UBE2O Remodels the Proteome During Terminal Erythroid Differentiation

Overview

Journal Science

Specialty Science

Date 2017 Aug 5

PMID 28774900

Citations 80

Authors

Anthony T Nguyen

Miguel A Prado

Paul J Schmidt

Anoop K Sendamarai

Joshua T Wilson-Grady

Mingwei Min

Dean R Campagna

Geng Tian

Yuan Shi

Verena Dederer

Mona Kawan

Nathalie Kuehnle

Joao A Paulo

Yu Yao

Mitchell J Weiss

Monica J Justice

Steven P Gygi

Mark D Fleming

Daniel Finley

Affiliations

Soon will be listed here.

Abstract

During terminal differentiation, the global protein complement is remodeled, as epitomized by erythrocytes, whose cytosol is ~98% globin. The erythroid proteome undergoes a rapid transition at the reticulocyte stage; however, the mechanisms driving programmed elimination of preexisting cytosolic proteins are unclear. We found that a mutation in the murine gene, which encodes a ubiquitin-conjugating enzyme induced during erythropoiesis, results in anemia. Proteomic analysis suggested that UBE2O is a broad-spectrum ubiquitinating enzyme that remodels the erythroid proteome. In particular, ribosome elimination, a hallmark of reticulocyte differentiation, was defective in mutants. UBE2O recognized ribosomal proteins and other substrates directly, targeting them to proteasomes for degradation. Thus, in reticulocytes, the induction of ubiquitinating factors may drive the transition from a complex to a simple proteome.

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