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Atg22 recycles amino acids to link the degradative and recycling functions of autophagy

机译:Atg22回收氨基酸以连接自噬的降解和回收功能

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In response to stress conditions (such as nutrient limitation or accumulation of damaged organelles) and certain pathological situations, eukaryotic cells use autophagy as a survival mechanism. During nutrient stress the main purpose of autophagy is to degrade cytoplasmic materials within the lysosome/vacuole lumen and generate an internal nutrient pool that is recycled back to the cytosol. This study elucidates a molecular mechanism for linking the degradative and recycling roles of autophagy. We show that in contrast to published studies, Atg22 is not directly required for the breakdown of autophagic bodies within the lysosome/vacuole. Instead, we demonstrate that Atg22, Avt3, and Avt4 are partially redundant vacuolar effluxers, which mediate the efflux of leucine and other amino acids resulting from autophagic degradation. The release of autophagic amino acids allows the maintenance of protein synthesis and viability during nitrogen starvation. We propose a "recycling" model that includes the efflux of macromolecules from the lysosome/vacuole as the final step of autophagy.
机译:响应于压力条件(例如营养限制或受损细胞器的积累)和某些病理情况,真核细胞利用自噬作为生存机制。在营养胁迫期间,自噬的主要目的是降解溶酶体/真空管腔内的细胞质物质,并产生内部营养库,该营养库可循环回到细胞质中。这项研究阐明了连接自噬的降解和循环作用的分子机制。我们显示,与已发表的研究相反,溶酶体/真空中自噬体的分解并不直接需要Atg22。相反,我们证明Atg22,Avt3和Avt4是部分多余的液泡流出物,它们介导亮氨酸和其他自噬降解产生的氨基酸的流出。自噬氨基酸的释放可以在氮饥饿期间维持蛋白质合成和活力。我们提出了一个“回收”模型,其中包括溶酶体/真空中大分子的流出作为自噬的最后一步。

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