spaced or even fused composite, plaque-bearing adhering junctions (areae compositae, ACs), in a region usually termed "intercalated disk" (ID). We have recently reported that during late embryogenesis and postnatally these polar assemblies of AC-junction structures are gradually formed as replacements of distinct embryonal junctions representing desmosomes and fasciae adhaerentes which then may amalgamate to the fused AC structures, in some regions occupying more than 90% of the total ID area. Previous gene knockout results as well as mutation analyses of specific human cardiomyopathies have suggested that among the various AC constituents, the desmosomal plaque protein, plakophilin-2, plays a particularly important role in the formation, architectural organization and stability of these junctions interconnecting mature cardiomyocytes. To examine this hypothesis, we have decided to study losses of - or molecular alterations in - such AC proteins with respect to their effects on myocardiac organization and functions. Here we report that plakophilin-2 is indeed of obvious importance for myocardial architecture and cell-cell coupling of rat cardiomyocytes growing in culture. We show that siRNA-mediated reduction of the cardiomyocyte content of plakophilin-2 but not of some other major plaque components such as desmoplakin results in progressive disintegration - and losses - of AC junction structures and that numerous variously sized vesicles appear, which are plaque protein-associated as demonstrable by immunofluorescence and immunoelectron microscopy. The importance of plakophilin-2 as a kind of "organizer" protein in the formation, stabilization and functions of the AC structure and the ID architecture is discussed in relation to other junction proteins and to causes of certain cardiomyopathies.
机译:在成年哺乳动物的心脏中,心肌细胞通过紧密间隔或什至融合的,带有斑块的附着连接点(复合区,ACs)的大极性阵列相连,该区域通常称为“插层盘”(ID)。我们最近报道,在胚胎晚期和出生后,这些交流连接结构的极性组装逐渐形成,这是代表桥粒和筋膜筋膜的独特胚胎连接的替代,然后可能融合为融合的交流结构,在某些地区占90%以上总ID区域的。先前的基因敲除结果以及特定人类心肌病的突变分析表明,在各种AC成分中,桥粒斑蛋白plakophilin-2在这些连接成熟心肌细胞的连接的形成,结构组织和稳定性中起着特别重要的作用。 。为了检验该假设,我们决定研究此类AC蛋白对心肌组织和功能的影响,或研究此类AC蛋白的损失或分子变化。在这里,我们报告plakophilin-2确实对于培养中生长的大鼠心肌细胞的心肌结构和细胞-细胞偶联具有明显的重要性。我们显示,siRNA介导的plakophilin-2心肌细胞含量的减少,但不是一些其他主要斑块成分(例如,desmoplakin)的减少导致AC连接结构的逐步崩解和丢失,并且出现了许多大小不同的囊泡,它们是斑块蛋白通过免疫荧光和免疫电子显微镜证实。在其他结构蛋白和某些心肌病的病因中,讨论了亲脂蛋白2作为AC组织和ID结构的形成,稳定和功能的一种“组织者”蛋白的重要性。

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