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Novel hepatitis C virus reporter replicon cell lines enable efficient antiviral screening against genotype 1a.

机译:新型丙型肝炎病毒报告基因复制子细胞系能够针对基因型1a进行有效的抗病毒筛选。

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The hepatitis C virus (HCV) subgenomic replicon is the primary tool for evaluating the activity of anti-HCV compounds in drug discovery research. Despite the prevalence of HCV genotype 1a (approximately 70% of U.S. HCV patients), few genotype 1a reporter replicon cell lines have been described; this is presumably due to the low replication capacity of such constructs in available Huh-7 cells. In this report, we describe the selection of highly permissive Huh-7 cell lines that support robust replication of genotype 1a subgenomic replicons harboring luciferase reporter genes. These novel cell lines support the replication of multiple genotype 1a replicons (including the H77 and SF9 strains), are significantly more permissive to genotype 1a HCV replication than parental Huh7-Lunet cells, and maintain stable genotype 1a replication levels suitable for antiviral screening. We found that the sensitivity of genotype 1a luciferase replicons to known antivirals was highly consistent between individual genotype 1a clonal cell lines but could vary significantly between genotypes 1a and 1b. Sequencing of the nonstructural region of 12 stable replicon cell clones suggested that the enhanced permissivity is likely due to cellular component(s) in these new cell lines rather than the evolution of novel adaptive mutations in the replicons. These new reagents will enhance drug discovery efforts targeting genotype 1a and facilitate the profiling of compound activity among different HCV genotypes and subtypes.
机译:丙型肝炎病毒(HCV)亚基因组复制子是在药物开发研究中评估抗HCV化合物活性的主要工具。尽管HCV基因型1a普遍存在(约占美国HCV患者的70%),但很少有人描述基因型1a报告基因复制子细胞系。推测这是由于此类构建体在可用的Huh-7细胞中的复制能力较低。在此报告中,我们描述了选择高度允许的Huh-7细胞系的选择,这些细胞系支持携带荧光素酶报道基因的基因型1a亚基因组复制子的强大复制。这些新型细胞系支持多种基因型1a复制子(包括H77和SF9菌株)的复制,与亲本Huh7-Lunet细胞相比,基因型1a HCV复制的容忍度明显更高,并保持适用于抗病毒筛选的稳定基因型1a复制水平。我们发现基因型1a荧光素酶复制子对已知抗病毒药的敏感性在各个基因型1a克隆细胞系之间高度一致,但在基因型1a和1b之间可能存在显着差异。对12个稳定复制子细胞克隆的非结构区进行测序表明,提高的介电常数很可能是由于这些新细胞系中的细胞成分所致,而不是复制子中新的适应性突变的发展。这些新试剂将增强针对基因型1a的药物发现工作,并促进不同HCV基因型和亚型之间化合物活性的概况分析。

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