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Genome-wide expression profiling of RNA interference of hepatitis B virus gene expression and replication

机译:乙型肝炎病毒基因表达与复制的RNA干扰全基因组表达谱

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Small interfering RNA (siRNA) has been used repeatedly to down-regulate viral gene expression and inhibit viral replication in mammalian cells. In this study, we showed that siRNAs specific for two conserved regions within the hepatitis B S antigen (HBsAg) gene can inhibit antigen production in two human liver cell lines which constitutively produce and secrete HBsAg. The inhibitory effect was concentration dependent for both PLC/PRF/5 and 2.2.15 cells. Decreases in the corresponding viral transcript levels were observed. The inhibitory effect was observed within 24 h and was still evident 7 days after the initial treatment with siRNA. A significant reduction in virion production was also observed for the 2.2.15 cells. A critical consideration in this study was the specificity of the siRNA-mediated inhibition. To address this, we first examined the effects on cell growth and viability. These were not affected in either cell line. cDNA microarrays were also used to examine genome-wide changes in gene regulation. No significant off-target gene regulation was observed in either cell line. Our findings thus indicate that siRNA can specifically mediate the down-regulation of viral gene expression leading to a reduction in virion production.
机译:小干扰RNA(siRNA)已被反复用于下调病毒基因表达并抑制病毒在哺乳动物细胞中的复制。在这项研究中,我们表明对B型肝炎S抗原(HBsAg)基因内两个保守区域具有特异性的siRNA可以抑制在两个组成性产生和分泌HBsAg的人类肝细胞系中的抗原产生。对于PLC / PRF / 5和2.2.15细胞,抑制作用均与浓度有关。观察到相应的病毒转录水平降低。在最初用siRNA处理7天后的24小时内观察到了抑制作用,并且仍然很明显。对于2.2.15细胞,还观察到病毒体产量的显着降低。这项研究中的关键考虑因素是siRNA介导的抑制作用的特异性。为了解决这个问题,我们首先检查了对细胞生长和活力的影响。这些在任一细胞系中均不受影响。 cDNA微阵列还用于检查基因调控范围内全基因组的变化。在两种细胞系中均未观察到明显的脱靶基因调控。因此,我们的发现表明,siRNA可以特异性介导病毒基因表达的下调,从而导致病毒体产量的减少。

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