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Development of new tools to study membrane-anchored mammalian Atg8 proteins

Authors
Park Sang-WonJeon PureumYamasaki AkinoriLee Hye EunChoi HaneulMun Ji YoungJun Yong-WooPark Ju-HuiLee Seung-HwanLee Soo-KyeongLee You-KyungSong Hyun KyuLazarou MichaelCho Dong-HyongKomatsu MasaakiNoda Nobuo N.Jang Deok-JinLee Jin-A
Issue Date
May-2023
Publisher
TAYLOR & FRANCIS INC
Keywords
Autophagy; GABARAP; LIR motif; mammalian ATG8; RavZ protein; selective mATG8-PE delipidation
Citation
AUTOPHAGY, v.19, no.5, pp.1424 - 1443
Journal Title
AUTOPHAGY
Volume
19
Number
5
Start Page
1424
End Page
1443
URI
http://scholarworks.bwise.kr/kbri/handle/2023.sw.kbri/125
ISSN
1554-8627
Abstract
Mammals conserve multiple mammalian Atg8-family proteins (mATG8s) consisting of GABARAP (GABA type A receptor-associated protein) and MAP1LC3/LC3 (microtubule associated protein 1 light chain 3) subfamilies that tightly bind to autophagic membranes in a membrane-anchored form. These proteins are crucial for selective autophagy and recruit proteins bearing LC3-interacting region (LIR) motifs. However, because limited research tools are available, information on the specific roles of each membrane-anchored mATG8 in selective autophagy is scarce. In this study, we identified LIR motifs specific to the membrane-anchored form of each mATG8 and characterized the residues critical for their selective interaction using cell-based assays and structural analyses. We then used these selective LIR motifs to develop probes and irreversible deconjugases that targeted selective membrane-anchored mATG8s in the autophagic membrane, revealing that membrane-anchored GABARAP subfamily proteins regulate the aggrephagy of amyotrophic lateral sclerosis-linked protein aggregates. Our tools will be useful for elucidating the functional significance of each mATG8 protein on autophagic membranes in autophagy research.
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