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The sarcomeric Z-disc component myopodin is a multiadapter protein that interacts with filamin and α-actinin

菲拉明 突触素 生物 细胞生物学 锚蛋白重复序列 肌动蛋白 戴斯弗林 骨骼肌 PDZ域 遗传学 肌营养不良 细胞骨架 基因 解剖 细胞 足细胞 蛋白尿
作者
Anja Linnemann,Peter F.M. van der Ven,Padmanabhan Vakeel,Bernhard Siegfried Albinus,Dirk Simonis,Gerd Bendas,Jörg A. Schenk,Burkhard Micheel,Rudolf A. Kley,Dieter O. Fürst
出处
期刊:European Journal of Cell Biology [Elsevier BV]
卷期号:89 (9): 681-692 被引量:61
标识
DOI:10.1016/j.ejcb.2010.04.004
摘要

Here we introduce myopodin as a novel filamin C binding partner. Corroborative yeast two-hybrid and biochemical analyses indicate that the central part of myopodin that shows high homology to the closely related protein synaptopodin and that is common to all its currently known or predicted variants interacts with filamin C immunoglobulin-like domains 20–21. A detailed characterization of the previously described interaction between myopodin and α-actinin demonstrates for the first time that myopodin contains three independent α-actinin-binding sites. Newly developed myopodin-specific antibodies reveal expression at the earliest stages of in vitro differentiation of human skeletal muscle cells preceding the expression of sarcomeric α-actinin. Myopodin colocalizes with filamin and α-actinin during all stages of muscle development. By contrast, colocalization with its previously identified binding partner zyxin is restricted to early developmental stages. Genetic and cellular analyses of skeletal muscle provided direct evidence for an alternative transcriptional start site in exon three, corroborating the expression of a myopodin variant lacking the PDZ domain encoded by exons 1 and 2 in skeletal muscle. We conclude that myopodin is a multiadapter protein of the sarcomeric Z-disc that links nascent myofibrils to the sarcolemma via zyxin, and might play a role in early assembly and stabilization of the Z-disc. Mutations in FLNC, ACTN2 and several other genes encoding Z-disc-related proteins cause myopathy and cardiomyopathy. Its localization and its association with the myopathy-associated proteins filamin C and α-actinin make myopodin an interesting candidate for a muscle disease gene.

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