Indolinone Tyrosine Kinase Inhibitors Block Kit Activation and Growth of Small Cell Lung Cancer Cells

Experimental Therapeutics

Indolinone Tyrosine Kinase Inhibitors Block Kit Activation and Growth of Small Cell Lung Cancer Cells¹

Geoffrey W. Krystal², Sittisak Honsawek, David Kiewlich, Congxin Liang, Stefan Vasile, Li Sun, Gerald McMahon and Kenneth E. Lipson

Departments of Internal Medicine [G. W. K.] and Microbiology/Immunology [G. W. K., S. H.], Virginia Commonwealth University, McGuire Veterans Affairs Medical Center, Richmond, Virginia 23249, and SUGEN, Incorporated, South San Francisco, California 94080 [D. K., C. L., S. V., L. S., G. M., K. E. L.]

Six indolinone tyrosine kinase inhibitors were characterizedfor their ability to inhibit Kit kinase and for their effectson the growth of small cell lung cancer (SCLC) cell lines. Allof the six compounds were potent inhibitors of Kit kinase ina biochemical assay. A homology model of compound binding tothe ATP binding site could account for the increased potencyobserved with the addition of a propionate moiety to the indolinonecore but not the increase observed with addition of a chloridemoiety. Although all of the compounds tested were potent inthe biochemical assay, several exhibited significantly lesspotency in cellular kinase assays. Their effects on stem cellfactor (SCF)-dependent Kit autophosphorylation and SCLC cellgrowth were also examined. Inhibition of SCF-stimulated Kitactivation and cell growth in the H526 cell line was dose-dependent.At concentrations that inhibited SCF-stimulated H526 cell growth,there was little effect on insulin-like growth factor-1-stimulatedgrowth, suggesting that these compounds exhibit reasonable selectivityfor inhibition of Kit-mediated proliferation. Higher doses ofthe compounds were needed to inhibit serum-stimulated growth.Of the six compounds examined, SU5416 and SU6597 demonstratedthe best cellular potency and, therefore, their effect on thegrowth of multiple SCLC cell lines in serum-containing mediawas examined. In addition to inhibiting proliferation, thesecompounds also induced significant cell death of several SCLCcell lines, but not of normal human diploid fibroblasts, incomplete media. These observations suggest that Kit kinase inhibitorssuch as these may offer a new approach for inhibiting Kit-mediatedproliferation of tumors such as SCLC, gastrointestinal stromaltumors, seminomas, and leukemias.

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