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外泌体亚基 Sec3 N 端结构域的功能研究。

Structure-function study of the N-terminal domain of exocyst subunit Sec3.

机构信息

Department of Physiology, School of Medicine, University of Pennsylvania, Philadelphia, Pennsylvania 19104, USA.

出版信息

J Biol Chem. 2010 Apr 2;285(14):10424-33. doi: 10.1074/jbc.M109.096966. Epub 2010 Feb 5.

Abstract

The exocyst is an evolutionarily conserved octameric complex involved in polarized exocytosis from yeast to humans. The Sec3 subunit of the exocyst acts as a spatial landmark for exocytosis through its ability to bind phospholipids and small GTPases. The structure of the N-terminal domain of Sec3 (Sec3N) was determined ab initio and defines a new subclass of pleckstrin homology (PH) domains along with a new family of proteins carrying this domain. Respectively, N- and C-terminal to the PH domain Sec3N presents an additional alpha-helix and two beta-strands that mediate dimerization through domain swapping. The structure identifies residues responsible for phospholipid binding, which when mutated in cells impair the localization of exocyst components at the plasma membrane and lead to defects in exocytosis. Through its ability to bind the small GTPase Cdc42 and phospholipids, the PH domain of Sec3 functions as a coincidence detector at the plasma membrane.

摘要

外被体是一个进化上保守的八聚体复合物,参与从酵母到人类的极化胞吐作用。外被体的 Sec3 亚基通过结合磷脂和小 GTP 酶发挥作用,成为胞吐作用的空间标志物。Sec3(Sec3N)的 N 端结构域的结构是通过从头计算确定的,它定义了一个新的 PH 结构域子类,以及携带该结构域的新蛋白家族。分别在 PH 结构域的 N 和 C 末端,Sec3N 呈现出另外一个α螺旋和两个β链,通过结构域交换介导二聚化。结构确定了负责与磷脂结合的残基,当这些残基在细胞中发生突变时,会损害外被体成分在质膜上的定位,并导致胞吐作用缺陷。Sec3 的 PH 结构域通过结合小 GTP 酶 Cdc42 和磷脂,在质膜上作为一个巧合探测器发挥作用。

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