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人源 ATG9A 结构及其与类脂双层的相互作用。

The structure of human ATG9A and its interplay with the lipid bilayer.

机构信息

Section on Intracellular Protein Trafficking, Neurosciences and Cellular and Structural Biology Division, Eunice Kennedy Shriver National Institute of Child Health and Human Development, National Institutes of Health , Bethesda, MD, USA.

Unit on Structural and Chemical Biology of Membrane Proteins, Neurosciences and Cellular and Structural Biology Division, Eunice Kennedy Shriver National Institute of Child Health and Human Development, National Institutes of Health , Bethesda, MD, USA.

出版信息

Autophagy. 2020 Dec;16(12):2292-2293. doi: 10.1080/15548627.2020.1830522. Epub 2020 Oct 16.

Abstract

ATG9, the only transmembrane protein in the core macroautophagy/autophagy machinery, is a key player in the early stages of autophagosome formation. Yet, the lack of a high-resolution structure of ATG9 was a major impediment in understanding its three-dimensional organization and function. We recently solved a high-resolution cryoEM structure of the ubiquitously expressed human ATG9A isoform. The structure revealed that ATG9A is a domain-swapped homotrimer with a unique fold, and has an internal network of branched cavities. analyses demonstrated the functional importance of the cavity-lining residues. These cavities could serve as conduits for transport of hydrophilic moieties, such as lipid headgroups, across the bilayer. Finally, structure-guided molecular dynamics predicted that ATG9A has membrane-bending properties, which is consistent with its localization to highly curved membranes.

摘要

ATG9 是核心巨自噬/自噬机制中唯一的跨膜蛋白,是自噬体形成早期的关键参与者。然而,缺乏 ATG9 的高分辨率结构是理解其三维结构和功能的主要障碍。我们最近解决了普遍表达的人 ATG9A 同工型的高分辨率冷冻电镜结构。该结构表明,ATG9A 是一种具有独特折叠的结构域交换同源三聚体,并且具有分支腔的内部网络。分析表明腔衬里残基的功能重要性。这些腔可以作为亲水分子,如脂质头部,穿过双层的通道。最后,结构导向的分子动力学预测 ATG9A 具有膜弯曲性质,这与其定位于高度弯曲的膜一致。

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