| Literature DB >> 35413118 |
Thapi D Rao1,2, Mengyao Xu3, Stephanie Eng1,4, Guangli Yang5, Robin Manson1, Nestor Rosales1, Raj Kumar3, Irva E Veillard3, Qin Zhou6, Alexia Iasonos6, Ouathek Ouerfelli1, Hakim Djaballah1,7, David R Spriggs1,3, Oladapo O Yeku3.
Abstract
Significant strides have been made in the development of precision therapeutics for cancer. Aberrantly expressed glycoproteins represent a potential avenue for therapeutic development. The MUC16/CA125 glycoprotein serves as a biomarker of disease and a driver of malignant transformation in epithelial ovarian cancer. Previously, we demonstrated a proof-of-principle approach to selectively targeting MUC16+ cells. In this report, we performed a synthetic lethal kinase screen using a human kinome RNAi library and identified key pathways preferentially targetable in MUC16+ cells using isogenic dual-fluorescence ovarian cancer cell lines. Using a separate approach, we performed high-content small-molecule screening of six different libraries of 356,982 compounds for MUC16/CA125-selective agents and identified lead candidates that showed preferential cytotoxicity in MUC16+ cells. Compounds with differential activity were selected and tested in various other ovarian cell lines or isogenic pairs to identify lead compounds for structure-activity relationship (SAR) selection. Lead siRNA and small-molecule inhibitor candidates preferentially inhibited invasion of MUC16+ cells in vitro and in vivo, and we show that this is due to decreased activation of MAPK, and non-receptor tyrosine kinases. Taken together, we present a comprehensive screening approach to the development of a novel class of MUC16-selective targeted therapeutics and identify candidates suitable for further clinical development. ©2022 American Association for Cancer Research.Entities:
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Year: 2022 PMID: 35413118 PMCID: PMC9081202 DOI: 10.1158/1535-7163.MCT-21-0572
Source DB: PubMed Journal: Mol Cancer Ther ISSN: 1535-7163 Impact factor: 6.009