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20724-73-6
  • names:

    NM107

  • CAS號(hào):

    20724-73-6

    MDL Number: MFCD02682947
  • MF(分子式): C10H15N3O5 MW(分子量): 257.24
  • EINECS: Reaxys Number:
  • Pubchem ID:500902 Brand:BIOFOUNT
NM107
NM107(20724-73-6)具有抗丙型肝炎病毒(HCV)活性的核苷類(lèi)似物。 在被磷酸化為5-三磷酸形式后,這種代謝物會(huì)抑制病毒RNA鏈延長(zhǎng)和病毒RNA依賴性RNA聚合酶活性。 這會(huì)阻止HCV RNA的病毒產(chǎn)生,從而阻止病毒復(fù)制。
貨品編碼 規(guī)格 純度 價(jià)格 (¥) 現(xiàn)價(jià)(¥) 特價(jià)(¥) 庫(kù)存描述 數(shù)量 總計(jì) (¥)
YZM000566-10mg 10mg 99.52% ¥ 911.00 ¥ 911.00 2-3天
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0.00
YZM000566-5mg 5mg 99.52% ¥ 585.00 ¥ 585.00 2-3天
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中文別名 NM107(cas:20724-73-6),2'-C-甲基胞嘧啶核苷,2'-C-甲基胞苷,2'-C-甲基胞嘧啶核苷
英文別名 NM107(cas:20724-73-6),2'-C-Methylcytidine,NM 107,NM-107,2'C-Me-C,2'-C-methyl-cytidine
CAS號(hào) 20724-73-6
Inchi InChI=1S/C10H15N3O5/c1-10(17)7(15)5(4-14)18-8(10)13-3-2-6(11)12-9(13)16/h2-3,5,7-8,14-15,17H,4H2,1H3,(H2,11,12,16)/t5-,7-,8-,10-/m1/s1
InchiKey PPUDLEUZKVJXSZ-VPCXQMTMSA-N
分子式 Formula C10H15N3O5
分子量 Molecular Weight 257.24
溶解度Solubility 生物體外In Vitro:H2O≥ 50 mg/mL(194.37 mM)*"≥" means soluble可溶, but saturation unknown溶解度未知.
性狀 固體粉末,Power
儲(chǔ)藏條件 Storage conditions -20°C 3 years年 4°C 2 years年 / In solvent溶液中:-80°C 6 months月 -20°C 1 month月
NM107(CAS:20724-73-6)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(guò)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(duì)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(lèi)存儲(chǔ),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:NM107蒸汽壓,NM107合成,NM107標(biāo)準(zhǔn),NM107應(yīng)用,NM107合成,NM107沸點(diǎn),NM107閃點(diǎn),NM107用途,NM107溶解度,NM107價(jià)格,NM107作用,NM107結(jié)構(gòu)式,NM107用處
產(chǎn)品說(shuō)明 NM107(20724-73-6)是丙型肝炎病毒 (HCV) NS5B 聚合酶的核苷的抑制劑
IntroductionNM107 ((20724-73-6,2'ethylcytidine) is an nucleoside inhibitor of thehepatitis C virus (HCV) NS5B polymerase, theEC50of NM107 in the wildype replicon cells is 1.85 μM[2].
Application1
Application2
Application3
2014-03-13 Nucleotide prodrugs of 2'-deoxy-2'-spirooxetane ribonucleosides as novel inhibitors of the HCV NS5B polymerase Journal of medicinal chemistry
2012-11-02 Inhibition of norovirus replication by the nucleoside analogue 2'-C-methylcytidine Biochemical and biophysical research communications
2012-06-15 Synthesis and characterization of 2'-C-Me branched C-nucleosides as HCV polymerase inhibitors Bioorganic & medicinal chemistry letters
2012-05-01 Anti-hepatitis C virus activity of 3-hydroxy caruilignan C from Swietenia macrophylla stems Journal of viral hepatitis
2012-03-01 Novel substituted 9-norbornylpurines and their activities against RNA viruses Bioorganic & medicinal chemistry letters
1.Nucleoside analogue 2’-C-methylcytidine inhibits hepatitis E virus replication but antagonizes ribavirin    Archives of Virology    2017
Abstract:
Hepatitis E virus (HEV) infection has emerged as a global health issue, but no approved medication is available. The nucleoside analogue 2’-C-methylcytidine (2CMC), a viral polymerase inhibitor, has been shown to inhibit infection with a variety of viruses, including hepatitis C virus (HCV). Here, we report that 2CMC significantly inhibits the replication of HEV in a subgenomic replication model and in a system using a full-length infectious virus. Importantly, long-term treatment with 2CMC did not result in a loss of antiviral potency, indicating a high barrier to drug resistance development. However, the combination of 2CMC with ribavirin, an off-label treatment for HEV, exerts antagonistic effects. Our results indicate that 2CMC serves as a potential antiviral drug against HEV infection.
2.Zika Virus: Where Is the Treatment?    Current Treatment Options in Infectious Diseases    2016
Abstract:In the twenty-first century, we have seen the (re-)emergence of several RNA viruses causing severe infections in humans, like SARS and MERS coronavirus, and more recently Ebola virus and Zika virus (ZIKV). A problem with (re-)emerging virus infections is the lack of available medical countermeasures, including antiviral treatment. Therefore, the development of broadly acting antiviral compounds, as well as screening of existing drugs for potential repurposing are explored as ways to fast-track the drug development pipeline for emerging viral diseases. Here, we briefly discuss the available information on potential antiviral treatment of ZIKV infection, as well as specific challenges regarding use of antivirals.
Zika virus is a positive-sense single-stranded RNA arbovirus that belongs to the genus Flavivirus of the family Flaviviridae. Based on nucleotide sequences, ZIKV can be further divided into an African lineage and an Asian lineage. The main vector for ZIKV transmission are Aedes mosquitoes. The first isolation of ZIKV was made in 1947 from serum of a febrile rhesus monkey in the Zika forest of Uganda. During the twentieth century, sporadic human cases of ZIKV infection were reported in Africa caused by the African lineage, and in Asia caused by Asian lineage. The epidemiology of ZIKV changed dramatically in the last decade, when major outbreaks of the Asian lineage of ZIKV were reported on the Island of Yap in 2007 and in French Polynesia in 2013. Subsequently, the Asian lineage of ZIKV spread to the Americas in 2015.
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