Genetic Analysis of High-Risk E6 in Episomal Maintenance of Human Papillomavirus Genomes in Primary Human Keratinocytes

doi:10.1128/JVI.76.22.11359-11364.2002

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Journal of Virology, November 2002, p. 11359-11364, Vol. 76, No. 22
0022-538X/02/$04.00+0 DOI: 10.1128/JVI.76.22.11359-11364.2002
Copyright © 2002, American Society for Microbiology. All Rights Reserved.

Genetic Analysis of High-Risk E6 in Episomal Maintenance of Human Papillomavirus Genomes in Primary Human Keratinocytes

Regina B. Park¹^, and Elliot J. Androphy¹^,2^*

Department of Molecular Biology and Microbiology, Tufts University School of Medicine,¹ Department of Dermatology, Tufts-New England Medical Center, Boston, Massachusetts²

Received 21 May 2002/ Accepted 13 August 2002

Papillomaviruses possess small DNA genomes that encode fiveearly (E) proteins. Transient DNA replication requires activitiesof the E1 and E2 proteins and a DNA segment containing theirbinding sites. The E6 and E7 proteins of cancer-associated humanpapillomavirus (HPV) transform cells in culture. Recent reportshave shown that E6 and E7 are necessary for episomal maintenanceof HPV in primary keratinocytes. The functions of E6 necessaryfor viral replication have not been determined, and to addressthis question we used a recently developed transfection systembased on HPV31. To utilize a series of HPV16 E6 mutations, HPV31E6 was replaced by its HPV16 counterpart. This chimeric genomewas competent for both transient and stable replication in keratinocytes.Four HPV16 E6 mutations that do not stimulate p53 degradationwere unable to support stable viral replication, suggestingthis activity may be necessary for episomal maintenance. E7has also been shown to be essential for episomal maintenanceof the HPV31 genome. A point mutation in the Rb binding motifof HPV E7 has been reported to render HPV31 unable to stablyreplicate. Interestingly, HPV31 genomes harboring two of thethree p53 degradation-defective E6 mutations combined with thisE7 mutation were maintained as replicating episomes. These findingsimply that the balance between E6 and E7 functions in infectedcells is critical for episomal maintenance of high-risk HPVgenomes. This model will be useful to dissect the activitiesof E6 and E7 necessary for viral DNA replication.

* Corresponding author. Present address: University of Massachusetts Medical School, LRB 328, 364 Plantation St., Worcester, MA 01605-2324. Phone: (508) 856-6605. Fax: (508) 856-6588. E-mail: elliot.androphy{at}umassmed.edu.

Present address: PKC Corporation, Burlington, VT 05401.

Journal of Virology, November 2002, p. 11359-11364, Vol. 76, No. 22
0022-538X/02/$04.00+0 DOI: 10.1128/JVI.76.22.11359-11364.2002
Copyright © 2002, American Society for Microbiology. All Rights Reserved.

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