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The crystal structure of the FAM134B-GABARAP complex provides mechanistic insights into the selective binding of FAM134 to the GABARAP subfamily

机译:FAM134B-GABARAP 复合物的晶体结构为 FAM134 与 GABARAP 亚家族的选择性结合提供了机制见解

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摘要

The mammalian Atg8 family (Atg8s proteins) consists of two subfamilies: GABARAP and LC3. All members can bind to the LC3-interacting region (LIR) or Atg8-interacting motif and participate in multiple steps of autophagy. The endoplasmic reticulum (ER) autophagy receptor FAM134B contains an LIR motif that can bind to Atg8s, but whether it can differentially bind to the two subfamilies and, if so, the structural basis for this preference remains unknown. Here, we found that FAM134B bound to the GABARAP subfamily more strongly than to the LC3 subfamily. We then solved the crystal structure of the FAM134B-GABARAP complex and demonstrated that FAM134B used both its LIR core and the C-terminal helix to bind to GABARAP. We further showed that these properties might be conserved in FAM134A or FAM134C. The structure also allowed us to identify the structural determinants for the binding selectivity. Our work may be valuable for studying the differential functions of GABARAP and LC3 subfamilies in ER phagy in future.
机译:哺乳动物 Atg8 家族(Atg8s 蛋白)由两个亚家族组成:GABARAP 和 LC3。所有成员都可以与 LC3 相互作用区 (LIR) 或 Atg8 相互作用基序结合,并参与自噬的多个步骤。内质网 (ER) 自噬受体 FAM134B 包含一个可以与 Atg8s 结合的 LIR 基序,但它是否可以与两个亚家族差异结合,如果是这样,这种偏好的结构基础仍然未知。在这里,我们发现FAM134B与GABARAP亚家族的结合比与LC3亚家族的结合更强。然后,我们解析了FAM134B-GABARAP复合物的晶体结构,并证明FAM134B同时使用其LIR核心和C端螺旋与GABARAP结合。我们进一步表明,这些特性可能在FAM134A或FAM134C中是保守的。该结构还使我们能够确定结合选择性的结构决定因素。我们的工作对未来研究GABARAP和LC3亚家族在内质网自噬中的差异功能可能具有价值。

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