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Rab1A regulates anterograde melanosome transport by recruiting kinesin-1 to melanosomes through interaction with SKIP

机译:Rab1A通过与SKIP相互作用将kinesin-1募集到黑素体中来调节顺行黑素体运输。

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摘要

Melanosomes are lysosome-related organelles in melanocytes that are transported from the perinucleus to the cell periphery by coordination between bidirectional (anterograde and retrograde) microtubule-dependent transport and unidirectional actin-dependent transport. Although the molecular machineries that mediate retrograde transport and actin-dependent transport have already been identified, little is known about the anterograde transport complex on microtubules in mammalian cells. Here we discovered that small GTPase Rab1A on melanosomes recruits SKIP/PLEKHM2 as a Rab1A-specific effector and that Rab1A, SKIP, and a kinesin-1/(Kif5b+KLC2) motor form a transport complex that mediates anterograde melanosome transport in melanocytes. Interestingly, Arl8, Arf-like small GTPase that also interacts with SKIP, is specifically localized at lysosomes and regulates their anterograde transport in melanocytes. Our findings suggest that the anterograde microtubule-dependent transport of melanosomes and lysosomes are differently regulated by independent cargo receptors, i.e., Rab1A and Arl8, respectively, but that a SKIP–kinesin-1 mechanism is responsible for the transport of both.
机译:黑素体是黑素细胞中与溶酶体相关的细胞器,通过双向(顺行和逆行)微管依赖性转运和单向肌动蛋白依赖性转运之间的协调而从核周转运到细胞周围。尽管已经确定了介导逆行转运和肌动蛋白依赖性转运的分子机制,但对于哺乳动物细胞中微管上的顺行转运复合物知之甚少。在这里,我们发现黑素体上的小GTP酶Rab1A募集SKIP / PLEKHM2作为Rab1A特异的效应子,并且Rab1A,SKIP和kinesin-1 /(Kif5b + KLC2)运动形成介导黑素细胞中顺行黑素体转运的转运复合体。有趣的是,Arl8,也与SKIP相互作用的类似Arf的小GTP酶,特异性地定位在溶酶体中,并调节其在黑素细胞中的顺行转运。我们的发现表明,黑素体和溶酶体的顺行微管依赖性转运分别受独立的货物受体Rab1A和Arl8的调控,但SKIP-kinesin-1机制负责两者的转运。

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