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BI-9564
CAS No. 1883429-22-8
BI-9564 ( BI 9564 | BI9564 )
产品货号. M12927 CAS No. 1883429-22-8
BI-9564 (BI9564) 是一种有效、选择性、细胞渗透性且无细胞毒性的 BRD9 bromodomain 抑制剂,IC50 为 75 nM,Kd <20 nM。
纯度: >98% (HPLC)
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规格 | 价格/人民币 | 库存 | 数量 |
5MG | ¥381 | 有现货 |
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10MG | ¥721 | 有现货 |
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25MG | ¥1523 | 有现货 |
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50MG | ¥2900 | 有现货 |
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100MG | ¥4253 | 有现货 |
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200MG | 获取报价 | 有现货 |
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500MG | 获取报价 | 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BI-9564
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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BI-9564 (BI9564) 是一种有效、选择性、细胞渗透性且无细胞毒性的 BRD9 bromodomain 抑制剂,IC50 为 75 nM,Kd <20 nM。
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产品描述BI-9564? (BI9564) is a potent, selective, cell-permeable and noncytotoxic BRD9 bromodomain inhibitor with IC50 of 75 nM, Kd of <20 nM; displays 45-fold selectiveity over BRD7, and >5,000-fold over BRD4-BD1, BRD4-BD2, and BRD2-BD1; blocks EOL-1 cell proliferation with EC50 of 0.8 uM, and displays antitumor activity in an AML xenograft model.
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体外实验BI-9564 (<5 μM) shows no activity against 324 kinases, and at 10 μM, an inhibition >40% is observed for only 2 out of 55 GPCRs. BI-9564 has antiproliferative effect on human acute myeloid eosinophilic leukemia cell line EOL-1, with EC50 of 800 nM. BI-9564 shows Kd of 73 nM for BRD7, and is >10-fold more selective for BRD9 over the highly homologues bromodomain BRD7, which has been implied as a tumor suppressor and is down-regulated in cancer cells.
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体内实验BI-9564 (180 mg/kg, p.o.) shows attractive ADME/PK profiles for in vivo proof-of-concept studies. BI-9564 results in a modest but significant additional survival benefit of 2 days compared to survival of the control group in a xenograft model of human AML.
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同义词BI 9564 | BI9564
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通路Chromatin/Epigenetic
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靶点Bromodomain
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受体BRD7|BRD9|CECR2
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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 Number1883429-22-8
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分子量353.4149
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分子式C20H23N3O3
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纯度>98% (HPLC)
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溶解度DMSO: 7.2 mg/mL (Need warming)
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SMILESO=C1N(C)C=C(C2=CC(OC)=C(CN(C)C)C=C2OC)C3=CC=NC=C13
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化学全称4-(4-((dimethylamino)methyl)-2,5-dimethoxyphenyl)-2-methyl-2,7-naphthyridin-1(2H)-one
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. Martin LJ, et al. J Med Chem. 2016 May 26;59(10):4462-75.
2. Kr?mer KF, et al. Int J Mol Sci. 2017 Jul 16;18(7). pii: E1537.