Small Molecule Inhibitors of Phospholipase C from a Novel High-throughput Screen |
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| Authors: | Weigang Huang Matthew Barrett Nicole Hajicek Stephanie Hicks T Kendall Harden John Sondek Qisheng Zhang |
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| Institution: | From the ‡Division of Chemical Biology and Medicinal Chemistry and ;§Department of Pharmacology, University of North Carolina, Chapel Hill, North Carolina 27599 |
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| Abstract: | Phospholipase C (PLC) isozymes are important signaling molecules, but few small molecule modulators are available to pharmacologically regulate their function. With the goal of developing a general approach for identification of novel PLC inhibitors, we developed a high-throughput assay based on the fluorogenic substrate reporter WH-15. The assay is highly sensitive and reproducible: screening a chemical library of 6280 compounds identified three novel PLC inhibitors that exhibited potent activities in two separate assay formats with purified PLC isozymes in vitro. Two of the three inhibitors also inhibited G protein-coupled receptor-stimulated PLC activity in intact cell systems. These results demonstrate the power of the high-throughput assay for screening large collections of small molecules to identify novel PLC modulators. Potent and selective modulators of PLCs will ultimately be useful for dissecting the roles of PLCs in cellular processes, as well as provide lead compounds for the development of drugs to treat diseases arising from aberrant phospholipase activity. |
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| Keywords: | High-throughput Screening (HTS) Inositol 1 4 5-Trisphosphate Phosphatidylinositol Phospholipase C Small Molecules |
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