A single-codon mutation converts HPV16 E6 oncoprotein into a potential tumor suppressor, which induces p53-dependent senescence of HPV-positive HeLa cervical cancer cells
T Ristriani1, S Fournane1, G Orfanoudakis1, G Travé1 and M Masson1
Correspondence: Dr M Masson, Equipe Oncoprotéines, CNRS-UMR 7175, ESBS, Boulevard Sébastien Brant, BP10413, Illkirch, Bas-Rhin 67412, France. E-mail: masson@esbs.u-strasbg.fr; Dr G Travé, Equipe Oncoprotéines, CNRS-UMR 7175, ESBS, Boulevard Sébastien Brant, BP10413, Illkirch, Bas-Rhin 67412, France. E-mail: gtrave@titus.u-strasbg.fr
Received 21 August 2008; Revised 29 September 2008; Accepted 21 October 2008; Published online 17 November 2008.
High-risk mucosal human papillomaviruses (HPV), mainly HPV16 and HPV18, are implicated in cervical carcinogenesis. HPV16 E6 oncoprotein binds and often targets for degradation numerous cell proteins, including the tumor suppressor p53 and several PDZ domain proteins. Here, we show that a single-point mutation, F47R, is sufficient to convert the HPV16 E6 oncoprotein into a suppressor of HPV-positive HeLa cervical cancer cells proliferation. The E6 F47R mutant is defective for polyubiquitination and subsequent degradation of p53. When expressed in HPV-positive cervical cancer cells, E6 F47R acts as a dominant negative mutant by counteracting the p53 degradation activity of endogenous E6 and restoring high p53 protein levels. Moreover, the prolonged expression of E6 F47R leads to suppression of HeLa cells proliferation through the induction of premature senescence. This phenotype is independent on the PDZ-binding activity of E6. F47R-senescent HeLa cells exhibit a sustained expression of p53, hMDM2 and p21CIP proteins and a reduced expression of endogenous HPV18 E6 protein. Finally, small interfering RNAs directed against p53 counteract the effect of E6 F47R expression, indicating that E6 F47R-induced cellular senescence is strongly dependent on p53 signaling pathway.
Keywords: human papillomavirus, cervical cancer, E6 oncoprotein, senescence, p53 protein