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高通量平台实时分析膜裂变反应揭示了动力蛋白的功能。

A high-throughput platform for real-time analysis of membrane fission reactions reveals dynamin function.

机构信息

Indian Institute of Science Education and Research, Dr. Homi Bhabha Road Pashan, Pune 411008, Maharashtra, India.

出版信息

Nat Cell Biol. 2015 Dec;17(12):1588-96. doi: 10.1038/ncb3254. Epub 2015 Oct 19.

Abstract

Dynamin, the paradigmatic membrane fission catalyst, assembles as helical scaffolds that hydrolyse GTP to sever the tubular necks of clathrin-coated pits. Using a facile assay system of supported membrane tubes (SMrT) engineered to mimic the dimensions of necks of clathrin-coated pits, we monitor the dynamics of a dynamin-catalysed tube-severing reaction in real time using fluorescence microscopy. We find that GTP hydrolysis by an intact helical scaffold causes progressive constriction of the underlying membrane tube. On reaching a critical dimension of 7.3 nm in radius, the tube undergoes scission and concomitant splitting of the scaffold. In a constant GTP turnover scenario, scaffold assembly and GTP hydrolysis-induced tube constriction are kinetically inseparable events leading to tube-severing reactions occurring at timescales similar to the characteristic fission times seen in vivo. We anticipate SMrT templates to allow dynamic fluorescence-based detection of conformational changes occurring in self-assembling proteins that remodel membranes.

摘要

动力蛋白是典型的膜裂变催化剂,组装成螺旋支架,通过水解 GTP 来切断网格蛋白包被的凹陷的管状颈部。我们使用一种简单的支持膜管(SMrT)测定系统,该系统经过工程设计可模拟网格蛋白包被的凹陷颈部的尺寸,利用荧光显微镜实时监测动力蛋白催化的管状切割反应的动力学。我们发现,完整的螺旋支架的 GTP 水解会导致下面的膜管逐渐变细。当达到半径为 7.3nm 的临界尺寸时,管会发生分裂,同时支架也会分裂。在恒定的 GTP 周转率情况下,支架组装和 GTP 水解诱导的管收缩是动力学上不可分离的事件,导致管切割反应发生的时间尺度与体内观察到的特征裂变时间相似。我们预计 SMrT 模板将允许基于动态荧光的检测自组装蛋白质在重塑膜时发生的构象变化。

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