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秀丽隐杆线虫横纹肌和非横纹肌细胞中肌钙蛋白T突变的发育遗传学分析。

Developmental genetic analysis of troponin T mutations in striated and nonstriated muscle cells of Caenorhabditis elegans.

作者信息

Myers C D, Goh P Y, Allen T S, Bucher E A, Bogaert T

机构信息

Department of Cell and Developmental Biology, University of Pennsylvania, School of Medicine, Philadelphia 19104-6058, USA.

出版信息

J Cell Biol. 1996 Mar;132(6):1061-77. doi: 10.1083/jcb.132.6.1061.

Abstract

We have been investigating a set of genes, collectively called mups, that are essential to striated body wall muscle cell positioning in Caenorhabditis elegans. Here we report our detailed characterization of the mup-2 locus, which encodes troponin T (TnT). Mutants for a heat-sensitive allele, called mup-2(e2346ts), and for a putative null, called mup-2(up1), are defective for embryonic body wall muscle cell contraction, sarcomere organization, and cell positioning. Characterizations of the heat-sensitive allele demonstrate that mutants are also defective for regulated muscle contraction in larval and adult body wall muscle, defective for function of the nonstriated oviduct myoepithelial sheath, and defective for epidermal morphogenesis. We cloned the mup-2 locus and its corresponding cDNA. The cDNA encodes a predicted 405-amino acid protein homologous to vertebrate and invertebrate TnT and includes an invertebrate-specific COOH-terminal tail. The mup-2 mutations lie within these cDNA sequences: mup-2(up1) is a termination codon near NH2 terminus (Glu94) and mup-2(e2346ts) is a termination codon in the COOH-terminal invertebrate-specific tail (Trp342). TnT is a muscle contractile protein that, in association with the thin filament proteins tropomyosin, troponin I and troponin C, regulates myosin-actin interaction in response to a rise in intracellular Ca2+. Our findings demonstrate multiple essential functions for TnT and provide a basis to investigate the in vivo functions and protein interactions of TnT in striated and nonstriated muscles.

摘要

我们一直在研究一组基因,统称为mup基因,它们对于秀丽隐杆线虫横纹肌体壁肌肉细胞的定位至关重要。在此,我们报告对mup - 2基因座的详细表征,该基因座编码肌钙蛋白T(TnT)。一个热敏感等位基因mup - 2(e2346ts)和一个假定的无效等位基因mup - 2(up1)的突变体,在胚胎体壁肌肉细胞收缩、肌节组织和细胞定位方面存在缺陷。对热敏感等位基因的表征表明,突变体在幼虫和成虫体壁肌肉的调节性肌肉收缩方面也存在缺陷,在非横纹输卵管肌上皮鞘的功能方面存在缺陷,并且在表皮形态发生方面存在缺陷。我们克隆了mup - 2基因座及其相应的cDNA。该cDNA编码一个预测的405个氨基酸的蛋白质,与脊椎动物和无脊椎动物的TnT同源,并包括一个无脊椎动物特有的COOH末端尾巴。mup - 2突变位于这些cDNA序列内:mup - 2(up1)是靠近NH2末端(Glu94)的终止密码子,mup - 2(e2346ts)是COOH末端无脊椎动物特有的尾巴中的终止密码子(Trp342)。TnT是一种肌肉收缩蛋白,它与细肌丝蛋白原肌球蛋白、肌钙蛋白I和肌钙蛋白C一起,响应细胞内Ca2+浓度的升高来调节肌球蛋白 - 肌动蛋白的相互作用。我们的研究结果证明了TnT的多种重要功能,并为研究TnT在横纹肌和非横纹肌中的体内功能及蛋白质相互作用提供了基础。

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