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443642-29-3
  • names:

    MK-0608

  • CAS號:

    443642-29-3

    MDL Number: MFCD14584964
  • MF(分子式): C12H16N4O4 MW(分子量): 280.28
  • EINECS: Reaxys Number:
  • Pubchem ID:3011893 Brand:BIOFOUNT
MK-0608
MK-0608(443642-29-3)是一種有效的HCV復(fù)制抑制劑,在亞基因組復(fù)制子分析中,EC50為0.3μM(EC90=1.3μM)。
貨品編碼 規(guī)格 純度 價(jià)格 (¥) 現(xiàn)價(jià)(¥) 特價(jià)(¥) 庫存描述 數(shù)量 總計(jì) (¥)
YZM000546-10mg 10mg 99% ¥ 3560.00 ¥ 3560.00 2-3天
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YZM000546-5mg 5mg 99% ¥ 2180.00 ¥ 2180.00 2-3天
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中文別名 MK-0608(cas:443642-29-3),MK-0608,MK-608
英文別名 MK-0608(cas:443642-29-3),MK-0608,MK-608,7-Deaza-2'-C-methyladenosine
CAS號 443642-29-3
Inchi InChI=1S/C12H16N4O4/c1-12(19)8(18)7(4-17)20-11(12)16-3-2-6-9(13)14-5-15-10(6)16/h2-3,5,7-8,11,17-19H,4H2,1H3,(H2,13,14,15)/t7-,8-,11-,12-/m1/s1
InchiKey IRZRJANZDIOOIF-GAJNKVMBSA-N
分子式 Formula C12H16N4O4
分子量 Molecular Weight 280.28
溶解度Solubility
性狀 Solid
儲藏條件 Storage conditions 請根據(jù)產(chǎn)品建議的存儲條件進(jìn)行存儲,Please store the product under the recommended condition sin the description.
MK-0608(CAS:443642-29-3)實(shí)驗(yàn)注意事項(xiàng):
1.實(shí)驗(yàn)前需戴好防護(hù)眼鏡,穿戴防護(hù)服和口罩,佩戴手套,避免與皮膚接觸。
2.實(shí)驗(yàn)過程中如遇到有毒或者刺激性物質(zhì)及有害物質(zhì)產(chǎn)生,必要時(shí)實(shí)驗(yàn)操作需要手套箱內(nèi)完成以免對實(shí)驗(yàn)人員造成傷害
3.實(shí)驗(yàn)后產(chǎn)生的廢棄物需分類存儲,并交于專業(yè)生物廢氣物處理公司處理,以免造成環(huán)境污染Experimental considerations:
1. Wear protective glasses, protective clothing and masks, gloves, and avoid contact with the skin during the experiment.
2. The waste generated after the experiment needs to be stored separately, and handed over to a professional biological waste gas treatment company to avoid environmental pollution.
Tag:MK-0608蒸汽壓,MK-0608合成,MK-0608標(biāo)準(zhǔn),MK-0608應(yīng)用,MK-0608合成,MK-0608沸點(diǎn),MK-0608閃點(diǎn),MK-0608用途,MK-0608溶解度,MK-0608價(jià)格,MK-0608作用,MK-0608結(jié)構(gòu)式,MK-0608用處
產(chǎn)品說明 MK-0608(443642-29-3) 是一種有效的HCV復(fù)制的抑制劑,在亞基因組復(fù)制子測定中,EC50是 0.3 μM (EC90=1.3 μM)
IntroductionMK608(443642-29-3) is a potent and orally bioavailable inhibitor of HCV replicationin vitro with anEC50of 0.3 μM (EC90=1.3 μM) in the subgenomiceplicon assay.
Application1
Application2
Application3
2013-04-01 Synthesis and evaluation against hepatitis C virus of 7-deaza analogues of 2'-C-methyl-6-O-methyl guanosine nucleoside and L-Alanine ester phosphoramidates Bioorganic & medicinal chemistry
2012-08-01 Synthesis and antiviral properties of novel 7-heterocyclic substituted 7-deaza-adenine nucleoside inhibitors of Hepatitis C NS5B polymerase Bioorganic & medicinal chemistry
2012-06-15 Synthesis and characterization of 2'-C-Me branched C-nucleosides as HCV polymerase inhibitors Bioorganic & medicinal chemistry letters
2011-05-01 Elimination of hepatitis C virus by short term NS3-4A and NS5B inhibitor combination therapy in human hepatocyte chimeric mice Journal of hepatology
2009-03-01 Robust antiviral efficacy upon administration of a nucleoside analog to hepatitis C virus-infected chimpanzees Antimicrobial agents and chemotherapy
1.Viral RNA Polymerase Inhibitors/Todd Appleby i-hung shi and Wei understand zhong/02 May 2009
abstract:Infections by RNA viruses continue to exist as significant public health problems worldwide. In response to the urgent need for safer and more efficacious treatment options against infections caused by RNA viruses, the pharmaceutical and biotechnology industries have devoted significant efforts over the last two decades to discovering and developing new antiviral agents. As the primary viral enzyme responsible for genome replication and transcription, RNA-dependent RNA polymerases (RdRps) emerged early and remained as one of the most promising targets for therapeutic intervention of RNA virus infections. Advances in both basic research and drug discovery technology have resulted in the identification of a significant number of nucleoside (NIs) and non-nucleoside inhibitors (NNIs) of viral RdRps. In this chapter, we will focus our attention on various classes of viral RdRp inhibitors, with main emphases on those of hepatitis C virus (HCV) due to its significant unmet medical need. Recent progress in understanding their mechanism of action, antiviral activity profiles, and emergence of drug resistance mutations will be discussed.
2.Approaches for the Development of Antiviral Compounds: The Case of Hepatitis C Virus/Raymond F. SchinaziEmail authorSteven J. CoatsLeda C. BassitJohan LennerstrandJames H. NettlesSelwyn J. Hurwitz
abstract:Traditional methods for general drug discovery typically include evaluating random compound libraries for activity in relevant cell-free or cell-based assays. Success in antiviral development has emerged from the discovery of more focused libraries that provide clues about structure activity relationships. Combining these with more recent approaches including structural biology and computational modeling can work efficiently to hasten discovery of active molecules, but that is not enough. There are issues related to biology, toxicology, pharmacology, and metabolism that have to be addressed before a hit compound becomes nominated for clinical development. The objective of gaining early preclinical knowledge is to reduce the risk of failure in Phases 1, 2, and 3, leading to the goal of approved drugs that benefit the infected individual. This review uses hepatitis C virus (HCV), for which we still do not have an ideal therapeutic modality, as an example of the multidisciplinary efforts needed to discover new antiviral drugs for the benefit of humanity.
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