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obscurin在肌节M带周边与一种新型的慢肌球蛋白结合蛋白C(MyBP-C)异构体相互作用,并调节粗肌丝组装。

Obscurin interacts with a novel isoform of MyBP-C slow at the periphery of the sarcomeric M-band and regulates thick filament assembly.

作者信息

Ackermann Maegen A, Hu Li-Yen R, Bowman Amber L, Bloch Robert J, Kontrogianni-Konstantopoulos Aikaterini

机构信息

Department of Biochemistry and Molecular Biology, University of Maryland School of Medicine, Baltimore, MD 21201, USA.

出版信息

Mol Biol Cell. 2009 Jun;20(12):2963-78. doi: 10.1091/mbc.e08-12-1251. Epub 2009 Apr 29.

Abstract

Obscurin is a multidomain protein composed of adhesion and signaling domains that plays key roles in the organization of contractile and membrane structures in striated muscles. Overexpression of the second immunoglobulin domain of obscurin (Ig2) in developing myotubes inhibits the assembly of A- and M-bands, but not Z-disks or I-bands. This effect is mediated by the direct interaction of the Ig2 domain of obscurin with a novel isoform of myosin binding protein-C slow (MyBP-C slow), corresponding to variant-1. Variant-1 contains all the structural motifs present in the known forms of MyBP-C slow, but it has a unique COOH terminus. Quantitative reverse transcription-polymerase chain reaction indicated that MyBP-C slow variant-1 is expressed in skeletal muscles both during development and at maturity. Immunolabeling of skeletal myofibers with antibodies to the unique COOH terminus of variant-1 demonstrated that, unlike other forms of MyBP-C slow that reside in the C-zones of A-bands, variant-1 preferentially concentrates around M-bands, where it codistributes with obscurin. Overexpression of the Ig2 domain of obscurin or reduction of expression of obscurin inhibited the integration of variant-1 into forming M-bands in skeletal myotubes. Collectively, our experiments identify a new ligand of obscurin at the M-band, MyBP-C slow variant-1 and suggest that their interaction contributes to the assembly of M- and A-bands.

摘要

obscurin是一种多结构域蛋白,由粘附和信号结构域组成,在横纹肌收缩和膜结构的组织中起关键作用。 obscurin的第二个免疫球蛋白结构域(Ig2)在发育中的肌管中过表达会抑制A带和M带的组装,但不会抑制Z盘或I带的组装。这种效应是由obscurin的Ig2结构域与肌球蛋白结合蛋白-C慢型(MyBP-C慢型)的一种新型异构体直接相互作用介导的,该异构体对应于变体-1。变体-1包含已知形式的MyBP-C慢型中存在的所有结构基序,但它有一个独特的COOH末端。定量逆转录-聚合酶链反应表明,MyBP-C慢型变体-1在发育和成熟阶段的骨骼肌中均有表达。用针对变体-1独特COOH末端的抗体对骨骼肌纤维进行免疫标记表明,与其他位于A带C区的MyBP-C慢型形式不同,变体-1优先集中在M带周围,在那里它与obscurin共分布。obscurin的Ig2结构域过表达或obscurin表达降低会抑制变体-1整合到骨骼肌管中正在形成的M带中。总的来说,我们的实验确定了M带处obscurin的一种新配体,即MyBP-C慢型变体-1,并表明它们的相互作用有助于M带和A带的组装。

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