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首页> 外文期刊>Molecular biology of the cell >Kinesin-related Smy1 enhances the Rab-dependent association of myosin-V with secretory cargo
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Kinesin-related Smy1 enhances the Rab-dependent association of myosin-V with secretory cargo

机译:驱动蛋白相关的Smy1增强了肌球蛋白V与分泌性货物的Rab依赖性结合。

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摘要

The mechanisms by which molecular motors associate with specific cargo is a central problem in cell organization. The kinesin-like protein Smy1 of budding yeast was originally identified by the ability of elevated levels to suppress a conditional myosin-V mutation (myo2-66), but its function with Myo2 remained mysterious. Subsequently, Myo2 was found to provide an essential role in delivery of secretory vesicles for polarized growth and in the transport of mitochondria for segregation. By isolating and characterizing myo2 smy1 conditional mutants, we uncover the molecular function of Smy1 as a factor that enhances the association of Myo2 with its receptor, the Rab Sec4, on secretory vesicles. The tail of Smy1-which binds Myo2-its central dimerization domain, and its kinesin-like head domain are all necessary for this function. Consistent with this model, overexpression of full-length Smy1 enhances the number of Sec4 receptors and Myo2 motors per transporting secretory vesicle. Rab proteins Sec4 and Ypt11, receptors for essential transport of secretory vesicles and mitochondria, respectively, bind the same region on Myo2, yet Smy1 functions selectively in the transport of secretory vesicles. Thus a kinesin-related protein can function intimately with a myosin-V and its receptor in the transport of a specific cargo.
机译:分子马达与特定货物相关联的机制是细胞组织中的中心问题。最初通过升高的水平抑制条件性肌球蛋白-V突变(myo2-66)的能力来鉴定出芽酵母的驱动蛋白样蛋白Smy1,但其与Myo2的功能仍然神秘。随后,Myo2被发现在分泌性囊泡的极化生长和线粒体的分离转运中起着至关重要的作用。通过分离和表征myo2 smy1条件突变体,我们发现Smy1的分子功能是一个因子,可增强Myo2及其受体Rab Sec4在分泌性囊泡上的结合。 Smy1的尾部结合了Myo2的中央二聚结构域,其驱动蛋白样头部结构域对于此功能而言都是必需的。与该模型一致,全长Smy1的过表达增加了每个转运分泌小泡的Sec4受体和Myo2马达的数量。 Rab蛋白Sec4和Ypt11,分别是分泌小泡和线粒体必需转运的受体,结合Myo2的相同区域,而Smy1在分泌小泡的转运中选择性发挥功能。因此,在特定货物的运输中,驱动蛋白相关蛋白可与肌球蛋白V及其受体密切相关。

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