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Onvansertib,1034616-18-6

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  • ¥295 - 4900
  • MedChemExpress(MCE)已认证
  • 美国
  • HY-15828
  • 2025年12月05日
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    • 详细信息
    • 询价记录
    • 技术资料
    • 保存条件

      Powder: -20°C, 3 years; 4°C, 2 years.In solvent: -80°C, 6 months; -20°C, 1 month.

    • 英文名

      NMS-1286937; NMS-P937

    • 库存

      货期:1-2天

    • 供应商

      MedChemExpress LLC

    • CAS号

      1034616-18-6

    • 规格

      10 mM * 1 mL/1 mg/5 mg/10 mg/50 mg/100 mg

    规格:10 mM * 1 mL产品价格:¥762.0
    规格:1 mg产品价格:¥295.0
    规格:5 mg产品价格:¥650.0
    规格:10 mg产品价格:¥1000.0
    规格:50 mg产品价格:¥2600.0
    规格:100 mg产品价格:¥4900.0

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    Onvansertib

    CAS No. : 1034616-18-6

    MCE 国际站:Onvansertib

    产品活性:nMS-1286937 是一种有效、高选择性、可口服的 PLK1 抑制剂,IC50 值为 2 nM。

    研究领域:Cell Cycle/DNA Damage  |  Apoptosis

    作用靶点:Polo-like Kinase (PLK)  |  Apoptosis

    In Vitro: NMS-1286937 is a potent, selective and orally available PLK1 inhibitor, with IC50 of 2 nM. NMS-1286937 also shows inhibitory activities against FLT3, MELK, and CK2, with IC50s of 510, 744, and 826 nM, respectively. NMS-P937 possesses a pure ATP competitive mechanism with a reversible dissociation and no time dependency. NMS-P937 (10 μM) is selective with a marginal activity of 48% and 40% inhibition on PLK2 and PLK3, respectively. NMS-P937 shows antiproliferative activity against a panel of 137 cell lines, with IC50 values of below 100 nM for 60 of 137 cell lines and higher than 1 μM for only 9 of 137 cell lines. NMS-P937 shows cytotoxic activity against AmL-NS8 cells with IC50 of 36 nM.

    In Vivo: NMS-1286937 (45 mg/kg, i.v.) shows a good tumor growth inhibition with acceptable and reversible body weight loss in CD1 nu/nu mice xenografted with human HCT116 colon adenocarcinoma cells. NMS-1286937 (60 mg/kg, p.o.) also inhibits the growth of tumor on HCT116 xenograft model. NMS-P937 (45 mg/kg, i.v.or 60 mg/kg, p.o) inhibits tumor growth to a comparable degree (TGI, 83% and 79% intravenously and orally, respectively) in HCT116-bearing mice. The combination of NMS-P937 (120 mg/kg given for 4 cycles of 2 consecutive days with 10-day rest) and cytarabine (75 mg/kg for 4 cycles of 5 consecutive days with 7-day rest) in the disseminated leukemia model AmL-PS is well tolerated and clearly showed increased mice survival. NMS-P937 (60 mg/kg bid os per day over 2 days with a 5 day rest) shows good efficacy compared to standard therapies, with a significant increase in median survival time (MST) in the established disease setting.

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