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成熟心肌细胞肌节中雷帕霉素靶蛋白和原肌球蛋白的不同定位和细胞行为。

Different localizations and cellular behaviors of leiomodin and tropomodulin in mature cardiomyocyte sarcomeres.

机构信息

Program in Cell and Molecular Biology, Institute of Biotechnology, University of Helsinki, Helsinki 00790, Finland.

出版信息

Mol Biol Cell. 2010 Oct 1;21(19):3352-61. doi: 10.1091/mbc.E10-02-0109. Epub 2010 Aug 4.

Abstract

Leiomodin (Lmod) is a muscle-specific F-actin-nucleating protein that is related to the F-actin pointed-end-capping protein tropomodulin (Tmod). However, Lmod contains a unique ∼150-residue C-terminal extension that is required for its strong nucleating activity. Overexpression or depletion of Lmod compromises sarcomere organization, but the mechanism by which Lmod contributes to myofibril assembly is not well understood. We show that Tmod and Lmod localize through fundamentally different mechanisms to the pointed ends of two distinct subsets of actin filaments in myofibrils. Tmod localizes to two narrow bands immediately adjacent to M-lines, whereas Lmod displays dynamic localization to two broader bands, which are generally more separated from M-lines. Lmod's localization and F-actin nucleation activity are enhanced by interaction with tropomyosin. Unlike Tmod, the myofibril localization of Lmod depends on sustained muscle contraction and actin polymerization. We further show that Lmod expression correlates with the maturation of myofibrils in cultured cardiomyocytes and that it associates with sarcomeres only in differentiated myofibrils. Collectively, the data suggest that Lmod contributes to the final organization and maintenance of sarcomere architecture by promoting tropomyosin-dependent actin filament nucleation.

摘要

肌球蛋白调节蛋白(Lmod)是一种肌肉特异性的 F-actin 成核蛋白,与 F-actin 端帽蛋白原肌球蛋白(Tmod)有关。然而,Lmod 包含一个独特的约 150 个残基的 C 端延伸,这是其强大的成核活性所必需的。Lmod 的过表达或耗竭会破坏肌节的组织,但 Lmod 如何有助于肌原纤维组装的机制尚不清楚。我们表明,Tmod 和 Lmod 通过根本不同的机制定位到肌原纤维中两个不同的肌动蛋白丝子集的尖端。Tmod 定位到紧邻 M 线的两个狭窄带,而 Lmod 则显示出动态定位到两个更宽的带,这些带通常与 M 线分离得更远。Lmod 的定位和 F-actin 成核活性通过与原肌球蛋白的相互作用而增强。与 Tmod 不同,Lmod 在肌原纤维中的定位依赖于持续的肌肉收缩和肌动蛋白聚合。我们进一步表明,Lmod 的表达与培养的心肌细胞中肌原纤维的成熟相关,并且仅在分化的肌原纤维中与肌节相关联。总之,这些数据表明,Lmod 通过促进依赖原肌球蛋白的肌动蛋白丝成核,有助于肌节结构的最终组织和维持。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3b58/2947471/4ccc194bdfc8/zmk0191095820001.jpg

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