Human Papillomavirus E6 Knockdown Restores Adenovirus Mediated-estrogen Response Element Linked p53 Gene Transfer in HeLa Cells.

Koji Kajitani,Masayasu Koyama,Toshiyuki Sumi,Osamu Ishiko,Honda Ken-Ichi,Tomoyo Yasui,Hiroyuki Terada

doi:10.7314/apjcp.2015.16.18.8239

Koji Kajitani, Masayasu Koyama + Show 5 more

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https://doi.org/10.7314/apjcp.2015.16.18.8239

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Abstract

The p53 gene is inactivated by the human papillomavirus (HPV) E6 protein in the majority of cervical cancers. Treatment of HeLa S3 cells with siRNA for HPV E6 permitted adenovirus-mediated transduction of a p53 gene linked to an upstream estrogen response element (ERE). Our previous study in non-siRNA treated HHUA cells, which are derived from an endometrial cancer and express estrogen receptor β, showed enhancing effects of an upstream ERE on adenovirus-mediated p53 gene transduction. In HeLa S3 cells treated with siRNA for HPV E6, adenovirus-mediated transduction was enhanced by an upstream ERE linked to a p53 gene carrying a proline variant at codon 72, but not for a p53 gene with arginine variant at codon 72. Expression levels of p53 mRNA and Coxsackie/adenovirus receptor (CAR) mRNA after adenovirus-mediated transfer of an ERE-linked p53 gene (proline variant at codon 72) were higher compared with those after non-ERE-linked p53 gene transfer in siRNA-treated HeLa S3 cells. Western blot analysis showed lower β-tubulin levels and comparatively higher p53/β-tubulin or CAR /β-tubulin ratios in siRNA-treated HeLa S3 cells after adenovirus-mediated ERE-linked p53 gene (proline variant at codon 72) transfer compared with those in non-siRNA-treated cells. Apoptosis, as measured by annexin V binding, was higher after adenovirus-mediated ERE-linked p53 gene (proline variant at codon 72) transfer compared with that after non-ERE-linked p53 gene transfer in siRNA-treated cells.

Highlights

The p53 gene is inactivated by the human papillomavirus (HPV) E6 protein in the majority of cervical cancers
In HeLa S3 cells treated with siRNA for HPV E6, adenovirus-mediated transduction was enhanced by an upstream estrogen response element (ERE) linked to a p53 gene carrying a proline variant at codon 72, but not for a p53 gene with arginine variant at codon 72
We studied the effect of the ERE on adenovirusmediated p53 transduction in HeLa S3 cells, which are derived from a human cervical cancer and contain integrated DNA of HPV type 18

Summary

Introduction

The p53 gene is inactivated by the human papillomavirus (HPV) E6 protein in the majority of cervical cancers. Our previous study in non-siRNA treated HHUA cells, which are derived from an endometrial cancer and express estrogen receptor β, showed enhancing effects of an upstream ERE on adenovirus-mediated p53 gene transduction. When E6 mRNA was silenced in HeLa S3 cells by incubation with siRNA for HPV type 18 E6, adenovirus-mediated transduction of the ERE-linked p53 gene (proline variant at codon 72) was restored and early-phase apoptosis rates were increased. These results suggested an unknown effect of ERE on trans-membrane and nuclear transport of the adenovirus-mediated p53 gene (proline variant at codon 72) and therapeutic potential for HPV-associated neoplasm

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