DUX4-induced HSATII transcription causes KDM2A/B–PRC1 nuclear foci and impairs DNA damage response-Reference-Cited by-同舟云学术

DUX4-induced HSATII transcription causes KDM2A/B–PRC1 nuclear foci and impairs DNA damage response

Published:2024-03-07 Issue:5 Volume:223 Page:
ISSN:0021-9525
Container-title:Journal of Cell Biology
language:en
Short-container-title:

Author:

Arends Tessa¹^ORCID,Tsuchida Hiroshi²^ORCID,Adeyemi Richard O.²^ORCID,Tapscott Stephen J.¹³⁴^ORCID

Affiliation:

1. Fred Hutchinson Cancer Center 1 Human Biology Division, , Seattle, WA, USA

2. Fred Hutchinson Cancer Center 2 Basic Sciences Division, , Seattle, WA, USA

3. Fred Hutchinson Cancer Center 3 Clinical Research Division, , Seattle, WA, USA

4. University of Washington 4 Department of Neurology, , Seattle, WA, USA

Abstract

Polycomb repressive complexes regulate developmental gene programs, promote DNA damage repair, and mediate pericentromeric satellite repeat repression. Expression of pericentromeric satellite repeats has been implicated in several cancers and diseases, including facioscapulohumeral dystrophy (FSHD). Here, we show that DUX4-mediated transcription of HSATII regions causes nuclear foci formation of KDM2A/B–PRC1 complexes, resulting in a global loss of PRC1-mediated monoubiquitination of histone H2A. Loss of PRC1-ubiquitin signaling severely impacts DNA damage response. Our data implicate DUX4-activation of HSATII and sequestration of KDM2A/B–PRC1 complexes as a mechanism of regulating epigenetic and DNA repair pathways.

Funder

Fred Hutch

National Institutes of Health

National Institutes of Arthritis and Musculoskeletal and Skin Diseases

National Cancer Institute

Friends of FSH Research

Ovarian Cancer Research Alliance

National Institute of General Medical Sciences

University of Washington

Seattle Children’s Cancer Consortium

Publisher

Rockefeller University Press