Computational Cell Cycle Profiling of Cancer Cells for Prioritizing FDA-Approved Drugs with Repurposing Potential

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作者
Yu-Chen Lo
Silvia Senese
Bryan France
Ankur A. Gholkar
Robert Damoiseaux
Jorge Z. Torres
机构
[1] Department of Chemistry and Biochemistry,
[2] University of California,undefined
[3] Program in Bioengineering,undefined
[4] University of California,undefined
[5] Department of Molecular and Medical Pharmacology,undefined
[6] California NanoSystems Institute,undefined
[7] University of California,undefined
[8] Jonsson Comprehensive Cancer Center,undefined
[9] University of California,undefined
[10] Molecular Biology Institute,undefined
[11] University of California,undefined
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Discovery of first-in-class medicines for treating cancer is limited by concerns with their toxicity and safety profiles, while repurposing known drugs for new anticancer indications has become a viable alternative. Here, we have developed a new approach that utilizes cell cycle arresting patterns as unique molecular signatures for prioritizing FDA-approved drugs with repurposing potential. As proof-of-principle, we conducted large-scale cell cycle profiling of 884 FDA-approved drugs. Using cell cycle indexes that measure changes in cell cycle profile patterns upon chemical perturbation, we identified 36 compounds that inhibited cancer cell viability including 6 compounds that were previously undescribed. Further cell cycle fingerprint analysis and 3D chemical structural similarity clustering identified unexpected FDA-approved drugs that induced DNA damage, including clinically relevant microtubule destabilizers, which was confirmed experimentally via cell-based assays. Our study shows that computational cell cycle profiling can be used as an approach for prioritizing FDA-approved drugs with repurposing potential, which could aid the development of cancer therapeutics.
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