Identification of cellular targets for the human papillomavirus E6 and E7 oncogenes by RNA interference and transcriptome analyses

被引:0
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作者
Ruprecht Kuner
Markus Vogt
Holger Sultmann
Andreas Buness
Susanne Dymalla
Julia Bulkescher
Mark Fellmann
Karin Butz
Annemarie Poustka
Felix Hoppe-Seyler
机构
[1] German Cancer Research Center,Molecular Genome Analysis
[2] German Cancer Research Center,Molecular Therapy of Virus
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关键词
HPV; RNA interference; Microarray; Gene expression; Cervical cancer;
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摘要
Specific types of human papillomaviruses (HPVs) cause cervical cancer, the second most common tumor in women worldwide. Both cellular transformation and the maintenance of the oncogenic phenotype of HPV-positive tumor cells are linked to the expression of the viral E6 and E7 oncogenes. To identify downstream cellular target genes for the viral oncogenes, we silenced endogenous E6 and E7 expression in HPV-positive HeLa cells by RNA interference (RNAi). Subsequently, we assessed changes of the cellular transcriptome by genome-wide microarray analysis. We identified 648 genes, which were either downregulated (360 genes) or upregulated (288 genes), upon inhibition of E6/E7 expression. A large fraction of these genes is involved in tumor-relevant processes, such as apoptosis control, cell cycle regulation, or spindle formation. Others may represent novel cellular targets for the HPV oncogenes, such as a large group of C-MYC-associated genes involved in RNA processing and splicing. Comparison with published microarray data revealed a substantial concordance between the genes repressed by RNAi-mediated E6/E7 silencing in HeLa cells and genes reported to be upregulated in HPV-positive cervical cancer biopsies.
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页码:1253 / 1262
页数:9
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