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Systemic Toxicity Reported for CDK8/19 Inhibitors CCT251921 and MSC2530818 Is Not Due to Target Inhibition.

Cells. 2019; 
Chen M, Li J, Liang J, Thompson ZS, Kathrein K, Broude EV, Roninson IB.
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Molecular Biology Tools … Microscopic examination was carried out by Olympus CKX41 Inverted Phase Contrast Microscope and the cell images were captured and processed with CellSens standard software. Human recombinant TNFα (Z00404-50) was obtained from GenScript (Piscataway, NJ, USA) … Get A Quote

摘要

CDK8/19 kinases, which mediate transcriptional reprogramming, have become an active target for cancer drug discovery. Several small-molecule CDK8/19 inhibitors showed in vivo efficacy and two have entered clinical trials, with no significant toxicities reported. However, Clarke et al. (eLife 2016; 5; e20722) found severe systemic toxicity associated with two potent CDK8/19 inhibitors, Cmpd3 (CCT251921) and Cmpd4 (MSC2530818), and suggested that their toxicity was due to on-target effects. Here, we compared five CDK8/19 inhibitors: Cmpd3, Cmpd4, Senexin B, 16-didehydro-cortistatin A (dCA) and 15w, in different assays. Only Cmpd4 showed striking toxicity in developing zebrafish. In cell-based assays for CDK8 and ... More

关键词

CDK19; CDK8; STAT1 serine phosphorylation; kinome profiling; zebrafish toxicity assays