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Targeting the PI5P4K Lipid Kinase Family in Cancer Using Covalent Inhibitors.

Cell chemical biology (2020-03-05)
Sindhu Carmen Sivakumaren, Hyeseok Shim, Tinghu Zhang, Fleur M Ferguson, Mark R Lundquist, Christopher M Browne, Hyuk-Soo Seo, Marcia N Paddock, Theresa D Manz, Baishan Jiang, Ming-Feng Hao, Pranav Krishnan, Diana G Wang, T Jonathan Yang, Nicholas P Kwiatkowski, Scott B Ficarro, James M Cunningham, Jarrod A Marto, Sirano Dhe-Paganon, Lewis C Cantley, Nathanael S Gray
ANOTACE

The PI5P4Ks have been demonstrated to be important for cancer cell proliferation and other diseases. However, the therapeutic potential of targeting these kinases is understudied due to a lack of potent, specific small molecules available. Here, we present the discovery and characterization of a pan-PI5P4K inhibitor, THZ-P1-2, that covalently targets cysteines on a disordered loop in PI5P4Kα/β/γ. THZ-P1-2 demonstrates cellular on-target engagement with limited off-targets across the kinome. AML/ALL cell lines were sensitive to THZ-P1-2, consistent with PI5P4K's reported role in leukemogenesis. THZ-P1-2 causes autophagosome clearance defects and upregulation in TFEB nuclear localization and target genes, disrupting autophagy in a covalent-dependent manner and phenocopying the effects of PI5P4K genetic deletion. Our studies demonstrate that PI5P4Ks are tractable targets, with THZ-P1-2 as a useful tool to further interrogate the therapeutic potential of PI5P4K inhibition and inform drug discovery campaigns for these lipid kinases in cancer metabolism and other autophagy-dependent disorders.

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Sigma-Aldrich
Anti-TFEB antibody produced in rabbit, affinity isolated antibody
Sigma-Aldrich
Anti-PIKFYVE Antibody, clone R159.4.3C9, clone R159.4.3C9, from mouse