| Literature DB >> 30305341 |
Takeshi Hisamatsu1, Michael McGuire1, Sherry Y Wu1, Rajesha Rupaimoole1, Sunila Pradeep1,2, Emine Bayraktar1, Kyunghee Noh1,3, Wei Hu1, Jean M Hansen1, Yasmin Lyons1, Kshipra M Gharpure1, Archana S Nagaraja1, Lingegowda S Mangala1,4, Takashi Mitamura1, Cristian Rodriguez-Aguayo5, Young Gyu Eun6, Johnathon Rose5, Geoffrey Bartholomeusz5, Cristina Ivan4,5, Ju-Seog Lee6, Koji Matsuo7, Michael Frumovitz1, Kwong K Wong1, Gabriel Lopez-Berestein4,5, Anil K Sood8,4,9.
Abstract
For mucinous ovarian cancer (MOC), standard platinum-based therapy is largely ineffective. We sought to identify possible mechanisms of oxaliplatin resistance of MOC and develop strategies to overcome this resistance. A kinome-based siRNA library screen was carried out using human MOC cells to identify novel targets to enhance the efficacy of chemotherapy. In vitro and in vivo validations of antitumor effects were performed using mouse MOC models. Specifically, the role of PRKRA/PACT in oxaliplatin resistance was interrogated. We focused on PRKRA, a known activator of PKR kinase, and its encoded protein PACT because it was one of the five most significantly downregulated genes in the siRNA screen. In orthotopic mouse models of MOC, we observed a significant antitumor effect of PRKRA siRNA plus oxaliplatin. In addition, expression of miR-515-3p was regulated by PACT-Dicer interaction, and miR-515-3p increased the sensitivity of MOC to oxaliplatin. Mechanistically, miR-515-3p regulated chemosensitivity, in part, by targeting AXL. The PRKRA/PACT axis represents an important therapeutic target in MOC to enhance sensitivity to oxaliplatin. ©2018 American Association for Cancer Research.Entities:
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Year: 2018 PMID: 30305341 PMCID: PMC6318044 DOI: 10.1158/1535-7163.MCT-17-1050
Source DB: PubMed Journal: Mol Cancer Ther ISSN: 1535-7163 Impact factor: 6.261