Get4 的结构揭示了一种适用于尾巴锚定蛋白生物发生中多种相互作用的 α-螺旋环折叠。

The structure of Get4 reveals an alpha-solenoid fold adapted for multiple interactions in tail-anchored protein biogenesis.

机构信息

Heidelberg University Biochemistry Center (BZH), Heidelberg, Germany.

出版信息

FEBS Lett. 2010 Apr 16;584(8):1509-14. doi: 10.1016/j.febslet.2010.02.070. Epub 2010 Mar 3.

DOI:10.1016/j.febslet.2010.02.070

PMID:20206626

Abstract

Tail-anchored proteins play important roles in protein translocation, membrane fusion and apoptosis. They are targeted to the endoplasmic reticulum membrane via the guided-entry of tail-anchored proteins (Get) pathway. We present the 2A crystal structure of Get4 which participates in early steps of the Get pathway. The structure shows an alpha-solenoid fold with particular deviations from the regular pairwise arrangement of alpha-helices. A conserved hydrophobic groove accommodates the flexible C-terminal region in trans. The structural organization of the Get4 helical hairpin motifs provides a scaffold for protein-protein interactions in the Get pathway.

摘要

尾部锚定蛋白在蛋白质易位、膜融合和细胞凋亡中发挥重要作用。它们通过尾部锚定蛋白引导进入（Get）途径靶向内质网膜。我们展示了参与 Get 途径早期步骤的 Get4 的 2A 晶体结构。该结构显示出一种 α-螺旋螺线管折叠，与 α-螺旋的常规成对排列有特殊偏差。一个保守的疏水性凹槽容纳了反式中的柔性 C 末端区域。Get4 螺旋发夹基序的结构组织为 Get 途径中的蛋白质-蛋白质相互作用提供了支架。

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Get4 的结构揭示了一种适用于尾巴锚定蛋白生物发生中多种相互作用的 α-螺旋环折叠。

The structure of Get4 reveals an alpha-solenoid fold adapted for multiple interactions in tail-anchored protein biogenesis.

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