| Literature DB >> 27753535 |
Anya Alayev1, Rachel S Salamon1, Subrata Manna1, Naomi S Schwartz1, Adi Y Berman1, Marina K Holz1,2.
Abstract
Homologous recombination (HR) is a conserved process that maintains genome stability and cell survival by repairing DNA double-strand breaks (DSBs). The RAD51-related family of proteins is involved in repair of DSBs; consequently, deregulation of RAD51 causes chromosomal rearrangements and stimulates tumorigenesis. RAD51C has been identified as a potential tumor suppressor and a breast and ovarian cancer susceptibility gene. Recent studies have also implicated estrogen as a DNA-damaging agent that causes DSBs. We found that in ERα-positive breast cancer cells, estrogen transcriptionally regulates RAD51C expression in ERα-dependent mechanism. Moreover, estrogen induces RAD51C assembly into nuclear foci at DSBs, which is a precursor to RAD51 complex recruitment to the nucleus. Additionally, disruption of ERα signaling by either anti-estrogens or siRNA prevented estrogen induced upregulation of RAD51C. We have also found an association of a worse clinical outcome between RAD51C expression and ERα status of tumors. These findings provide insight into the mechanism of genomic instability in ERα-positive breast cancer and suggest that individuals with mutations in RAD51C that are exposed to estrogen would be more susceptible to accumulation of DNA damage, leading to cancer progression.Entities:
Keywords: DNA double-strand break repair; ERα; RAD51C; breast cancer; estrogen
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Year: 2016 PMID: 27753535 PMCID: PMC5176134 DOI: 10.1080/15384101.2016.1241927
Source DB: PubMed Journal: Cell Cycle ISSN: 1551-4005 Impact factor: 4.534