| Literature DB >> 30353615 |
Awad Jarrar1,2,3, Fiorenza Lotti1,4, Jennifer DeVecchio1, Sylvain Ferrandon1, Gerald Gantt1,2, Adam Mace1,2, Georgios Karagkounis1,2, Matthew Orloff1, Monica Venere5, Masahiro Hitomi6, Justin Lathia6,7, Jeremy N Rich1, Matthew F Kalady1,2,7,8.
Abstract
Colorectal cancer (CRC) remains a leading killer in the U.S. with resistance to treatment as the largest hurdle to cure. Colorectal cancer-initiating cells (CICs) are a self-renewing tumor population that contribute to tumor relapse. Here, we report that patient-derived CICs display relative chemoresistance compared with differentiated progeny. In contrast, conventional cell lines failed model therapeutic resistance. CICs preferentially repaired chemotherapy-induced DNA breaks, prompting us to interrogate DNA damage pathways against which pharmacologic inhibitors have been developed. We found that CICs critically depended on the key single-strand break repair mediator, poly(ADP-ribose) polymerase (PARP), to survive treatment with standard-of-care chemotherapy. Small molecule PARP inhibitors (PARPi) sensitized CICs to chemotherapy and reduced chemotherapy-treated CIC viability, self-renewal, and DNA damage repair. Although PARPi monotherapy failed to kill CICs, combined PARPi therapy with chemotherapy attenuated tumor growth in vivo. Clinical significance of PARPi for CRC patients was supported by elevated PARP levels in colorectal tumors compared with normal colon, with further increases in metastases. Collectively, our results suggest that PARP inhibition serves as a point of fragility for CICs by augmenting therapeutic efficacy of chemotherapy. Stem Cells 2019;37:42-53. © AlphaMed Press 2018.Entities:
Keywords: Cancer-initiating cells; Chemotherapy; Colon cancer; DNA repair; PARP
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Year: 2018 PMID: 30353615 DOI: 10.1002/stem.2929
Source DB: PubMed Journal: Stem Cells ISSN: 1066-5099 Impact factor: 6.277