| Literature DB >> 33353557 |
Rahel Polaczek1, Peter Schürmann1, Lisa-Marie Speith1, Robert Geffers2, Matthias Dürst3, Peter Hillemanns1, Tjoung-Won Park-Simon1, Clemens Liebrich4, Thilo Dörk5.
Abstract
Epithelial ovarian carcinoma (EOC) is a genetically heterogeneous disease that is partly driven by molecular defects in mismatch repair (MMR) or homology-directed DNA repair (HDR). Ribonuclease H2 serves to remove mis-incorporated ribonucleotides from DNA which alleviates HDR mechanisms and guides the MMR machinery. Although Ribonuclease H2 has been implicated in cancer, the role of germline variants for ovarian cancer is unknown. In the present case-control study, we sequenced the coding and flanking untranslated regions of the RNASEH2A, RNASEH2B and RNASEH2C genes, encoding all three subunits of Ribonuclease H2, in a total of 602 German patients with EOC and of 940 healthy females from the same population. We identified one patient with a truncating variant in RNASEH2B, p.C44X, resulting in a premature stop codon. This patient had high-grade serous EOC with an 8 years survival after platinum/taxane-based therapy. Subsequent analysis of TCGA data similarly showed a significantly longer progression-free survival in ovarian cancer patients with low RNASEH2B or RNASEH2C expression levels. In conclusion, loss-of-function variants in Ribonuclease H2 genes are not common predisposing factors in ovarian cancer but the possibility that they modulate therapeutic platinum response deserves further investigation.Entities:
Keywords: Epithelial ovarian carcinoma; Homologous recombination; MMR deficiency; Platinum resistance; RNase H2; Ribonucleotide excision repair
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Year: 2020 PMID: 33353557 PMCID: PMC7756920 DOI: 10.1186/s13048-020-00753-1
Source DB: PubMed Journal: J Ovarian Res ISSN: 1757-2215 Impact factor: 4.234