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Regulation of the clathrin-coated vesicle cycle by reversible phosphorylation

机译:通过可逆磷酸化调节克拉仑涂覆的囊泡循环

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Reversible phosphorylation has long been an attractive mechanism to control cycles of coat assembly and disassembly during clathrin-mediated endocytosis.Many of the coat proteins are phosphorylated in vivo and in vitro.Our work has focused on the role of phosphorylation of the mu2 subunit of AP-2 (adaptor protein 2),which appears to be necessary for efficient cargo recruitment.Studies to probe the regulation of mu2 phosphorylation demonstrated that clathrin is a specific activator of the mu2 kinase,and,in permeabilized cells,cargo sequestration,driven by exogenously added clathrin,results in elevated levels of mu2 phosphorylation.Furthermore,phosphorylated mu2 is mainly associated with assembled clathrin in vivo and its steady-state level is strongly reduced in cells depleted of clathrin heavy chain.Our results imply a central role for clathrin in the regulation of cargo selection via modulation of phospho-mu2 levels.This is therefore a novel regulatory role for clathrin that is independent of its structural role and that provides elegant spatial control of AP-2 and cargo interactions,ensuring that AP-2 is only activated at the correct cellular location and in the correct functional context.Ongoing studies are exploring further the roles of reversible phosphorylation in the coated vesicle cycle.
机译:可逆的磷酸化长期以来一直是有吸引力的机制,以包衣的控制周期的组装和拆卸的外壳蛋白的网格蛋白介导endocytosis.Many期间磷酸化在体内和vitro.Our工作集中于AP的MU2亚基的磷酸化的作用-2(衔接蛋白2),这似乎是必需的高效的货物recruitment.Studies探测MU2磷酸化的调节表明,网格蛋白是MU2激酶的特异性活化剂,并且,在透化的细胞,货物封存,通过外源驱动加入网格蛋白,在MU2 phosphorylation.Furthermore水平升高的结果,磷酸化MU2主要与在体内和其稳态电平组装网格蛋白相关联的在耗尽蛋白重chain.Our结果细胞中强烈降低意味着在对网格蛋白核心作用因此通过磷酸MU2各级工作的调制货物选择的调节对于网格蛋白的新型的调节作用是自主创新结其结构的作用ndent并且提供AP-2和货物相互作用的优雅空间控制,从而确保AP-2在正确的细胞位置,并在正确的功能context.Ongoing研究只激活正在探索进一步在可逆磷酸化的作用经涂覆的小泡循环。

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