CDK6/PIM1-IN-1 is a potent and balanced dualCDK6/PIM1inhibitor withIC₅₀ values of 39 and 88 nM, respectively. CDK6/PIM1-IN-1 inhibitsCDK4(IC₅₀=3.6 nM). CDK6/PIM1-IN-1 significantly inhibits acute myeloid leukemia (AML) cell proliferation, arrest cell cycle at the G1 phase, and promote cellapoptosis. CDK6/PIM1-IN-1 exhibits potent anti-AML activity^[1].

CDK6/PIM1-IN-1 (compound 51) exhibits more than 10 times selectivity over CDK1 (IC₅₀>10 μM), CDK2 (IC₅₀=2.274 μM), CDK3 (IC₅₀>10 μM), CDK5 (IC₅₀>10 μM), CDK7 (IC₅₀=393 nM), CDK9 (IC₅₀=440 nM), CDK12 (IC₅₀>10 μM), and CDK13 (IC₅₀>10 μM). CDK6/PIM1-IN-1 shows inhibitory activity against PIM2 (IC₅₀>10 μM) and PIM3 (IC₅₀=92 nM)^[1].
CDK6/PIM1-IN-1 inhibits proliferation in AML cells (K562 cell,GI₅₀=1.026 μM; HL-60 cell,GI₅₀=1.069 μM; MOLM13 cell, GI₅₀=1.362 μM)^[1].
CDK6/PIM1-IN-1 (0.5, 1, 1.5 μM) causes a G1 arrest in a dose-dependent manner in K562 and HL-60 cell lines^[1].
CDK6/PIM1-IN-1 (1, 2, 4 μM) promotes the apoptosis of K562 and HL-60 cell lines in a dose-dependent manner^[1].
CDK6/PIM1-IN-1 (0.5, 1, 1.5 μM; for 24 h) reduces p-retinoblastoma (RB) and p-BAD levels in a concentration-dependent manner. CDK6/PIM1-IN-1 decreases the PIM1 level^[1].

CDK6/PIM1-IN-1 (compound 51; orally; 60, 90 mg/kg/day; 17 days) displays more potent antitumor activity in BALB/c mice with K562 cell lines^[1].
CDK6/PIM1-IN-1 (iv; 5 mg/kg) has the t_1/2, MRT_0-∞, and AUC_0-∞ values of 9.78 h, 14.61 h, and 1153.74 h·ng/mL, respectively in Sprague–Dawley (SD) rats^[1].
CDK6/PIM1-IN-1 (po; 5 mg/kg) has the t_1/2, T_max, C_max, and AUC_0-∞of 15.81 h, 11 h, 152.31 ng/mL, and 5152.92 h·ng/mL, respectively in SD rats^[1].

473.55

C₂₅H₂₈FN₉

2677026-14-9

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