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首页> 外文期刊>FEBS Letters >Specific inhibition of gene expression and transactivation functions of hepatitis B virus X protein and c‐myc by small interfering RNAs
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Specific inhibition of gene expression and transactivation functions of hepatitis B virus X protein and c‐myc by small interfering RNAs

机译:小干扰RNA特异性抑制乙型肝炎病毒X蛋白和c-myc的基因表达和反式激活功能

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摘要

>With a view to developing therapeutic strategies against hepatocellular carcinoma (HCC), we have recently shown that co-expression of c-myc and the X protein of hepatitis B virus (HBx) resulted in the development of HCC in the X-myc transgenic mice [Lakhtakia et al., J. Gastroenterol. Hepatol. 18 (2003) 80–91]. We now show in cell culture-based studies that small interfering RNA (siRNA) corresponding to HBx and c-myc can regulate expression and transactivation of the target genes. Expression vectors for small hairpin RNAs (shRNAs) against two different regions each of the HBx and c-myc open reading frames were constructed and their regulatory effects were investigated in COS-1 cells. A dose-dependent specific inhibition in the expression levels of HBx and c-myc was observed with individual shRNAs. Further, the recombinantly expressed shRNAs also blocked the transactivation functions of their cognate genes. Though each shRNA worked at a different efficiency, the inhibitory effects with two different shRNAs were cumulative. These results appear promising for developing a siRNA-based therapy for HCC.
机译:>为了制定针对肝细胞癌(HCC)的治疗策略,我们最近发现c- myc 和乙型肝炎病毒X蛋白(HBx)的共同表达导致X- myc 转基因小鼠中HCC的发育[Lakhtakia等,J。Gastroenterol。肝素18(2003)80-91]。现在,我们在基于细胞培养的研究中表明,与HBx和c- myc 相对应的小干扰RNA(siRNA)可以调节靶基因的表达和反式激活。构建了针对HBx和c- myc 开放阅读框两个不同区域的小发夹RNA(shRNA)的表达载体,并研究了它们在COS-1细胞中的调控作用。用单个shRNA观察到HBx和c- myc 表达水平的剂量依赖性特异性抑制。此外,重组表达的shRNA也阻断了其同源基因的反式激活功能。尽管每种shRNA的工作效率不同,但两种不同shRNA的抑制作用是累积的。这些结果对于开发基于siRNA的HCC治疗方法似乎很有希望。

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