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Novel functions for integrin-associated proteins revealed by analysis of myofibril attachment in Drosophila

机译:果蝇中肌原纤维的附着分析揭示了整合素相关蛋白的新功能

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We use the myotendinous junction of Drosophila flight muscles to explore why many integrin associated proteins (IAPs) are needed and how their function is coordinated. These muscles revealed new functions for IAPs not required for viability: Focal Adhesion Kinase (FAK), RSU1, tensin and vinculin. Genetic interactions demonstrated a balance between positive and negative activities, with vinculin and tensin positively regulating adhesion, while FAK inhibits elevation of integrin activity by tensin, and RSU1 keeps PINCH activity in check. The molecular composition of myofibril termini resolves into 4 distinct layers, one of which is built by a mechanotransduction cascade: vinculin facilitates mechanical opening of filamin, which works with the Arp2/3 activator WASH to build an actin-rich layer positioned between integrins and the first sarcomere. Thus, integration of IAP activity is needed to build the complex architecture of the myotendinous junction, linking the membrane anchor to the sarcomere.
机译:我们使用果蝇飞行肌的肌末端连接来探索为什么需要许多整联蛋白相关蛋白(IAPs)以及它们的功能如何被协调。这些肌肉揭示了IAPs并非生存所需的新功能:粘着斑激酶(FAK),RSU1,肌腱蛋白和纽蛋白。遗传相互作用证明正负活性之间具有平衡,其中纽蛋白和肌腱正调控粘附力,而FAK抑制肌腱使整联蛋白活性升高,而RSU1抑制PINCH活性。肌原纤维末端的分子成分分解为4个不同的层,其中一个层是由机械转导级联构建的:纽蛋白促进了纤维蛋白的机械打开,后者与Arp2 / 3活化剂WASH共同作用,在整合素和蛋白质之间形成了一个富含肌动蛋白的层。第一个肌节。因此,需要整合IAP活性来构建肌腱连接的复杂结构,从而将膜锚与肌节连接起来。

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