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首页> 外文期刊>Protein Science: A Publication of the Protein Society >Insights into links between autophagy and the ubiquitin system from the structure of LC3B bound to the LIR motif from the E3 ligase NEDD4
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Insights into links between autophagy and the ubiquitin system from the structure of LC3B bound to the LIR motif from the E3 ligase NEDD4

机译:从E3 Ligase NEDD4与LIR主题结合的LC3B结构与LIR主题的结构之间的洞察洞察

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Abstract Members of the LC3/GABARAP family of ubiquitin‐like proteins function during autophagy by serving as membrane linked protein‐binding platforms. Their C‐termini are physically attached to membranes through covalent linkage to primary amines on lipids such as phosphatidylethanolamine, while their ubiquitin‐like fold domains bind “LIR” (LC3‐Interacting Region) sequences found within an extraordinarily diverse array of proteins including regulators of autophagy, adaptors that recruit ubiquitinated cargoes to be degraded, and even proteins controlling processes at membranes that are not associated with autophagy. Recently, LC3/GABARAP proteins were found to bind the ubiquitin E3 ligase NEDD4 to influence ubiquitination associated with autophagy in human cell lines. Here, we use purified recombinant proteins to define LC3B interactions with a specific LIR sequence from NEDD4, present a crystal structure showing atomic details of the interaction, and show that LC3B‐binding can steer intrinsic NEDD4 E3 ligase activity. The data provide detailed molecular insights underlying recruitment of an E3 ubiquitin ligase to phagophores during autophagy.
机译:通过用作膜连接的蛋白质结合平台,在自噬过程中杂皮蛋白样蛋白质的LC3 / Gabarap系列的摘要成员。它们的C-Termini通过对磷脂酰乙醇胺的脂质的共价胺对膜物理连接到膜,而其泛素状的折叠结构域在包括调节器(包括调节器)的异常不同的蛋白质中发现的“LC3相互作用区域)序列结合自噬,招募普遍的货物的适配器降解,甚至蛋白质控制与自噬无关的膜的过程。最近,发现LC3 / Gabarap蛋白结合泛素E3连接酶NEDD4以影响与人细胞系中的自噬相关的ubiquitch。这里,我们使用纯化的重组蛋白来利用来自NEDD4的特定LIR序列的LC3B相互作用,表明晶体结构显示相互作用的原子细节,并表明LC3B结合可以引导内在的NEDD4 E3连接酶活性。该数据在自噬期期间提供了对E3泛素连接酶的募集至吞噬细胞的详细分子见解。

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