| Literature DB >> 31006538 |
Haruka Chino1, Tomohisa Hatta2, Tohru Natsume2, Noboru Mizushima3.
Abstract
Certain proteins and organelles can be selectively degraded by autophagy. Typical substrates and receptors of selective autophagy have LC3-interacting regions (LIRs) that bind to autophagosomal LC3 and GABARAP family proteins. Here, we performed a differential interactome screen using wild-type LC3B and a LIR recognition-deficient mutant and identified TEX264 as a receptor for autophagic degradation of the endoplasmic reticulum (ER-phagy). TEX264 is an ER protein with a single transmembrane domain and a LIR motif. TEX264 interacts with LC3 and GABARAP family proteins more efficiently and is expressed more ubiquitously than previously known ER-phagy receptors. ER-phagy is profoundly blocked by deletion of TEX264 alone and almost completely by additional deletion of FAM134B and CCPG1. A long intrinsically disordered region of TEX264 is required for its ER-phagy receptor function to bridge the gap between the ER and autophagosomal membranes independently of its amino acid sequence. These results suggest that TEX264 is a major ER-phagy receptor.Entities:
Keywords: ER-phagy; intrinsically disordered region; organellar contact site; selective autophagy
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Year: 2019 PMID: 31006538 DOI: 10.1016/j.molcel.2019.03.033
Source DB: PubMed Journal: Mol Cell ISSN: 1097-2765 Impact factor: 17.970