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人 ATG3 与脂双层的结合:脂质几何形状和电荷的作用。

Human ATG3 binding to lipid bilayers: role of lipid geometry, and electric charge.

机构信息

Instituto Biofisika (CSIC, UPV/EHU) and Departamento de Bioquímica y Biología Molecular, Universidad del País Vasco, Bilbao, Spain.

出版信息

Sci Rep. 2017 Nov 15;7(1):15614. doi: 10.1038/s41598-017-15057-6.

Abstract

Specific protein-lipid interactions lead to a gradual recruitment of AuTophaGy-related (ATG) proteins to the nascent membrane during autophagosome (AP) formation. ATG3, a key protein in the movement of LC3 towards the isolation membrane, has been proposed to facilitate LC3/GABARAP lipidation in highly curved membranes. In this work we have performed a biophysical study of human ATG3 interaction with membranes containing phosphatidylethanolamine, phosphatidylcholine and anionic phospholipids. We have found that ATG3 interacts more strongly with negatively-charged phospholipid vesicles or nanotubes than with electrically neutral model membranes, cone-shaped anionic phospholipids (cardiolipin and phosphatidic acid) being particularly active in promoting binding. Moreover, an increase in membrane curvature facilitates ATG3 recruitment to membranes although addition of anionic lipid molecules makes the curvature factor relatively less important. The predicted N-terminus amphipathic α-helix of ATG3 would be responsible for membrane curvature detection, the positive residues Lys 9 and 11 being essential in the recognition of phospholipid negative moieties. We have also observed membrane aggregation induced by ATG3 in vitro, which could point to a more complex function of this protein in AP biogenesis. Moreover, in vitro GABARAP lipidation assays suggest that ATG3-membrane interaction could facilitate the lipidation of ATG8 homologues.

摘要

特定的蛋白-脂相互作用导致在自噬体 (AP) 形成过程中,AuTophaGy 相关 (ATG) 蛋白逐渐募集到新生膜上。ATG3 是 LC3 向隔离膜运动的关键蛋白,据推测,它有助于 LC3/GABARAP 在高度弯曲的膜上进行脂化。在这项工作中,我们对人 ATG3 与含有磷脂酰乙醇胺、磷脂酰胆碱和阴离子磷脂的膜的相互作用进行了生物物理研究。我们发现,ATG3 与带负电荷的磷脂囊泡或纳米管的相互作用比与电中性模型膜的相互作用更强,其中锥形阴离子磷脂(心磷脂和磷脂酸)特别活跃,能促进结合。此外,增加膜曲率有利于 ATG3 向膜募集,尽管添加阴离子脂质分子使曲率因子相对不那么重要。ATG3 的预测 N 端两亲性α-螺旋将负责检测膜曲率,阳性残基 Lys 9 和 11 对于识别磷脂的负部分至关重要。我们还观察到 ATG3 在体外诱导的膜聚集,这可能表明该蛋白在 AP 生物发生中具有更复杂的功能。此外,体外 GABARAP 脂化测定表明,ATG3-膜相互作用可能有助于 ATG8 同源物的脂化。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/623f/5688168/569b99d6d7e9/41598_2017_15057_Fig1_HTML.jpg

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