
Plx-4032
CAS No. 1029872-54-5
Plx-4032 ( Vemurafenib )
产品货号. M22533 CAS No. 1029872-54-5
PLX-4032是一种小分子B-Raf抑制剂,用于潜在治疗恶性黑色素瘤。PLX-4032及其相关类似物是B-Raf活性的高效抑制剂,对V600E突变的选择性是野生型的3倍。型激酶。
纯度: >98% (HPLC)






规格 | 价格/人民币 | 库存 | 数量 |
10MG | ¥405 | 有现货 |
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50MG | ¥583 | 有现货 |
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100MG | ¥810 | 有现货 |
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200MG | ¥1458 | 有现货 |
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500MG | ¥2479 | 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Plx-4032
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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PLX-4032是一种小分子B-Raf抑制剂,用于潜在治疗恶性黑色素瘤。PLX-4032及其相关类似物是B-Raf活性的高效抑制剂,对V600E突变的选择性是野生型的3倍。型激酶。
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产品描述PLX-4032 is a small-molecule B-Raf inhibitor for the potential treatment of malignant melanoma.PLX-4032 and its related analogs are highly potent inhibitors of B-Raf activity, with 3-fold selectivity for the V600E mutation over the wild-type kinase.?In preclinical models, PLX-4032 and its analogs inhibited the growth of BRAFV600E-positive melanoma cell lines both in vitro and in vivo.(In Vitro):Vemurafenib (PLX4032) selectively blocks the RAF/MEK/ERK pathway in BRAF mutant cells. RG7204 is a potent inhibitor of proliferation in those expressing RAFV600E but not BRAFWT in 17 melanoma cell lines. Vemurafenib (RG7204) induces MEK and ERK phosphorylation at high concentrations in CHL-1 cells. Ectopic expression of EGFR in melanoma cells is sufficient to cause resistance to PLX4032.(In Vivo):Vemurafenib (PLX4032, 20, 25, 75 mg/kg, p.o.) causes dose-dependent inhibition of tumor growth, with higher exposures resulting in tumor regression of BRAF mutant xenografts. RG7204 (12.5, 25, and 75 mg/kg, p.o.) significantly inhibits tumor growth and induced tumor regression in mice bearing LOX tumor xenografts.
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体外实验——
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体内实验——
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同义词Vemurafenib
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通路MAPK/ERK Signaling
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靶点Raf
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受体B-Raf
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研究领域——
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适应症——
化学信息
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CAS Number1029872-54-5
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分子量489.92
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分子式C23H18ClF2N3O3S
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纯度>98% (HPLC)
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溶解度——
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SMILESCCCS(=O)(=O)Nc1ccc(F)c(C(=O)c2c[nH]c3ncc(cc23)-c2ccc(Cl)cc2)c1F
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化学全称——
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. Smalley K S M . PLX-4032, a small-molecule B-Raf inhibitor for the potential treatment of malignant melanoma.[J]. Current Opinion in Investigational Drugs, 2010, 11(6):699-706.
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