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RNAi对HCV ns5b基因表达的抑制作用 被引量:4

Inhibitory effect of RNAi on HCV ns5b gene expression
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摘要 目的 :研究RNAi(RNAinterference)效应对HCVns5b基因表达的抑制作用 .方法 :根据HCVns5b基因序列及其二级结构特征 ,依据Tuschl等设计siRNA的原则 ,确定并合成了针对ns5b基因的siRNAs;利用电转化方法将合成的siRNAs转染NS5B EGFPHepG2细胞株 ,以未转染的细胞为对照 ;细胞爬片后经DAPI染色 ,荧光显微镜下观察和半定量RT PCR法检测siRNAs的抑制效应 .结果 :化学合成的siRNAs可以抑制HCVns5b基因的表达 ,效率可达 70 %-80 %以上 .结论 :在细胞水平上 ,化学合成的siRNAs可以抑制HCVns5b基因的表达 。 AIM: To inhibit HCV ns5b gene expression with RNAi. METHODS: According to the gene sequence and secondary structure of HCV ns5b , we designed the siRNAs targeting ns5b gene following the requirement from Tuschl et al and it was synthesized in Dharmacon company. HepG2 cells stably expressing NS5B EGFP protein were transfected by synthesized siRNAs with electroportion, the non transfected cells and non specific siRNAs transfected cells were taken as controls. Inhibitory effect of siRNAs was detected under fluorescence microscope with DAPI dyeing and by semi quantitative RT PCR. RESULTS: Synthesized siRNA inhibited HCV ns5b gene expression by 70%-80%. CONCLUSION: At the cell level, inhibition of HCV ns5b gene expression by synthesized siRNA provides the new method for anti HCV study.
作者 雷迎峰 薛小平 尹文 张伟 吕欣
机构地区 第四军医大学基础部微生物学教研室
出处 《第四军医大学学报》 北大核心 2003年第12期1082-1084,共3页 Journal of the Fourth Military Medical University
基金 第四军医大学校创新工程资助项目 (CX0 1A0 1 1 ) 陕西省自然科学基金(2 0 0 1SM 51 )
关键词 C型肝炎样病毒属 非结构区5b基因 小干扰性RNA 抑制效应 Hepatitis C like viruses ns5b gene siRNAs inhibitory effect
分类号 R373.21 [医药卫生—病原生物学]
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参考文献10

  • 1[1]Lei YF, Xue XP, Yin W. Advance in RNAi [J]. Guowai Yixue Fenzi Shengwuxue Fence (Sect Foreign Med Mol Biol). 2002;4(24):3-5.
  • 2[2]Elbashir SM, Harborth J, Lendeckel W, Yalcin A, Weber K, T. Tuschl. 2001. Duplexes of 21-nucleotide RNAs mediate RNA interference in cultured mammalian cells [J]. Nature, 2001;411(6836):494-498.
  • 3[3]Lei YF, Xue XP, Yin W, Zhang W, Lü X. Construction of eukaryotic expression vector expressing HCV NS5B and EGFP fusion protein and establishment of stably transfected HepG2 cell line [C]. Quanguo Diyici Mianyi Zhenduan Jishu Dahui Lunwen Huibian (Article Collection of First Immunological and Diagnostic Technique Conference in China), Beijing, 2002;65-69.
  • 4[4]Tom Tuschl, Sayda Elbashir, Jens Harborth, and Klaus Weber. The siRNA user guide. http://www.mpibpc.gwdg.de/abteilungen/100/105/sirna.html. October 11, 2002.
  • 5[5]Paul CP, Good PD, Winer I, Engelke DR. Effective expression of small interfering RNA in human cells [J]. Nat Biotechnol, 2002;20(5):505-508.
  • 6[6]Hannon GJ. RNA interference [J]. Nature, 2002;418(6894):244-251.
  • 7[7]Miyagishi M, Taira K. U6 promoter-driven siRNAs with four uridine 3' overhangs efficiently suppress targeted gene expression in mammalian cells [J]. Nat Biotechnol, 2002;20(5):497-500.
  • 8[8]Zhou YX, Jia ZS, Lian JQ. Cellular immune and its impact of anti-HCV ribozyme [J]. Di-si Junyi Daxue Xuebao (J Fourth Mil Med Univ), 2000;21(7):796-801.
  • 9[9]Yu JY, DeRuiter SL, Turner DL. RNA interference by expression of short-interfering RNAs and hairpin RNAs in mammalian cells [J]. Proc Natl Acad Sci USA, 2002;99(9):6047-6052.
  • 10[10]Zhou YX, Jia ZS. To improve the research on geneitic therapy of hepatitis virus [J]. Di-si Junyi Daxue Xuebao (J Fourth Mil Med Univ), 2000;21(7):781-783.

同被引文献67

  • 1凌世淦.丙型肝炎疫苗研究的挑战与希望[J].中华微生物学和免疫学杂志,2004,24(11):921-926. 被引量:11
  • 2陈佳玉,李凡.乙型肝炎核心抗原为载体进行丙型肝炎混合性治疗疫苗的实验[J].中华传染病杂志,2007,25(3):137-142. 被引量:2
  • 3[20]Holen T, Amarzguioui M, Wiiger MT, et al. Potitional effects of short interfering RNAs targeting the human cogulation trigger tissue factor. Nucleic Acids Research ,2002,30 ( 8 ): 1757-1766.
  • 4[21]Shirane D, Sugao K,Namiki S et al. Enzymatic production of RNAi libraries from cDNAs. Nat Genet,2004,36(2): 190-196.
  • 5[22]Liu CM, Liu DP, Dong, WJ et al. Retrovirus vector-mediated stable gene silencing in human cell. Biochem Biophys Res Commun,2004,313(3): 716-720.
  • 6[23]Bain JR, Schisler JC, Takeuchi K et al. An adenovirus vector for efficient RNA interference-mediated suppression of target genes in insulinoma cells and pancreatic islets of langerhans. Diabetes ,2004,53(9): 2190-2194.
  • 7[24]Wohlbold L, Van Der Kuip H et al. Inhibition of bcr-abl gene expression by small interfering RNA sensitizes for imatinib mesylate ( STI571 ). Blood, 2003,102 (6): 2236-2239.
  • 8[25]Scacheri PC, Rosen OR, Caplen NJ et al. Short interfering RNAs can induce unexpected and divergent changes in the levels of untargeted proteins in mammlian cells. PNAS,2004,101:1892-1897.
  • 9[13]Elbashir SM, Harborth J, Lendeckel W, et al. Duplexes of 21 nucleotide RNAs mediate RNAs interference in culture mammalian cells. Nature,2001,411 (6836) :494-498.
  • 10[14]Brummelkamp TR, Bernards B,Agami R. A system for stable expression of short interfering RNAs in mammalian cells. Science,2002,296: 550-553.

引证文献4

第四军医大学学报
2003年 第12期

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