In vivo effects of a recombinant vaccinia virus expressing a mouse mammary tumor virus superantigen

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J. Virol., May 1996, 3026-3031, Vol 70, No. 5
Copyright © 1996, American Society for Microbiology

In vivo effects of a recombinant vaccinia virus expressing a mouse mammary tumor virus superantigen

C Krummenacher, H Diggelmann and H Acha-Orbea
Institute for Microbiology, University of Lausanne, Switzerland.

Early after infection, the mouse mammary tumor virus (MMTV) expresses a superantigen (SAg) at the surface of B lymphocytes. Interaction with the T-cell receptor Vbeta domain induces a polyclonal proliferative response of the SAg-reactive T cells. Stimulated T cells become anergic and are deleted from the T-cell repertoire. We have used a recombinant vaccinia virus encoding the MMTV(GR) SAg to dissect the effects of the retroviral SAg during an unrelated viral infection. Subcutaneous infection with this recombinant vaccinia virus induces a very rapid increase of Vbeta14 T cells in the draining lymph node. This stimulation does not require a large Plumber of infectious particles and is not strictly dependent on the expression of the major histocompatibility complex class II I-E molecule, as it is required after MMTV(GR) infection. In contrast to MMTV infection during which B cells are infected, we do not observe any clonal deletion of the reactive T cells following the initial stimulation phase. Our data show that contrary to the case with MMTV, macrophages but not B cells are the targets of infection by vaccinia virus in the lymph node, indicating the ability of these cells to present a retroviral SAg. The altered SAg expression in a different target cell observed during recombinant vaccinia virus infection therefore results in significant changes in the SAg response.

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Wirth, S., Vessaz, A., Krummenacher, C., Baribaud, F., Acha-Orbea, H., Diggelmann, H. (2002). Regions of Mouse Mammary Tumor Virus Superantigen Involved in Interaction with the Major Histocompatibility Complex Class II I-A Molecule. J. Virol. 76: 11172-11175 [Abstract] [Full Text]
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Clin. Vaccine Immunol.	ALL ASM JOURNALS