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Your Position: Home > Small Molecule Compounds > Anti-Infection > Antiviral > Danoprevir

Danoprevir

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Cat.No:ID1080 Solarbio

CAS:850876-88-9

Storage:Powder:2-8℃,2 years;Insolvent(Mother Liquid):-20℃,6 months;-80℃,1 year

Purity:≥98%

Appearance:White to off-white Solid

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Product Information

CAS 850876-88-9
Name Danoprevir
Molecular Formula C35H46FN5O9S
Molecular Weight 731.83
Solubility Soluble in DMSO
Purity ≥98%
Appearance White to off-white Solid
Storage Powder:2-8℃,2 years;Insolvent(Mother Liquid):-20℃,6 months;-80℃,1 year
MDL MFCD16038038
SMILES O=S(NC([C@@]1(NC([C@]2([H])C[C@@H](OC(N3CC4=C(C3)C=CC=C4F)=O)CN2C5=O)=O)C[C@]1(/C=C/CCCCC[C@@H]5NC(OC(C)(C)C)=O)[H])=O)(C6CC6)=O
Target Point HCV Protease
Passage Metabolic Enzyme/Protease
Background Danoprevir is a peptidomimetic inhibitor that inhibits HCV NS3/4A protease.
Biological Activity Danoprevir 是一种模拟肽类抑制剂, 能够抑制 HCV NS3/4A protease, IC50 值为 0.2-3.5 nM[1-3]。
IC50 IC50: 0.2-3.5nM (NS3/4A protease) [1-3]
In Vitro 在用嵌合重组病毒转染的Huh7.5细胞中,Danoprevir对HCV基因型1,4和6具有抗病毒抑制作用,IC50为2-3 nM,比基因型2/3/5(280-750)低100倍。 nM)的[1]。 Danoprevir(0.29 nM)半数最大限度地抑制参考基因型1 NS3 / 4A蛋白酶,但高剂量的Danoprevir(10μM)在一组79种蛋白酶,离子通道,转运蛋白和细胞表面受体中没有显示出明显的抑制作用。在初始结合后,Danoprevir仍然与NS3 / 4A结合并抑制超过5小时。 Danoprevir(45 nM)从肝细胞来源的Huh7细胞中消除了源自患者的HCV基因型1b复制子,EC50为1.8 nM [2]。在含有单个突变的HCV亚基因组复制子细胞系中,V36M,R109K和V170A取代对Danoprevir几乎没有或没有抗性,但R155K取代赋予对Danoprevir的高水平(62倍增加)抗性[3]。
In Vivo 给予大鼠或猴子的Danoprevir(30mg / kg,口服)显示其在给药后12小时其在肝脏中的浓度超过消除细胞复制子RNA所需的Danoprevir浓度[2]。
Animal Experiment 在大鼠和猴子中评估药代动力学特性。通过口服管饲法(6mg / mL水溶液)给Sprague-Dawley大鼠(每个时间点三只)施用30mg / kg体重剂量的ITMN-191。通过口服强饲法(3mg / mL水溶液)给食蟹猴(每个时间点两个)施用30mg / kg剂量的ITMN-191。对于每个物种,在给药后1,4,8,12和24小时收集末端血液样品和整个灌注的肝脏。在EDTA中收集血液样品,通过在5℃下离心处理血浆,并在-20℃下储存直至进行分析。将肝脏样品快速冷冻并储存在-70℃直至进行分析。将空白的,标准的和未知的血浆样品和含有内标的均质肝(ITMN-191类似物)用酸化的乙腈处理并离心以除去沉淀的蛋白质。考虑肝组织的密度以允许两个隔室中的浓度表示为每单位体积的重量。将澄清的上清液以1:1稀释到高效液相色谱级水中,并在装有以负离子模式操作的Turbo-Ionspray源的4000 Q-trap液相色谱 - 串联质谱仪上进行分析。使用多反应监测扫描监测分析物和内标,并使用ABI Analyst软件1.4.2进行校准。对于血浆样品和肝匀浆的定量,校准标准品的范围分别为0.0169 ng / mL至37.0 ng / mL和7.47 ng / mL至5,440 ng / mL。使用具有1 / x加权的二次拟合,其中在两个矩阵中实现> 0.999的R2值。
Kinase Experiment 测定缓冲液含有25μMNS4A肽,50mM Tris-HCl,pH 7.5,15%(vol / vol)甘油,0.6mM月桂基二甲基胺N-氧化物,10mM二硫苏糖醇和0.5μM荧光素/ QXL520标记的FRET底物{Ac -DE-DAP(QXL520)-EE-阿布ψ-[COO] -AS-半胱氨酸(5- FAMsp)-NH 2}。加入K2040酶(50pM)以引发反应。在黑色96孔板中建立反应,并收集荧光数据。包括缺乏抑制剂和酶的对照反应。初始速率由反应的线性相(最多1小时)计算并用于获得IC 50。从预先形成的Danoprevir-NS3 / 4A复合物中恢复活性通过将10nM NS3 / 4A与2倍过量的Danoprevir在1x测定缓冲液中预孵育15分钟,然后将预先形成的复合物快速200倍稀释到含有底物的测定缓冲液在没有预孵育NS3 / 4A和Danoprevir的情况下,通过向其他完全反应混合物中加入酶来引发具有相同最终条件的对照反应。其他对照反应缺乏Danoprevir或NS3。在5小时内进行反应进程。
Data Literature Source [1]. Imhof I, et al. Genotype differences in susceptibility and resistance development of hepatitis C virus to protease inhibitors telaprevir (VX-950) and danoprevir (ITMN-191) .Hepatology. 2011 Apr; 53 (4) :1090-9.
[2]. Seiwert, Scott D., et al. Preclinical characteristics of the hepatitis C virus NS3/4A protease inhibitor ITMN-191 (R7227) . Antimicrobial Agents and Chemotherapy (2008) , 52 (12) , 4432-4441.
[3]. Bartels DJ, et al. Natural prevalence of hepatitis C virus variants with decreased sensitivity to NS3.4A protease inhibitors in treatment-naive subjects. J Infect Dis. 2008 Sep 15; 198 (6) :800-7
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Danoprevir 是一种模拟肽类抑制剂,能够抑制 HCV NS3/4A protease。

Remark:These protocols are for reference only. Solarbio does not independently validate these methods.

Note:

1. The products are all for scientific research use only. Do not use it for medical, clinical diagnosis or treatment, food and cosmetics, etc. Do not store them in ordinary residential areas.

2. For your safety and health, please wear laboratory clothes, disposable gloves and masks.

3. The experimental results may be affected by many factors, after-sale service is limited to the product itself and does not involve other compensation.

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