ZEB Negatively Regulates the Lytic-Switch BZLF1 Gene Promoter of Epstein-Barr Virus

doi:10.1128/JVI.77.1.199-207.2003

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Journal of Virology, January 2003, p. 199-207, Vol. 77, No. 1
0022-538X/03/$08.00+0 DOI: 10.1128/JVI.77.1.199-207.2003
Copyright © 2003, American Society for Microbiology. All Rights Reserved.

ZEB Negatively Regulates the Lytic-Switch BZLF1 Gene Promoter of Epstein-Barr Virus

Richard J. Kraus, Jacqueline G. Perrigoue, and Janet E. Mertz^*

McArdle Laboratory for Cancer Research, University of Wisconsin Medical School, Madison, Wisconsin 53706-1599

Received 13 June 2002/ Accepted 6 August 2002

Epstein-Barr virus (EBV) is a human herpesvirus capable of establishinga latent state in B lymphocytes. The product of the immediate-earlyBZLF1 gene, Zta, is a transcriptional transactivator essentialfor viral DNA amplification and virion production. Previously,we identified a negative cis-acting element within the BZLF1promoter termed ZV. ZV contains the sequence 5'-CAGGTA-3' locatedat nucleotides -17 to -12 relative to the transcription initiationsite. It sequence specifically binds a cellular factor, ZVR.Based on sequence binding specificity, we postulated that ZVRmay be zinc finger E-box binding factor (ZEB) or a related zincfinger/homeodomain family member. We show here by immunoshiftassays that ZVR and human ZEB specifically cross-react withan antibody to ${delta}$ EF1, the chicken homolog of ZEB. Competitionelectrophoretic mobility shift assays confirmed that ZEB bindsto the ZV element with the same binding specificity as ZVR.Overexpression of ZEB in either B-lymphocytic DG75 cells ormammary epithelial MCF-7 cells repressed Zta-induced activationof the BZLF1 promoter four- to fivefold via the ZV site. Thus,we conclude that the previously identified cellular repressorZVR is, in fact, ZEB. We also present evidence that other cellularfactors likely affect the transcriptional activity of ZEB. Lastly,we identify a ZEB-binding site within the promoter of the lyticBRLF1 gene of EBV. We postulate that ZEB likely plays an importantrole in regulating the life cycle of EBV.

* Corresponding author. Mailing address: Department of Oncology, McArdle Laboratory for Cancer Research, University of Wisconsin—Madison, 1400 University Ave., Madison, WI 53706-1599. Phone: (608) 262-2383. Fax: (608) 262-2824. E-mail: mertz{at}oncology.wisc.edu.