| Literature DB >> 32071169 |
Alison M Kurimchak1, Carlos Herrera-Montávez1, Jennifer Brown1, Katherine J Johnson1,2, Valerie Sodi3, Nishi Srivastava1, Vikas Kumar1, Safoora Deihimi1, Shane O'Brien3, Suraj Peri4, Gina M Mantia-Smaldone5, Angela Jain5, Ryan M Winters6, Kathy Q Cai7, Jonathan Chernoff1, Denise C Connolly3, James S Duncan8.
Abstract
High-grade serous ovarian carcinoma (HGSOC) is the most lethal gynecological cancer with few effective, targeted therapies. HGSOC tumors exhibit genomic instability with frequent alterations in the protein kinome; however, only a small fraction of the kinome has been therapeutically targeted in HGSOC. Using multiplexed inhibitor beads and mass spectrometry, we mapped the kinome landscape of HGSOC tumors from patients and patient-derived xenograft models. The data revealed a prevalent signature consisting of established HGSOC driver kinases, as well as several kinases previously unexplored in HGSOC. Loss-of-function analysis of these kinases in HGSOC cells indicated MRCKA (also known as CDC42BPA) as a putative therapeutic target. Characterization of the effects of MRCKA knockdown in established HGSOC cell lines demonstrated that MRCKA was integral to signaling that regulated the cell cycle checkpoint, focal adhesion, and actin remodeling, as well as cell migration, proliferation, and survival. Moreover, inhibition of MRCKA using the small-molecule BDP9066 decreased cell proliferation and spheroid formation and induced apoptosis in HGSOC cells, suggesting that MRCKA may be a promising therapeutic target for the treatment of HGSOC.Entities:
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Year: 2020 PMID: 32071169 PMCID: PMC7294993 DOI: 10.1126/scisignal.aax8238
Source DB: PubMed Journal: Sci Signal ISSN: 1945-0877 Impact factor: 8.192