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Comparative analysis of adaptor-mediated clathrin assembly reveals general principles for adaptor clustering

机译:适配器介导的网格蛋白组装的比较分析揭示了适配器簇的一般原理

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Clathrin-mediated endocytosis (CME) manages the sorting and uptake of the bulk of membrane proteins (or cargo) from the plasma membrane. CME is initiated by the formation of clathrin-coated pits (CCPs), in which adaptors nucleate clathrin assembly. Clathrin adaptors display diversity in both the type and number of evolutionarily conserved clathrin-binding boxes. How this diversity relates to the process of adaptor clustering as clathrin assembles around a growing pit remains unclear. Using real-time, fluorescence microscopy–based assays, we compare the formation kinetics and distribution of clathrin assemblies on membranes that display five unique clathrin adaptors. Correlations between equilibrium and kinetic parameters of clathrin assembly to the eventual adaptor distribution indicate that adaptor clustering is determined not by the amount of clathrin recruited or the degree of clathrin clustered but instead by the rate of clathrin assembly. Together our results emphasize the need to analyze kinetics of protein interactions to better understand mechanisms that regulate CME.
机译:网格蛋白介导的内吞作用(CME)管理着质膜中大部分膜蛋白(或货物)的分选和摄取。 CME通过形成网格蛋白涂层的凹坑(CCP)来启动,其中衔接子使网格蛋白组装成核。网格蛋白衔接子在进化上保守的网格蛋白结合盒的类型和数量上都表现出多样性。网格蛋白围绕生长的小窝聚集时,这种多样性与衔接子簇集过程之间的关系尚不清楚。使用基于实时荧光显微镜的分析方法,我们比较了网格蛋白组装体在膜上的形成动力学和分布,该膜具有五个独特的网格蛋白衔接子。网格蛋白组装的平衡和动力学参数与最终衔接子分布之间的相关性表明,衔接子簇集不是由募集的网格蛋白的量或网格蛋白的簇集程度决定的,而是由网格蛋白组装的速率决定的。我们的研究结果共同强调了需要分析蛋白质相互作用的动力学,以更好地了解调节CME的机制。

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