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Phenotype-Led Identification of IL-10 Upregulators in Human CD4+ T‑cells and Elucidation of Their Pharmacology as Highly Selective CDK8/CDK19 Inhibitors

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Figshare2025-01-09 更新2026-04-28 收录
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https://figshare.com/articles/dataset/Phenotype-Led_Identification_of_IL-10_Upregulators_in_Human_CD4_sup_sup_T_cells_and_Elucidation_of_Their_Pharmacology_as_Highly_Selective_CDK8_CDK19_Inhibitors/28171264
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Therapeutics promoting the endogenous production of IL-10 have the potential to restore homeostasis in inflammatory disorders such as inflammatory bowel disease (IBD). Here we describe the identification of a series of IL-10 upregulators based on a pyrimidyl-piperidine scaffold through a high throughput phenotypic CD4+ T-cell multiplex assay. In vitro optimization of the initial hit yielded a lead with good potency and an in vitro clearance profile, compound 3–7, which additionally demonstrated efficacy in a murine endotoxin challenge PK–PD mechanistic model. Target deconvolution efforts identified compound 3–7 as a highly selective CDK8/19 inhibitor, and crystallographic studies unveiled its binding mode to the CDK8/Cyclin-C complex, characterized by an unusual water-mediated hydrogen bond to the kinase hinge region.
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2025-01-09
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