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线粒体自噬中人类Atg8与心磷脂的相互作用:LC3B、GABARAPL2和GABARAP的特异性特性

Human Atg8-cardiolipin interactions in mitophagy: Specific properties of LC3B, GABARAPL2 and GABARAP.

作者信息

Antón Zuriñe, Landajuela Ane, Hervás Javier H, Montes L Ruth, Hernández-Tiedra Sonia, Velasco Guillermo, Goñi Felix M, Alonso Alicia

机构信息

a Instituto Biofisika (CSIC, UPV/EHU) and Departamento de Bioquímica y Biología Molecular , Universidad del País Vasco , Bilbao , Spain.

b Departamento de Bioquímica y Biología Molecular I , Universidad Complutense , Madrid , Spain.

出版信息

Autophagy. 2016 Dec;12(12):2386-2403. doi: 10.1080/15548627.2016.1240856. Epub 2016 Oct 20.

Abstract

The phospholipid cardiolipin (CL) has been proposed to play a role in selective mitochondrial autophagy, or mitophagy. CL externalization to the outer mitochondrial membrane would act as a signal for the human Atg8 ortholog subfamily, MAP1LC3 (LC3). The latter would mediate both mitochondrial recognition and autophagosome formation, ultimately leading to removal of damaged mitochondria. We have applied quantitative biophysical techniques to the study of CL interaction with various Atg8 human orthologs, namely LC3B, GABARAPL2 and GABARAP. We have found that LC3B interacts preferentially with CL over other di-anionic lipids, that CL-LC3B binding occurs with positive cooperativity, and that the CL-LC3B interaction relies only partially on electrostatic forces. CL-induced increased membrane fluidity appears also as an important factor helping LC3B to bind CL. The LC3B C terminus remains exposed to the hydrophilic environment after protein binding to CL-enriched membranes. In intact U87MG human glioblastoma cells rotenone-induced autophagy leads to LC3B translocation to mitochondria and subsequent delivery of mitochondria to lysosomes. We have also observed that GABARAP, but not GABARAPL2, interacts with CL in vitro. However neither GABARAP nor GABARAPL2 were translocated to mitochondria in rotenone-treated U87MG cells. Thus the various human Atg8 orthologs might play specific roles in different autophagic processes.

摘要

磷脂心磷脂(CL)被认为在选择性线粒体自噬(即线粒体自噬)中发挥作用。CL外化至线粒体外膜将作为人类Atg8直系同源亚家族MAP1LC3(LC3)的信号。后者将介导线粒体识别和自噬体形成,最终导致受损线粒体的清除。我们应用定量生物物理技术研究了CL与各种人类Atg8直系同源物(即LC3B、GABARAPL2和GABARAP)的相互作用。我们发现,与其他二价阴离子脂质相比,LC3B优先与CL相互作用,CL-LC3B结合以正协同性发生,并且CL-LC3B相互作用仅部分依赖于静电力。CL诱导的膜流动性增加似乎也是帮助LC3B结合CL的重要因素。蛋白质与富含CL的膜结合后,LC3B的C末端仍暴露于亲水环境中。在完整的U87MG人胶质母细胞瘤细胞中,鱼藤酮诱导的自噬导致LC3B转运至线粒体,并随后将线粒体递送至溶酶体。我们还观察到,GABARAP而非GABARAPL2在体外与CL相互作用。然而,在鱼藤酮处理的U87MG细胞中,GABARAP和GABARAPL2均未转运至线粒体。因此,各种人类Atg8直系同源物可能在不同的自噬过程中发挥特定作用。

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