Oligomerization of Selective Autophagy Receptors for the Targeting and Degradation of Protein Aggregates
Wenjun Chen, Tianyun Shen, Lijun Wang, Kefeng Lu
Abstract
The selective targeting and disposal of solid protein aggregates are essential for cells to maintain protein homoeostasis. Autophagy receptors including p62, NBR1, Cue5/TOLLIP (CUET), and Tax1-binding protein 1 (TAX1BP1) proteins function in selective autophagy by targeting ubiquitinated aggregates through ubiquitin-binding domains. Here, we summarize previous beliefs and recent findings on selective receptors in aggregate autophagy. Since there are many reviews on selective autophagy receptors, we focus on their oligomerization, which enables receptors to function as pathway determinants and promotes phase separation.
Topics & Concepts
AutophagyReceptorUbiquitinCell biologyProtein aggregationProtein degradationG protein-coupled receptorFunction (biology)ChemistryBiologyBiochemistryApoptosisGeneAutophagy in Disease and TherapyStudies on Chitinases and ChitosanasesEndoplasmic Reticulum Stress and Disease