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    Date Issued2019 (1)Author
    Becerra Artiles, Aniuska (1)
    Cruz, John (1)Leszyk, John D. (1)Sette, Alessandro (1)Shaffer, Scott A. (1)View MoreUMass Chan AffiliationDepartment of Biochemistry and Molecular Pharmacology (1)Department of Pathology (1)Mass Spectrometry Facility (1)Document TypeJournal Article (1)KeywordAmino Acids, Peptides, and Proteins (1)CD4 T cells (1)Cells (1)cytotoxicity (1)Enzymes and Coenzymes (1)View MoreJournalEuropean journal of immunology (1)

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    Naturally processed HLA-DR3-restricted HHV-6B peptides are recognized broadly with polyfunctional and cytotoxic CD4 T-cell responses

    Becerra Artiles, Aniuska; Cruz, John; Leszyk, John D.; Sidney, John; Sette, Alessandro; Shaffer, Scott A.; Stern, Lawrence J. (2019-08-01)
    Human herpes virus 6B (HHV-6B) is a widespread virus that infects most people early in infancy and establishes a chronic life-long infection with periodic reactivation. CD4 T cells have been implicated in control of HHV-6B, but antigenic targets and functional characteristics of the CD4 T-cell response are poorly understood. We identified 25 naturally processed MHC-II peptides, derived from six different HHV-6B proteins, and showed that they were recognized by CD4 T-cell responses in HLA-matched donors. The peptides were identified by mass spectrometry after elution from HLA-DR molecules isolated from HHV-6B-infected T cells. The peptides showed strong binding to matched HLA alleles and elicited recall T-cell responses in vitro. T-cell lines expanded in vitro were used for functional characterization of the response. Responding cells were mainly CD3(+) CD4(+) , produced IFN-gamma, TNF-alpha, and low levels of IL-2, alone or in combination, highlighting the presence of polyfunctional T cells in the overall response. Many of the responding cells mobilized CD107a, stored granzyme B, and mediated specific killing of peptide-pulsed target cells. These results highlight a potential role for polyfunctional cytotoxic CD4 T cells in the long-term control of HHV-6B infection.
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