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Mammalian Atg2 proteins are essential for autophagosome formation and important for regulation of size and distribution of lipid droplets

机译:哺乳动物Atg2蛋白对于自噬体形成至关重要对调节脂滴的大小和分布也很重要

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摘要

Macroautophagy is an intracellular degradation system by which cytoplasmic materials are enclosed by the autophagosome and delivered to the lysosome. Autophagosome formation is considered to take place on the endoplasmic reticulum and involves functions of autophagy-related (Atg) proteins. Here, we report the identification and characterization of mammalian Atg2 homologues Atg2A and Atg2B. Simultaneous silencing of Atg2A and Atg2B causes a block in autophagic flux and accumulation of unclosed autophagic structures containing most Atg proteins. Atg2A localizes on the autophagic membrane, as well as on the surface of lipid droplets. The Atg2A region containing amino acids 1723–1829, which shows relatively high conservation among species, is required for localization to both the autophagic membrane and lipid droplet and is also essential for autophagy. Depletion of both Atg2A and Atg2B causes clustering of enlarged lipid droplets in an autophagy-independent manner. These data suggest that mammalian Atg2 proteins function both in autophagosome formation and regulation of lipid droplet morphology and dispersion.
机译:巨自噬是一种细胞内降解系统,细胞质材料通过该系统被自噬体包裹并传递至溶酶体。自噬体形成被认为发生在内质网上,并涉及自噬相关(Atg)蛋白的功能。在这里,我们报告哺乳动物Atg2同源物Atg2A和Atg2B的鉴定和表征。 Atg2A和Atg2B同时沉默会导致自噬通量受阻,并导致包含大多数Atg蛋白的未封闭自噬结构积累。 Atg2A定位在自噬膜以及脂滴表面。 Atg2A区域包含1723–1829位氨基酸,在物种之间显示出较高的保守性,是定位到自噬膜和脂质滴的必需区域,并且对于自噬也是必不可少的。 Atg2A和Atg2B的耗尽都会以自噬无关的方式导致放大的脂质液滴聚集。这些数据表明,哺乳动物Atg2蛋白在自噬小体的形成以及脂滴形态和分散的调节中均起作用。

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