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Discovery of a Potent Chloroacetamide GPX4 Inhibitor with Bioavailability to Enable Target Engagement in Mice, a Potential Tool Compound for Inducing Ferroptosis In Vivo .

John T RandolphMatthew J O'ConnorFei HanCharles W HutchinsY Amy SiuMin ChoYunan ZhengJonathan A HicksonJana L MarkleyVlasios ManavesMikkel AlgireKenton A BakerAlex M ChapmanSujatha M GopalakrishnanSanjay C PanchalKelly Foster-DukeDeAnne F StolarikAnita Kempf-GroteDarby DammeierStacey FosseyQi SunChaohong SunYu ShenMichael J DartWarren M KatiAlbert LaiAri J FirestoneMichael E Kort
Published in: Journal of medicinal chemistry (2023)
Compounds that inhibit glutathione peroxidase 4 (GPX4) hold promise as cancer therapeutics in their ability to induce a form of nonapoptotic cell death called ferroptosis. Our research identified 24 , a structural analog of the potent GPX4 inhibitor RSL3, that has much better plasma stability ( t 1/2 > 5 h in mouse plasma). The bioavailability of 24 provided efficacious plasma drug concentrations with IP dosing, thus enabling in vivo studies to assess tolerability and efficacy. An efficacy study in mouse using a GPX4-sensitive tumor model found that doses of 24 up to 50 mg/kg were tolerated for 20 days but had no effect on tumor growth, although partial target engagement was observed in tumor homogenate.
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