
CP-31398 dihydrochloride
CAS No. 1217195-61-3
CP-31398 dihydrochloride ( CP31398 dihydrochloride )
产品货号. M10814 CAS No. 1217195-61-3
CP-31398 是一种小分子 p53 重激活剂,可保护 p53 免受热变性。
纯度: >98% (HPLC)






规格 | 价格/人民币 | 库存 | 数量 |
2MG | ¥356 | 有现货 |
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5MG | ¥567 | 有现货 |
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10MG | ¥940 | 有现货 |
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25MG | ¥1831 | 有现货 |
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50MG | ¥2940 | 有现货 |
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100MG | ¥4803 | 有现货 |
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200MG | ¥6828 | 有现货 |
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500MG | ¥10125 | 有现货 |
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1G | 获取报价 | 有现货 |
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生物学信息
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产品名称CP-31398 dihydrochloride
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注意事项本公司产品仅用于科研实验,不得用于人体或动物的临床与诊断
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产品简述CP-31398 是一种小分子 p53 重激活剂,可保护 p53 免受热变性。
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产品描述CP-31398 is a small molecule p53 reactivator that protects p53 from thermal denaturation, not only reactivates mutant p53 but also induces stabilization of wild type p53; shows anti-tumor activity in vivo in a transgenic UPII-SV40T mouse model of bladder transitional cell carcinoma.
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体外实验CP-31398 (36.75 μM, 16 h) induces p21 in p53-mutant cells.CP-31398 (15 μg/mL, 20 hours) could induce apoptosis and cell cycle arrest in SW480 cells. Western Blot Analysis Cell Line:Saos-2 cells expressing transfected mutant p53.Concentration:36.75 μM.Incubation Time:16 h.Result:Induction of p21 in cells expressing only mutant p53.Western Blot Analysis Cell Line:LN-18 and U87MG cells.Concentration:36 μM.Incubation Time:16 h. Result:Decreased the levels of procaspase 3 and induced cleavage of caspase 7.
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体内实验CP-31398 (100 mg/kg, orally) exhibits significant anti-tumor activity in mice models. Animal Model:Small human tumor xenografts in mice.Dosage:100 mg/kg.Administration:Orally twice daily for 7 days.Result:Suppressed A375.S2 tumor growth by -50%.
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同义词CP31398 dihydrochloride
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通路Apoptosis
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靶点MDM2-p53
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受体MDM2-p53
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研究领域Cancer
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适应症——
化学信息
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CAS Number1217195-61-3
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分子量435.39
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分子式C22H26N4O.2HCl
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纯度>98% (HPLC)
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溶解度In Vitro:?DMSO : 200 mg/mL (459.36 mM)
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SMILESCN(C)CCCNC1=C2C=CC=CC2=NC(/C=C/C3=CC=C(OC)C=C3)=N1.[H]Cl.[H]Cl
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化学全称N'-[2-[2-(4-Methoxyphenyl)ethenyl]-4-quinazolinyl]-N,N-dimethyl-1,3-propanediamine dihydrochloride
运输与储存
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储存条件(-20℃)
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运输条件With Ice Pack
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稳定性≥ 2 years
参考文献
1. Foster BA, et al. Science. 1999 Dec 24;286(5449):2507-10.
2. Madka V, et al. Neoplasia. 2013 Aug;15(8):966-74.
3. Wang W, et al. Mol Cell Biol. 2003 Mar;23(6):2171-81.
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