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原肌球蛋白在肌生成过程中的非经典作用。

Noncanonical roles for Tropomyosin during myogenesis.

作者信息

Williams Jessica, Boin Nathan G, Valera Juliana M, Johnson Aaron N

机构信息

Department of Integrative Biology, University of Colorado Denver, Denver, CO 80217, USA.

Department of Integrative Biology, University of Colorado Denver, Denver, CO 80217, USA

出版信息

Development. 2015 Oct 1;142(19):3440-52. doi: 10.1242/dev.117051. Epub 2015 Aug 20.

Abstract

For skeletal muscle to produce movement, individual myofibers must form stable contacts with tendon cells and then assemble sarcomeres. The myofiber precursor is the nascent myotube, and during myogenesis the myotube completes guided elongation to reach its target tendons. Unlike the well-studied events of myogenesis, such as myoblast specification and myoblast fusion, the molecules that regulate myotube elongation are largely unknown. In Drosophila, hoi polloi (hoip) encodes a highly conserved RNA-binding protein and hoip mutant embryos are largely paralytic due to defects in myotube elongation and sarcomeric protein expression. We used the hoip mutant background as a platform to identify novel regulators of myogenesis, and uncovered surprising developmental functions for the sarcomeric protein Tropomyosin 2 (Tm2). We have identified Hoip-responsive sequences in the coding region of the Tm2 mRNA that are essential for Tm2 protein expression in developing myotubes. Tm2 overexpression rescued the hoip myogenic phenotype by promoting F-actin assembly at the myotube leading edge, by restoring the expression of additional sarcomeric RNAs, and by promoting myoblast fusion. Embryos that lack Tm2 also showed reduced sarcomeric protein expression, and embryos that expressed a gain-of-function Tm2 allele showed both fusion and elongation defects. Tropomyosin therefore dictates fundamental steps of myogenesis prior to regulating contraction in the sarcomere.

摘要

为了使骨骼肌产生运动,单个肌纤维必须与肌腱细胞形成稳定的连接,然后组装肌节。肌纤维前体是新生的肌管,在肌生成过程中,肌管完成定向伸长以到达其目标肌腱。与研究充分的肌生成事件,如成肌细胞特化和成肌细胞融合不同,调节肌管伸长的分子在很大程度上是未知的。在果蝇中,hoi polloi(hoip)编码一种高度保守的RNA结合蛋白,hoip突变胚胎由于肌管伸长和肌节蛋白表达缺陷而基本瘫痪。我们以hoip突变背景为平台来鉴定肌生成的新调节因子,并发现了肌节蛋白原肌球蛋白2(Tm2)惊人的发育功能。我们在Tm2 mRNA的编码区鉴定出了Hoip反应序列,这些序列对于发育中的肌管中Tm2蛋白的表达至关重要。Tm2的过表达通过促进肌管前沿的F-肌动蛋白组装、恢复其他肌节RNA的表达以及促进成肌细胞融合,挽救了hoip的肌生成表型。缺乏Tm2的胚胎也显示出肌节蛋白表达减少,而表达功能获得性Tm2等位基因的胚胎则表现出融合和伸长缺陷。因此,原肌球蛋白在调节肌节收缩之前决定了肌生成的基本步骤。

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