| Literature DB >> 31669203 |
Reem Ali1, Muslim Alabdullah2, Adel Alblihy1, Islam Miligy3, Katia A Mesquita1, Stephen Yt Chan4, Paul Moseley4, Emad A Rakha3, Srinivasan Madhusudan5.
Abstract
PARP1 inhibitor (Niraparib, Olaparib, Rucaparib) maintenance therapy improves progression-free survival in platinum sensitive sporadic epithelial ovarian cancers. However, biomarkers of response to PARPi therapy is yet to be clearly defined. XRCC1, a scaffolding protein, interacts with PARP1 during BER and SSBR. In a large clinical cohort of 525 sporadic ovarian cancers, high XRCC1 or high PARP1 protein levels was not only associated with aggressive phenotypes but was also significantly linked with poor progression-free survival (p = 0.048 & p = 0.001 respectively) and poor ovarian cancer-specific survival (p = 0.020 & p = 0.008 respectively). Pre-clinically, Olaparib and Talazoparib therapy were selectively toxic in XRCC1 deficient or knock-out platinum sensitive ovarian cancer cells in 2D and 3D models. Increased sensitivity was associated with DNA double-strand break accumulation, cell cycle arrest and apoptotic cell accumulation. We conclude that XRCC1 deficiency predicts sensitivity to PARP inhibitor therapy. PARP1 targeting is a promising new approach in XRCC1 deficient ovarian cancers.Entities:
Keywords: Ovarian cancer; PARP; Synthetic lethality; XRCC1
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Year: 2019 PMID: 31669203 DOI: 10.1016/j.canlet.2019.10.035
Source DB: PubMed Journal: Cancer Lett ISSN: 0304-3835 Impact factor: 8.679