Control of Pathogenicity and Disease Specificity of a T-Lymphomagenic Gammaretrovirus by E-Box Motifs but Not by an Overlapping Glucocorticoid Response Element

doi:10.1128/JVI.01368-08

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Journal of Virology, January 2009, p. 336-346, Vol. 83, No. 1
0022-538X/09/$08.00+0 doi:10.1128/JVI.01368-08
Copyright © 2009, American Society for Microbiology. All Rights Reserved.

Control of Pathogenicity and Disease Specificity of a T-Lymphomagenic Gammaretrovirus by E-Box Motifs but Not by an Overlapping Glucocorticoid Response Element

Ditte Ejegod,¹ Karina Dalsgaard Sørensen,¹ Ilona Mossbrugger,² Leticia Quintanilla-Martinez,² Jörg Schmidt,³ and Finn Skou Pedersen¹^*

Department of Molecular Biology, University of Aarhus, Denmark,¹ Institute of Pathology,² Department of Comparative Medicine, Helmholtz Zentrum Munich, German Research Center for Environmental Health (GmbH), Neuherberg, Germany³

Received 1 July 2008/ Accepted 13 October 2008

Although transcription factors of the basic helix-loop-helixfamily have been shown to regulate enhancers of lymphomagenicgammaretroviruses through E-box motifs, the overlap of an E-boxmotif (Egre) with the glucocorticoid response element (GRE)has obscured their function in vivo. We report here that Egre,but not the GRE, affects disease induction by the murine T-lymphomagenicSL3-3 virus. Mutating all three copies of Egre prolonged thetumor latency period from 60 to 109 days. Further mutating anE-box motif (Ea/s) outside the enhancer prolonged the latencyperiod to 180 days, suggesting that Ea/s works as a backup sitefor Egre. While wild-type SL3-3 and GRE and Ea/s mutants exclusivelyinduced T-cell lymphomas with wild-type latencies mainly ofthe CD4⁺ CD8^– phenotype, Egre as well as the Egre andEa/s mutants induced B-cell lymphomas and myeloid leukemia inaddition to T-cell lymphomas. T-cell lymphomas induced by thetwo Egre mutants had the same phenotype as those induced bywild-type SL3-3, indicating the incomplete disruption of T-celllymphomagenesis, which is in contrast to previous findings fora Runx site mutant of SL3-3. Mutating the Egre site or Egreand Ea/s triggered several tumor phenotype-associated secondaryenhancer changes encompassing neighboring sites, none of whichled to the regeneration of an E-box motif. Taken together, ourresults demonstrate a role for the E-box but not the GRE inT lymphomagenesis by SL3-3, unveil an inherent broader diseasespecificity of the virus, and strengthen the notion of selectionfor more potent enhancer variants of mutated viruses duringtumor development.

* Corresponding author. Mailing address: Department of Molecular Biology, University of Aarhus, C. F. Møllers Alle, bldg. 130, DK-8000 Aarhus, Denmark. Phone: 4589422614. Fax: 4586196500. E-mail: fsp{at}mb.au.dk

Published ahead of print on 22 October 2008.

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