Publication

Identification of an Rta responsive promoter involved in driving gammaHV68 v-cyclin expression during virus replication

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Last modified
  • 02/20/2025
Type of Material
Authors
    Robert D. Allen, Emory UniversityMark N. DeZalia, Emory UniversitySam Speck, Emory University
Language
  • English
Date
  • 2007-09-01
Publisher
  • Elsevier
Publication Version
Copyright Statement
  • © 2007 Elsevier
License
Final Published Version (URL)
Title of Journal or Parent Work
ISSN
  • 0042-6822
Volume
  • 365
Issue
  • 2
Start Page
  • 250
End Page
  • 259
Grant/Funding Information
  • This work was supported by a Leukemia and Lymphoma Society grant to RDA (5575-02) and a National Institutes of Health grant to SHS (CA87650).
Abstract
  • Among the distinguishing characteristics of members of the gamma-2 herpesvirus family is the expression of a mammalian D-type cyclin homolog, termed v-cyclin. Murine gammaherpesvirus 68 (γHV68) is a γ2-herpesvirus that can infect inbred and outbred strains of mice, providing a genetic system for the study of gammaherpesvirus pathogenesis. Disruption of the v-cyclin gene of γHV68 results in a virus that establishes latency in infected mice to wild-type levels, but is severely attenuated for virus reactivation [L.F. van Dyk, H.W. Virgin IV, S.H. Speck (2000) J. Virol. 74:7451-7461]. Transcriptional regulation of the γHV68 v-cyclin has not been defined. We report here the initial characterization of the v-cyclin transcript expressed in permissive murine fibroblasts. Based on 5′ mapping of the v-cyclin transcript, we identified a promoter that is involved in driving v-cyclin expression during virus replication. In addition, we determined that the promoter is responsive to the major viral lytic transactivator, Rta, encoded by orf 50. Using reporter plasmids we have analyzed both basal and Rta-induced v-cyclin promoter activity - initially identifying two regions of the v-cyclin promoter important for both basal and Rta-induced activity. Notably, only one of these regions could be shown to confer Rta responsiveness on a reporter construct containing the hsp70 TATA box. The importance of this region in regulating v-cyclin expression during virus replication was confirmed by introducing these mutations into the context of the viral genome and assessing v-cyclin expression following infection of permissive murine fibroblasts in tissue culture. In addition, we show that mutations that severely cripple Rta-induction of v-cyclin expression did not adversely impact virus reactivation from splenocytes recovered from latently infected mice, indicating that alternatively regulated v-cyclin gene expression is required for virus reactivation.
Author Notes
  • Correspondence: Samuel H. Speck, Emory Vaccine Center, 1462 Clifton Road, Emory University School of Medicine, Rm 3001 Rollins Research Center, 1510 Clifton Rd., NE., Atlanta, GA 30322; Phone: (404) 727-7665; Email: sspeck@emory.edu
Research Categories
  • Health Sciences, Immunology
  • Biology, Microbiology

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