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A Ubiquitination Cascade Regulating the Integrated Stress Response and Survival in Carcinomas.

Authors :
Cervia LD
Shibue T
Borah AA
Gaeta B
He L
Leung L
Li N
Moyer SM
Shim BH
Dumont N
Gonzalez A
Bick NR
Kazachkova M
Dempster JM
Krill-Burger JM
Piccioni F
Udeshi ND
Olive ME
Carr SA
Root DE
McFarland JM
Vazquez F
Hahn WC
Source :
Cancer discovery [Cancer Discov] 2023 Mar 01; Vol. 13 (3), pp. 766-795.
Publication Year :
2023

Abstract

Systematic identification of signaling pathways required for the fitness of cancer cells will facilitate the development of new cancer therapies. We used gene essentiality measurements in 1,086 cancer cell lines to identify selective coessentiality modules and found that a ubiquitin ligase complex composed of UBA6, BIRC6, KCMF1, and UBR4 is required for the survival of a subset of epithelial tumors that exhibit a high degree of aneuploidy. Suppressing BIRC6 in cell lines that are dependent on this complex led to a substantial reduction in cell fitness in vitro and potent tumor regression in vivo. Mechanistically, BIRC6 suppression resulted in selective activation of the integrated stress response (ISR) by stabilization of the heme-regulated inhibitor, a direct ubiquitination target of the UBA6/BIRC6/KCMF1/UBR4 complex. These observations uncover a novel ubiquitination cascade that regulates ISR and highlight the potential of ISR activation as a new therapeutic strategy.<br />Significance: We describe the identification of a heretofore unrecognized ubiquitin ligase complex that prevents the aberrant activation of the ISR in a subset of cancer cells. This provides a novel insight on the regulation of ISR and exposes a therapeutic opportunity to selectively eliminate these cancer cells. See related commentary Leli and Koumenis, p. 535. This article is highlighted in the In This Issue feature, p. 517.<br /> (©2022 The Authors; Published by the American Association for Cancer Research.)

Details

Language :
English
ISSN :
2159-8290
Volume :
13
Issue :
3
Database :
MEDLINE
Journal :
Cancer discovery
Publication Type :
Academic Journal
Accession number :
36576405
Full Text :
https://doi.org/10.1158/2159-8290.CD-22-1230