Selective Autophagy: ATG8 Family Proteins, LIR Motifs and Cargo Receptors | Health & Environmental Research Online (HERO)

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Citation
Tags

HERO ID

7102097

Reference Type

Journal Article

Title

Selective Autophagy: ATG8 Family Proteins, LIR Motifs and Cargo Receptors

Author(s)

Johansen, T; Lamark, T; ,

Year

2020

Is Peer Reviewed?

Yes

Journal

Journal of Molecular Biology
ISSN: 0022-2836
EISSN: 1089-8638

Language

English

PMID

31310766

DOI

10.1016/j.jmb.2019.07.016

Abstract

Selective autophagy relies on soluble or membrane-bound cargo receptors that recognize cargo and bring about autophagosome formation at the cargo. The cargo-bound receptors interact with lipidated ATG8 family proteins anchored in the membrane at the concave side of the forming autophagosome. The interaction is mediated by 15- to 20-amino-acid-long sequence motifs called LC3-interacting region (LIR) motifs that bind to the LIR docking site (LDS) of ATG8 proteins. In this review, we focus on LIR-ATG8 interactions and the soluble mammalian selective autophagy receptors. We discuss the roles of ATG8 family proteins as membrane scaffolds in autophagy and the LIR-LDS interaction and how specificity for binding to GABARAP or LC3 subfamily proteins is achieved. We also discuss atypical LIR-LDS interactions and a novel LIR-independent interaction. Recently, it has become clear that several of the soluble cargo receptors are able to recruit components of the core autophagy apparatus to aid in assembling autophagosome formation at the site of cargo sequestration. A model on phagophore recruitment and expansion on a selective autophagy receptor-coated cargo incorporating the latest findings is presented.