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Get1 通过结合两个不同的界面稳定 Get3 ATP 酶的开放二聚体构象。

Get1 stabilizes an open dimer conformation of get3 ATPase by binding two distinct interfaces.

机构信息

Structural Biology Laboratory, Life Science Division, Synchrotron Radiation Research Organization and Institute of Molecular and Cellular Biosciences, the University of Tokyo, Tokyo 113‐0032, Japan.

出版信息

J Mol Biol. 2012 Sep 21;422(3):366-75. doi: 10.1016/j.jmb.2012.05.045. Epub 2012 Jun 7.

Abstract

Tail-anchored (TA) proteins are integral membrane proteins that possess a single transmembrane domain near their carboxy terminus. TA proteins play critical roles in many important cellular processes such as membrane trafficking, protein translocation, and apoptosis. The GET complex mediates posttranslational insertion of newly synthesized TA proteins to the endoplasmic reticulum membrane. The GET complex is composed of the homodimeric Get3 ATPase and its heterooligomeric receptor, Get1/2. During insertion, the Get3 dimer shuttles between open and closed conformational states, coupled with ATP hydrolysis and the binding/release of TA proteins. We report crystal structures of ADP-bound Get3 in complex with the cytoplasmic domain of Get1 (Get1CD) in open and semi-open conformations at 3.0- and 4.5-Å resolutions, respectively. Our structures and biochemical data suggest that Get1 uses two interfaces to stabilize the open dimer conformation of Get3. We propose that one interface is sufficient for binding of Get1 by Get3, while the second interface stabilizes the open dimer conformation of Get3.

摘要

尾部锚定(TA)蛋白是一类单一跨膜结构域蛋白,其跨膜结构域位于蛋白羧基端附近。TA 蛋白在许多重要的细胞过程中发挥着关键作用,如膜运输、蛋白易位和细胞凋亡。GET 复合物介导新合成的 TA 蛋白的翻译后插入内质网膜。GET 复合物由 Get3 二聚体 ATP 酶及其异源寡聚体受体 Get1/2 组成。在插入过程中,Get3 二聚体在开放和闭合构象之间穿梭,伴随着 ATP 水解和 TA 蛋白的结合/释放。我们报告了 ADP 结合的 Get3 与 Get1 细胞质结构域(Get1CD)在开放和半开放构象下的晶体结构,分辨率分别为 3.0 和 4.5Å。我们的结构和生化数据表明,Get1 使用两个界面来稳定 Get3 的开放二聚体构象。我们提出,一个界面足以使 Get3 结合 Get1,而第二个界面则稳定 Get3 的开放二聚体构象。

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