Journal
BIOCHEMISTRY AND CELL BIOLOGY
Volume 88, Issue 4, Pages 697-704Publisher
CANADIAN SCIENCE PUBLISHING
DOI: 10.1139/O10-005
Keywords
human papillomavirus; HeLa cell line; RNA interference
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The objective of this investigation was to determine if simultaneous silencing of the human papillomavirus type 18 (HPV-18) E6 and E7 oncogenes using RNA interference (RNAi) would be a potential therapeutic approach against the carcinogenic activity of this virus. Two synthetic double-stranded oligonucleotides, encoding short hairpin transcripts corresponding to HPV-18 E6 and E7 genes, were cloned into pGenesilence (pGS) 1 0 vectors to produce pGS-E6, pGS-E7. and pGS-(E6+E7), respectively Our results showed that the expression of HPV-I8 E6 class I and HPV-18 E7 in He La cells was markedly decreased after being transfccted with pGS-E6, pGS-E7, and pGS-(E6+E7) vectors Of the three vectors, pGS-(E6+E7) had a greater ability to decrease the growth rate of He La cells, Inhibit colony formation in soft agar, and significantly reduce tumor growth in nude mice We also found that depletion of HPV-I8 E6 and E7 in this manner promoted apoptosts of He La cells. Our data showed that simultaneously decreasing HPV-18 E6 and E7 gene expression in He La cells by RNA] could significantly inhibit tumor growth under in vitro conditions and in nude mice These data suggest that gene therapy may be a possible therapeutic approach for HPV-positive cervical cancers
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