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内体微自噬是氨基酸饥饿诱导自噬反应的一个组成部分。

Endosomal microautophagy is an integrated part of the autophagic response to amino acid starvation.

机构信息

a Molecular Cancer Research Group, Department of Medical Biology , University of Tromsø -The Arctic University of Norway , Tromsø , Norway.

b Department of Biochemistry , Institute for Cancer Research, Oslo University Hospital , Oslo , Norway.

出版信息

Autophagy. 2019 Jan;15(1):182-183. doi: 10.1080/15548627.2018.1532265. Epub 2018 Oct 25.

Abstract

Starvation is a fundamental type of stress naturally occurring in biological systems. All organisms have therefore evolved different safeguard mechanisms to cope with deficiencies in various types of nutrients. Cells, from yeast to humans, typically respond to amino acid starvation by initiating degradation of cellular components by inducing autophagy. This degradation releases metabolic building blocks to sustain essential core cellular processes. Increasing evidence indicates that starvation-induced autophagy also acts to prepare cells for prolonged starvation by degrading key regulators of different cellular processes. In a recent study, we found that within the first hours of amino acid starvation cells elicit an autophagic response causing rapid degradation of specific proteins. The response is executed independently of both MTOR and canonical macroautophagy. Based on RNAi-mediated knockdown of essential components of the Endosomal Sorting Complex Required for Transport (ESCRT) machinery and electron microscopy we conclude that the response relies on some sort of endosomal microautophagy, hence vesicle budding into endosomes. Substantiated by the different substrates that are selectively degraded by this novel pathway we propose that the response predominantly acts to prepare cells for prolonged starvation. Intriguingly, this includes shutting down selective macroautophagy in preparation for a massive induction of bulk macroautophagy.

摘要

饥饿是生物系统中自然发生的一种基本应激类型。因此,所有生物体都进化出不同的保护机制来应对各种营养物质的缺乏。从酵母到人类的细胞,通常会通过诱导自噬来降解细胞成分,以应对氨基酸饥饿。这种降解释放代谢构建块,以维持基本的核心细胞过程。越来越多的证据表明,饥饿诱导的自噬还可以通过降解不同细胞过程的关键调节剂来为细胞长时间饥饿做准备。在最近的一项研究中,我们发现,在氨基酸饥饿的最初几个小时内,细胞会引发自噬反应,导致特定蛋白质的快速降解。这种反应的执行独立于 MTOR 和经典的巨自噬。基于内体分选复合物必需成分的 RNAi 介导的敲低和电子显微镜,我们得出结论,该反应依赖于某种内体微自噬,因此囊泡进入内体。通过这种新途径选择性降解的不同底物证实,该反应主要作用是为细胞长时间饥饿做准备。有趣的是,这包括关闭选择性巨自噬,为大量诱导巨自噬做准备。

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