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S81145

PF-03814735

源叶(MedMol) 99%
  • 英文名:
  • PF-03814735
  • 别名:
  • Acetamide, N-[2-[(1S,4R)-6-[[4-(cyclobutylamino)-5-(trifluoromethyl)-2-pyrimidinyl]amino]-1,2,3,4-tetrahydronaphthalen-1,4-imin-9-yl]-2-oxoethyl]-
  • CAS号:
  • 942487-16-3
  • 分子式:
  • C23H25F3N6O2
  • 分子量:
  • 474.48
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源叶(MedMol) S81145-5mg 99% ¥1250.00元 预计交期:2-3天 - - - EA 加入购物车
源叶(MedMol) S81145-10mg 99% ¥2200.00元 预计交期:2-3天 - - - EA 加入购物车
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  • 提示:详情请下载说明书。
  • 产品描述: PF-03814735 is a potent, orally available, ATP-competitive and reversible aurora A and aurora B inhibitor with IC50s of 0.8 and 0.5 nM, respectively.
  • 靶点: Aurora 1:0.8 nM (IC50);Aurora 2:5 nM (IC50);Flt-1:10 nM (IC50);FAK:22 nM (IC50);TrkA;30 nM (IC50);Met:100 nM (IC50);FGFR1:100 nM (IC50);FAK; VEGFR; FLT; Trkreceptor; AuroraKinase
  • 体内研究:
    Once-daily oral administration of PF-03814735 to mice bearing human xenograft tumors produces a reduction in phosphohistone H3 in tumors at doses that are tolerable and that result in significant inhibition of tumor growth. The combination of PF-03814735 and docetaxel in xenograft mouse tumor models shows additive tumor growth inhibition. PF-03814735 is much more effective in NCI-H82 xenografts when administered on a weekly dosing schedule at 80 mg/kg compared with a daily schedule at 15 mg/kg. PF-03814735 delayed growth by 23.5 days on the weekly schedule, which corresponds to 0.9 logs of net cell kill during the course of treatment
  • 参考文献:
    1. Jani JP, et al. PF-03814735, an orally bioavailable small molecule aurora kinase inhibitor for cancer therapy. Mol Cancer Ther. 2010 Apr;9(4):883-94. 2. Hook KE, et al. An integrated genomic approach to identify predictive biomarkers of response to the aurora kinase inhibitor PF-03814735. Mol Cancer Ther. 2012 Mar;11(3):710-9.
  • 溶解性: Soluble  in  DMSO
  • 保存条件: -20℃
  • 配置溶液浓度参考:
    1mg 5mg 10mg
    1 mM 2.108 ml 10.538 ml 21.076 ml
    5 mM 0.422 ml 2.108 ml 4.215 ml
    10 mM 0.211 ml 1.054 ml 2.108 ml
    50 mM 0.042 ml 0.211 ml 0.422 ml
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