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在2,3-丁二酮一肟存在的情况下,与肌动蛋白结合的肌肉横桥会发生紊乱。

Muscle cross-bridges bound to actin are disordered in the presence of 2,3-butanedione monoxime.

作者信息

Zhao L, Naber N, Cooke R

机构信息

Department of Biochemistry and Biophysics, University of California, San Francisco 94143, USA.

出版信息

Biophys J. 1995 May;68(5):1980-90. doi: 10.1016/S0006-3495(95)80375-9.

Abstract

Electron paramagnetic resonance spectroscopy was used to monitor the orientation of muscle cross-bridges attached to actin in a low force and high stiffness state that may occur before force generation in the actomyosin cycle of interactions. 2,3-butanedione monoxime (BDM) has been shown to act as an uncompetitive inhibitor of the myosin ATPase that stabilizes a myosin.ADP.P(i) complex. Such a complex is thought to attach to actin at the beginning of the powerstroke. Addition of 25 mM BDM decreases tension by 90%, although stiffness remains high, 40-50% of control, showing that cross-bridges are attached to actin but generate little or no force. Active cross-bridge orientation was monitored via electron paramagnetic resonance spectroscopy of a maleimide spin probe rigidly attached to cys-707 (SH-1) on the myosin head. A new labeling procedure was used that showed improved specificity of labeling. In 25 mM BDM, the probes have an almost isotropic angular distribution, indicating that cross-bridges are highly disordered. We conclude that in the pre-powerstroke state stabilized by BDM, cross-bridges are attached to actin, generating little force, with a large portion of the catalytic domain of the myosin heads disordered.

摘要

电子顺磁共振光谱被用于监测在肌动球蛋白相互作用循环中力产生之前可能出现的低力和高刚度状态下附着于肌动蛋白的肌肉横桥的取向。已证明2,3 - 丁二酮单肟(BDM)可作为肌球蛋白ATP酶的非竞争性抑制剂,稳定肌球蛋白 - ADP - P(i)复合物。这种复合物被认为在动力冲程开始时附着于肌动蛋白。添加25 mM BDM可使张力降低90%,尽管刚度仍保持在较高水平,为对照的40 - 50%,这表明横桥附着于肌动蛋白但产生的力很小或几乎不产生力。通过对刚性附着于肌球蛋白头部cys - 707(SH - 1)上的马来酰亚胺自旋探针进行电子顺磁共振光谱来监测活性横桥的取向。采用了一种新的标记程序,显示出标记特异性有所提高。在25 mM BDM中,探针具有几乎各向同性的角度分布,表明横桥高度无序。我们得出结论,在由BDM稳定的动力冲程前状态下,横桥附着于肌动蛋白,产生的力很小,且肌球蛋白头部的大部分催化结构域无序。

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