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NR1D1 recruitment to sites of DNA damage inhibits repair and is associated with chemosensitivity of breast cancer

Cited 37 time in Web of Science Cited 33 time in Scopus
Authors

Ka, Na-Lee; Na, Tae-Young; Na, Hyelin; Lee, Min-Ho; Park, Han-Su; Hwang, Sewon; Kim, Il Yong; Seong, Je Kyung; Lee, Mi-Ock

Issue Date
2017-05
Publisher
American Association for Cancer Research
Citation
Cancer Research, Vol.77 No.9, pp.2453-2463
Abstract
DNA repair capacity is critical for survival of cancer cells upon therapeuticDNAdamage and thus is an important determinant of susceptibility to chemotherapy in cancer patients. In this study, we identified a novel function of nuclear receptor NR1D1 in DNA repair, which enhanced chemosensitivity in breast cancer cells. NR1D1 inhibited both nonhomologous end joining and homologous recombination double-strand breaks repair, and delayed the clearance of gamma H2AX DNA repair foci that formed after treatment of doxorubicin. PARylation of NR1D1 by PARP1 drove its recruitment to damaged DNA lesions. Deletion of the ligand binding domain of NR1D1 that interacted with PARP1, or treatment of 6-(5H)-phenanthridinone, an inhibitor of PARP1, sup-pressed the recruitment of NR1D1 to DNA damaged sites, indicating PARylation as a critical step for the NR1D1 recruitment. NR1D1 inhibited recruitment of the components of DNA damage response complex such as SIRT6, pNBS1, and BRCA1 to DNA lesions. Downregulation of NR1D1 in MCF7 cells resulted in resistance to doxorubicin, both in vitro and in vivo. Analysis of four public patient data sets indicated that NR1D1 expression correlates positively with clinical outcome in breast cancer patients who received chemotherapy. Our findings suggest that NR1D1 and its ligands provide therapeutic options that could enhance the outcomes of chemotherapy in breast cancer patients.
ISSN
0008-5472
URI
https://hdl.handle.net/10371/206722
DOI
https://doi.org/10.1158/0008-5472.CAN-16-2099
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