Phospho-Ser784-VCP Is Required for DNA Damage Response and Is Associated with Poor Prognosis of Chemotherapy-Treated Breast Cancer
Author(s) -
Cuige Zhu,
Anna Rogers,
Karama Asleh,
Jennifer R. Won,
Dongxia Gao,
Samuel Leung,
Shan Li,
Kiran Vij,
Jian Zhu,
Jason M. Held,
Zhongsheng You,
Torsten O. Nielsen,
Jieya Shao
Publication year - 2020
Publication title -
cell reports
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 6.264
H-Index - 154
eISSN - 2639-1856
pISSN - 2211-1247
DOI - 10.1016/j.celrep.2020.107745
Subject(s) - dna damage , chromatin , dna repair , proteostasis , biology , cancer research , breast cancer , phosphorylation , chromatin remodeling , cancer , microbiology and biotechnology , dna , biochemistry , genetics
Spatiotemporal protein reorganization at DNA damage sites induced by genotoxic chemotherapies is crucial for DNA damage response (DDR), which influences treatment response by directing cancer cell fate. This process is orchestrated by valosin-containing protein (VCP), an AAA+ ATPase that extracts polyubiquinated chromatin proteins and facilitates their turnover. However, because of the essential and pleiotropic effects of VCP in global proteostasis, it remains challenging practically to understand and target its DDR-specific functions. We describe a DNA-damage-induced phosphorylation event (Ser), which selectively enhances chromatin-associated protein degradation mediated by VCP and is required for DNA repair, signaling, and cell survival. These functional effects of Ser phosphorylation on DDR correlate with a decrease in VCP association with chromatin, cofactors NPL4/UFD1, and polyubiquitinated substrates. Clinically, high phospho-Ser-VCP levels are significantly associated with poor outcome among chemotherapy-treated breast cancer patients. Thus, Ser phosphorylation is a DDR-specific enhancer of VCP function and a potential predictive biomarker for chemotherapy treatments.
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