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动力蛋白结合和释放微管的结构基础。

Structural basis for microtubule binding and release by dynein.

机构信息

Department of Molecular and Cellular Biology, Harvard University, 52 Oxford Street, Cambridge, MA 02138, United States.

Department of Cell Biology, Harvard Medical School, 240 Longwood Avenue, Boston, MA 02115, USA.

出版信息

Science. 2012 Sep 21;337(6101):1532-1536. doi: 10.1126/science.1224151.

Abstract

Cytoplasmic dynein is a microtubule-based motor required for intracellular transport and cell division. Its movement involves coupling cycles of track binding and release with cycles of force-generating nucleotide hydrolysis. How this is accomplished given the ~25 nanometers separating dynein's track- and nucleotide-binding sites is not understood. Here, we present a subnanometer-resolution structure of dynein's microtubule-binding domain bound to microtubules by cryo-electron microscopy that was used to generate a pseudo-atomic model of the complex with molecular dynamics. We identified large rearrangements triggered by track binding and specific interactions, confirmed by mutagenesis and single-molecule motility assays, which tune dynein's affinity for microtubules. Our results provide a molecular model for how dynein's binding to microtubules is communicated to the rest of the motor.

摘要

细胞质动力蛋白是一种基于微管的马达,对于细胞内运输和细胞分裂是必需的。它的运动涉及到与力产生核苷酸水解循环相结合的轨道结合和释放循环。鉴于动力蛋白的轨道和核苷酸结合位点之间相隔约 25 纳米,这是如何完成的尚不清楚。在这里,我们通过冷冻电镜呈现了动力蛋白的微管结合结构域与微管结合的亚纳米分辨率结构,该结构用于通过分子动力学生成该复合物的拟原子模型。我们通过突变和单分子运动分析鉴定了轨道结合触发的大的重排以及特异性相互作用,这调节了动力蛋白对微管的亲和力。我们的结果提供了一个分子模型,说明动力蛋白与微管的结合如何传递给马达的其余部分。

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