doi: 10.1021/acsmedchemlett.3c00063.
eCollection 2023 Jul 13.
Discovery of Potent, Dual-Inhibitors of Diacylglycerol Kinases Alpha and Zeta Guided by Phenotypic Optimization
Affiliations
- PMID: 37465293
- PMCID: PMC10351048
- DOI: 10.1021/acsmedchemlett.3c00063
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Discovery of Potent, Dual-Inhibitors of Diacylglycerol Kinases Alpha and Zeta Guided by Phenotypic Optimization
ACS Med Chem Lett.
.
Abstract
We describe a phenotypic screening and optimization strategy to discover compounds that block intracellular checkpoint signaling in T-cells. We identified dual DGKα and ζ inhibitors notwithstanding the modest similarity between α and ζ relative to other DGK isoforms. Optimized compounds produced cytokine release and T-cell proliferation consistent with DGK inhibition and potentiated an immune response in human and mouse T-cells. Additionally, lead inhibitor BMS-502 demonstrated dose-dependent immune stimulation in the mouse OT-1 model, setting the stage for a drug discovery program.
© 2023 American Chemical Society.
Conflict of interest statement
The authors declare no competing financial interest.
Figures
(A)
Diacylglycerol phosphorylation. (B) TcR engagement leads to
IL2 production. DGK interrupts this pathway by depletion of DAG.
(A) Assay format using
the SEB-mediated T-cell interaction with
Raji cells to stimulate IL2 production. (B) Counter-screen without
PD-L1 presentation. .
(A) BMS-502 pharmacokinetic profile in C57 black mice.
(B) BMS-502 dose response in the OT1 model. %CD69+ T-cells = 100(CD69+ CD8s)/total CD8s in the spleen.
(C) Pharmacokinetic parameters for BMS-502.
Percent
identity of DGK isoforms in catalytic and accessory domains
grouped by type.
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