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Envelope-dependent transactivation by the retroviral oncoprotein v-Rel is required for efficient malignant transformation of chicken spleen cells

Oncogene volume 19pages 3131–3137 (2000)Cite this article

Abstract

The retroviral oncoprotein v-Rel is a chimeric protein that has 11 helper virus-derived Envelope (Env) amino acids (aa) at its N terminus. Within these N-terminal Env aa of v-Rel there are three aa substitutions compared to the Rev-A helper virus Env. These aa substitutions have previously been shown to impart a number of unique properties onto v-Rel, including increased transforming and transactivating ability. In this study, we have analysed the sequence requirements for the Env aa to influence several properties of v-Rel. Phe residues at aa 3 and 9 are critical for an N-terminal transactivation function of v-Rel, and the analysis of several Env mutants demonstrates that transactivation ability parallels the transforming ability of v-Rel. Substitutions of conservative aa, such as leucine and tyrosine, for Phe 3 and 9 are tolerated for transactivation in chicken embryo fibroblasts and for transformation of chicken spleen cells. In contrast, the substitution of 10 Phe residues at the N terminus of v-Rel does not enable transactivation, indicating that a distinct structure surrounding Phe-3 and Phe-9 is essential for v-Rel function. We also show that the addition of the v-Rel Env aa to the N terminus of human c-Rel can enable it to activate transcription. Taken together, these results indicate that Phe residues at positions 3 and 9 have been selected for their ability to enhance the oncogenicity of v-Rel by increasing its ability to activate transcription.

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Acknowledgements

We thank members of our laboratory for critical reading of the manuscript. This work was supported by research grants to TD Gilmore from the National Cancer Institute (CA47763) and the Council for Tobacco Research, and a small grant to EL Dvorin from the Undergraduate Research Opportunities Program of Boston University.J-C Epinat was supported by a fellowship from the Leukemia Research Foundation. EL Dvorin was supported by a Howard Hughes Medical Institute Undergraduate Research Fellowship, and he performed research as part of the Undergraduate Honors Program in Biochemistry & Molecular Biology.

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  1. Jean-Charles Epinat and Evan L Dvorin: J-C Epinat and EL Dvorin contributed equally to the research

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  1. Department of Biology, Boston University, 5 Cummington Street, Boston, 02215-2406, Massachusetts, MA, USA

    Jean-Charles Epinat, Evan L Dvorin & Thomas D Gilmore

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  1. Jean-Charles Epinat
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  2. Evan L Dvorin
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Epinat, JC., Dvorin, E. & Gilmore, T. Envelope-dependent transactivation by the retroviral oncoprotein v-Rel is required for efficient malignant transformation of chicken spleen cells. Oncogene 19, 3131–3137 (2000). https://doi.org/10.1038/sj.onc.1203651

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