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Beclin1 卷曲螺旋结构域的不完美界面调节与 Atg14L 和 UVRAG 的同源二聚体和异源二聚体形成。

Imperfect interface of Beclin1 coiled-coil domain regulates homodimer and heterodimer formation with Atg14L and UVRAG.

机构信息

Department of Applied Biology and Chemical Technology, State Key Laboratory of Chirosciences, The Hong Kong Polytechnic University, Hung Hom, Kowloon, Hong Kong, PR China.

出版信息

Nat Commun. 2012 Feb 7;3:662. doi: 10.1038/ncomms1648.

Abstract

Beclin 1 is a core component of the Class III Phosphatidylinositol 3-Kinase VPS34 complex. The coiled coil domain of Beclin 1 serves as an interaction platform for assembly of distinct Atg14L- and UVRAG-containing complexes to modulate VPS34 activity. Here we report the crystal structure of the coiled coil domain that forms an antiparallel dimer and is rendered metastable by a series of 'imperfect' a-d' pairings at its coiled coil interface. Atg14L and UVRAG promote the transition of metastable homodimeric Beclin 1 to heterodimeric Beclin1-Atg14L/UVRAG assembly. Beclin 1 mutants with their 'imperfect' a-d' pairings modified to enhance self-interaction, show distinctively altered interactions with Atg14L or UVRAG. These results suggest that specific utilization of the dimer interface and modulation of the homodimer-heterodimer transition by Beclin 1-interacting partners may underlie the molecular mechanism that controls the formation of various Beclin1-VPS34 subcomplexes to exert their effect on an array of VPS34-related activities, including autophagy.

摘要

Beclin 1 是 Class III 磷酸肌醇 3-激酶 VPS34 复合物的核心组成部分。Beclin 1 的卷曲螺旋结构域作为一个相互作用平台,用于组装不同的含有 Atg14L 和 UVRAG 的复合物,从而调节 VPS34 的活性。在此,我们报告了卷曲螺旋结构域的晶体结构,该结构域形成一个反平行二聚体,并通过一系列卷曲螺旋界面的“不完美”a-d' 配对使其处于亚稳态。Atg14L 和 UVRAG 促进亚稳态同源二聚体 Beclin 1 向异源二聚体 Beclin1-Atg14L/UVRAG 组装的转变。其“不完美”a-d' 配对被修饰以增强自身相互作用的 Beclin 1 突变体,与 Atg14L 或 UVRAG 的相互作用明显改变。这些结果表明,Beclin 1 相互作用伙伴对二聚体界面的特定利用和同源二聚体-异源二聚体转变的调节,可能是控制各种 Beclin1-VPS34 亚复合物形成的分子机制的基础,从而发挥其对一系列与 VPS34 相关的活性的影响,包括自噬。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d4b8/3293417/3c2757434729/ncomms1648-f1.jpg

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