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Linkage-specific deubiquitylation by OTUD5 defines an embryonic pathway intolerant to genomic variation

Authors :
Sander Pajusalu
Inga Talvik
Raymond Y. Wang
Daniel L. Kastner
Achim Werner
Mohammed Abul Basar
Precilla D'Souza
Katrin Õunap
Yutaka Nishimura
Johji Inazawa
Ken Saida
Ellen Macnamara
David B. Beck
Anthony J. Asmar
Kristin W. Barañano
Hirotsugu Oda
Marlies Kempers
Weiyi Mu
Naomichi Matsumoto
Joann Bodurtha
Tomoki Kosho
Joyce J. Thompson
Pedro P. Rocha
Ivona Aksentijevich
Apratim Mitra
Magdalena Walkiewicz
Tomoko Tamada
Ryan K. Dale
Satoshi Okada
Daniela Tiaki Uehara
Noriko Miyake
Cynthia J. Tifft
Source :
Science Advances, 7, 4, Science Advances, Science Advances, 7
Publication Year :
2021

Abstract

Disease-causing mutations in a linkage-specific deubiquitylase provide insights into chromatin remodeling during embryogenesis.<br />Reversible modification of proteins with linkage-specific ubiquitin chains is critical for intracellular signaling. Information on physiological roles and underlying mechanisms of particular ubiquitin linkages during human development are limited. Here, relying on genomic constraint scores, we identify 10 patients with multiple congenital anomalies caused by hemizygous variants in OTUD5, encoding a K48/K63 linkage–specific deubiquitylase. By studying these mutations, we find that OTUD5 controls neuroectodermal differentiation through cleaving K48-linked ubiquitin chains to counteract degradation of select chromatin regulators (e.g., ARID1A/B, histone deacetylase 2, and HCF1), mutations of which underlie diseases that exhibit phenotypic overlap with OTUD5 patients. Loss of OTUD5 during differentiation leads to less accessible chromatin at neuroectodermal enhancers and aberrant gene expression. Our study describes a previously unidentified disorder we name LINKED (LINKage-specific deubiquitylation deficiency–induced Embryonic Defects) syndrome and reveals linkage-specific ubiquitin cleavage from chromatin remodelers as an essential signaling mode that coordinates chromatin remodeling during embryogenesis.

Details

ISSN :
23752548
Database :
OpenAIRE
Journal :
Science Advances, 7, 4, Science Advances, Science Advances, 7
Accession number :
edsair.doi.dedup.....685f6090f52ead44cd34ca0941bfa4a1