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钙离子诱导的原肌球蛋白在肌肉细肌丝中的滚动:重新审视α带和β带假说

Ca2+-induced rolling of tropomyosin in muscle thin filaments: the alpha- and beta-band hypothesis revisited.

作者信息

Holthauzen Luis M F, Corrêa Fernando, Farah Chuck S

机构信息

Departamento de Bioquímica, Instituto de Química, Universidade de São Paulo, Av. Prof. Lineu Prestes 748, CEP 05508-900, São Paulo, SP, Brazil.

出版信息

J Biol Chem. 2004 Apr 9;279(15):15204-13. doi: 10.1074/jbc.M308904200. Epub 2004 Jan 13.

DOI:10.1074/jbc.M308904200
PMID:14724287
Abstract

Tropomyosin is a filamentous coiled-coil protein directly involved in the regulation of the actomyosin interaction responsible for muscle contraction: it transmits the local calcium-induced conformational change in troponin to the helical array of myosin-binding sites on the surface of the actin filament. McLachlan and Stewart (McLachlan, A. D., and Stewart, M. (1976) J. Mol. Biol. 103, 271-298) proposed that the tropomyosin coiled-coil structure can be divided into 14 alternating 19- to 20-residue "alpha- and beta-bands," which could act as alternate 7-fold sets of sites for specific binding to actin in the different conformational states of the regulated thin filament. Here we present the first direct experimental evidence in support of the alpha- and beta-band hypothesis: we analyze the acrylamide quenching of the fluorescence of mutant tropomyosins containing 5-hydroxytryptophan residues at different positions along the coiled-coil structure under a variety of conditions (alone, complexed with actin, and complexed with actin and troponin with or without Ca(2+)). We show that fluorescent probes placed in the alpha-bands become less solvent-exposed in the absence of calcium, whereas those in the beta-bands become less solvent-exposed in the presence of calcium. A model in which the tropomyosin coiled-coil rolls across the actin surface in response to Ca(2+)-binding to troponin most easily explains these observations.

摘要

原肌球蛋白是一种丝状的卷曲螺旋蛋白,直接参与调节负责肌肉收缩的肌动球蛋白相互作用:它将肌钙蛋白中局部钙诱导的构象变化传递到肌动蛋白丝表面肌球蛋白结合位点的螺旋阵列。麦克拉克伦和斯图尔特(麦克拉克伦,A.D.,和斯图尔特,M.(1976年)《分子生物学杂志》103卷,271 - 298页)提出,原肌球蛋白卷曲螺旋结构可分为14个交替的19至20个残基的“α带和β带”,在调节后的细肌丝的不同构象状态下,它们可作为与肌动蛋白特异性结合的交替7重位点集。在此,我们提供了支持α带和β带假说的首个直接实验证据:我们分析了在多种条件下(单独存在、与肌动蛋白复合、与肌动蛋白和肌钙蛋白复合且有或无Ca(2 +)),沿卷曲螺旋结构不同位置含有5 - 羟色氨酸残基的突变原肌球蛋白荧光的丙烯酰胺猝灭情况。我们发现,置于α带的荧光探针在无钙时溶剂暴露减少,而置于β带的荧光探针在有钙时溶剂暴露减少。一个原肌球蛋白卷曲螺旋响应肌钙蛋白结合Ca(2 +)在肌动蛋白表面滚动的模型最能解释这些观察结果。

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