Fas Ligand-mediated cytotoxicity of CD4+ T cells during chronic retrovirus infection

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作者
Anna Malyshkina
Elisabeth Littwitz-Salomon
Kathrin Sutter
Gennadiy Zelinskyy
Sonja Windmann
Simone Schimmer
Annette Paschen
Hendrik Streeck
Kim J. Hasenkrug
Ulf Dittmer
机构
[1] University Hospital Essen,Institute for Virology
[2] University of Duisburg-Essen,Department of Dermatology, Venereology, and Allergology
[3] University Hospital Essen,Institute for HIV Research
[4] University of Duisburg-Essen,Laboratory of Persistent Viral Diseases, Rocky Mountain Laboratories
[5] University Hospital Essen,undefined
[6] University Duisburg-Essen,undefined
[7] National Institute of Allergy and Infectious Diseases,undefined
[8] National Institutes of Health,undefined
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CD4+ helper T cells and cytotoxic CD8+ T cells are key players for adaptive immune responses against acute infections with retroviruses. Similar to textbook knowledge the most important function of CD4+ T cells during an acute retrovirus infection seems to be their helper function for other immune cells. Whereas there was no direct anti-viral activity of CD4+ T cells during acute Friend Virus (FV) infection, they were absolutely required for the control of chronic infection. During chronic FV infection a population of activated FV-specific CD4+ T cells did not express cytotoxic molecules, but Fas Ligand that can induce Fas-induced apoptosis in target cells. Using an MHC II-restricted in vivo CTL assay we demonstrated that FV-specific CD4+ T cells indeed mediated cytotoxic effects against FV epitope peptide loaded targets. CD4 + CTL killing was also detected in FV-infected granzyme B knockout mice confirming that the exocytosis pathway was not involved. However, killing could be blocked by antibodies against FasL, which identified the Fas/FasL pathway as critical cytotoxic mechanism during chronic FV infection. Interestingly, targeting the co-stimulatory receptor CD137 with an agonistic antibody enhanced CD4+ T cell cytotoxicity. This immunotherapy may be an interesting new approach for the treatment of chronic viral infections.
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