In Vitro |
MET kinase-IN-2 (compound 20j; 72 hours) inhibits U-87 MG, NIH-H460, HT-29, and MKN-45 cell lines with IC50s ranging 2.9 to 4.5 μM[1]. MET kinase-IN-2 inhibits AXL, Flt4, KDR, Mer, TEK, and TYRO3 with IC50s ranging from 16.5 to 198 nM[1].
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In Vivo |
MET kinase-IN-2 (3-37.5 mg/kg; p.o.; 7 days per week for 3 weeks) exhibits statistically significant tumor growth inhibition in the U-87 MG 24 xeograft model[1]. MET kinase-IN-2 treatment shows that the Cmax, AUC0-∞, T1/2,CL, and F% values are 1.5 µg/mL, 10.7 µg•h/mL, 4.9 hours, 0.5 L/h/kg, and F=32%, respectively[1]. Animal Model: 4-6 weeks old Female nude mice (U-87 MG xenograft model)[1] Dosage: 3, 6, 12.5, 37.5 mg/kg Administration: P.o.; 7 days per week for 3 weeks Result: Induced dose-dependent tumor growth inhibition. Animal Model: Male SD rats[1] Dosage: 5 mg/kg Administration: P.o. (Pharmacokinetic Analysis) Result: Displayed favorable overall PK profiles, with maximal plasma concentration (Cmax=1.5 µg/mL, 5-fold higher to that of IV), plasma exposure (AUC0-∞=10.7 µg•h/mL, 9.7-fold higher to that of IV), half-life (T1/2=4.9 h, 4.9-fold longer to that of IV), total clearance CL (0.5 L/h/kg; 10-fold lower to that of IV), and oral bioavailability (F=32%, 2.7-fold higher to that of IV) after oral dose of 5 mg/kg (10 mg/kg for IV).
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