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首页> 外文期刊>BMC Cell Biology >The interaction of Kinesin-1 with its adaptor protein JIP1 can be regulated via proteins binding to the JIP1-PTB domain
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The interaction of Kinesin-1 with its adaptor protein JIP1 can be regulated via proteins binding to the JIP1-PTB domain

机译:Kinesin-1及其衔接蛋白JIP1的相互作用可通过与JIP1-PTB结构域结合的蛋白来调节

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摘要

Background The regulatory mechanisms of motor protein-dependent intracellular transport are still not fully understood. The kinesin-1-binding protein, JIP1, can function as an adaptor protein that links kinesin-1 and other JIP1-binding “cargo” proteins. However, it is unknown whether these “cargo” proteins influence the JIP1–kinesin-1 binding. Results We show here that JIP1–kinesin-1 binding in Neuro2a cells was dependent on conserved amino acid residues in the JIP1-phosphotyrosine binding (PTB) domain, including F687. In addition, mutation of F687 severely affected the neurite tip localization of JIP1. Proteomic analysis revealed another kinesin-1 binding protein, JIP3, as a major JIP1 binding protein. The association between JIP1 and JIP3 was dependent on the F687 residue in JIP1, and this association induced the formation of a stable ternary complex with kinesin-1. On the other hand, the binding of JIP1 and JIP3 was independent of kinesin-1 binding. We also show that other PTB binding proteins can interrupt the formation of the ternary complex. Conclusions The formation of the JIP1–kinesin-1 complex depends on the protein binding-status of the JIP1 PTB domain. This may imply a regulatory mechanism of kinesin-1-dependent intracellular transport.
机译:背景技术运动蛋白依赖性细胞内转运的调节机制仍不完全清楚。驱动蛋白1结合蛋白JIP1可以充当衔接蛋白,该蛋白连接驱动蛋白1和其他结合JIP1的“货物”蛋白。但是,尚不清楚这些“货物”蛋白是否会影响JIP1-kinesin-1的结合。结果我们在这里显示Neuro2a细胞中的JIP1-驱动蛋白-1结合依赖于JIP1-磷酸酪氨酸结合(PTB)域(包括F687)中的保守氨基酸残基。另外,F687的突变严重影响了JIP1的神经突尖端定位。蛋白质组学分析显示,另一种驱动蛋白1结合蛋白JIP3是主要的JIP1结合蛋白。 JIP1和JIP3之间的关联取决于JIP1中的F687残基,并且这种关联诱导形成与kinesin-1稳定的三元复合物。另一方面,JIP1和JIP3的结合独立于驱动蛋白1的结合。我们还表明,其他PTB结合蛋白可以中断三元复合物的形成。结论JIP1-kinesin-1复合物的形成取决于JIP1 PTB结构域的蛋白质结合状态。这可能暗示了驱动蛋白1依赖性细胞内运输的调节机制。

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