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HERC3 facilitates ERAD of select membrane proteins by recognizing membrane-spanning domains

Yuka Kamada, Yuko Ohnishi, Chikako Nakashima, Aika Fujii, Mana Terakawa, Ikuto Hamano, Uta Nakayamada, Saori Katoh, N Hirata, H Tateishi, Ryosuke Fukuda, Hirotaka Takahashi, Gergely L. Lukács, Tsukasa Okiyoneda

2024The Journal of Cell Biology12 citationsDOIOpen Access PDF

Abstract

Aberrant proteins located in the endoplasmic reticulum (ER) undergo rapid ubiquitination by multiple ubiquitin (Ub) E3 ligases and are retrotranslocated to the cytosol as part of the ER-associated degradation (ERAD). Despite several ERAD branches involving different Ub E3 ligases, the molecular machinery responsible for these ERAD branches in mammalian cells remains not fully understood. Through a series of multiplex knockdown/knockout experiments with real-time kinetic measurements, we demonstrate that HERC3 operates independently of the ER-embedded ubiquitin ligases RNF5 and RNF185 (RNF5/185) to mediate the retrotranslocation and ERAD of misfolded CFTR. While RNF5/185 participates in the ERAD process of both misfolded ABCB1 and CFTR, HERC3 uniquely promotes CFTR ERAD. In vitro assay revealed that HERC3 directly interacts with the exposed membrane-spanning domains (MSDs) of CFTR but not with the MSDs embedded in liposomes. Therefore, HERC3 could play a role in the quality control of MSDs in the cytoplasm and might be crucial for the ERAD pathway of select membrane proteins.

Topics & Concepts

Endoplasmic-reticulum-associated protein degradationUbiquitinEndoplasmic reticulumCell biologyUbiquitin ligaseMembrane proteinDeubiquitinating enzymeCytoplasmUbiquitin-Protein LigasesCytosolBiologyChemistryBiochemistryUnfolded protein responseMembraneGeneEnzymeCystic Fibrosis Research AdvancesEndoplasmic Reticulum Stress and DiseaseLysosomal Storage Disorders Research
HERC3 facilitates ERAD of select membrane proteins by recognizing membrane-spanning domains | Litcius