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脂滴蛋白PLIN2的AMPK依赖性磷酸化触发其被CMA降解。

AMPK-dependent phosphorylation of lipid droplet protein PLIN2 triggers its degradation by CMA.

作者信息

Kaushik Susmita, Cuervo Ana Maria

机构信息

a Department of Developmental and Molecular Biology and Institute for Aging Studies, Albert Einstein College of Medicine , Bronx , NY USA.

出版信息

Autophagy. 2016;12(2):432-8. doi: 10.1080/15548627.2015.1124226.

Abstract

Lipids stored in lipid droplets are hydrolyzed via either cytosolic lipases or a selective form of macroautophagy known as lipophagy. We recently demonstrated that chaperone-mediated autophagy (CMA) is required for the initiation of lipolysis by either of these independent lipolytic pathways. CMA selectively degrades the lipid droplet proteins perilipins (PLIN) 2 and 3 from the lipid droplet surface, thus, facilitating the recruitment of cytosolic lipases and autophagy effector proteins to the lipid droplets. PLIN2 phosphorylation was observed upon induction of lipolysis, but the phosphorylating kinase and the relation of this phosphorylation with CMA of PLIN2 remained unknown. Here, we report that phosphorylation of PLIN2 is dependent on AMPK and occurs after the interaction of PLIN2 with the CMA chaperone HSPA8/Hsc70. Our results highlight a role for posttranslational modifications in priming proteins to be amenable for degradation by CMA.

摘要

储存在脂滴中的脂质可通过胞质脂肪酶或一种称为脂噬的选择性巨自噬形式进行水解。我们最近证明,伴侣介导的自噬(CMA)是这些独立脂解途径中任何一种启动脂解所必需的。CMA选择性地从脂滴表面降解脂滴蛋白围脂滴蛋白(PLIN)2和3,从而促进胞质脂肪酶和自噬效应蛋白募集到脂滴。在脂解诱导后观察到PLIN2磷酸化,但磷酸化激酶以及这种磷酸化与PLIN2的CMA之间的关系仍然未知。在这里,我们报告PLIN2的磷酸化依赖于AMPK,并且发生在PLIN2与CMA伴侣HSPA8/Hsc70相互作用之后。我们的结果突出了翻译后修饰在使蛋白质适于被CMA降解方面的作用。

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