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Human peripheral blood and bone marrow Epstein–Barr virus‐specific T‐cell repertoire in latent infection reveals distinct memory T‐cell subsets
Authors:Manuel Guerreiro  Il‐Kang Na  Anne Letsch  Doreen Haase  Sandra Bauer  Christian Meisel  Andy Roemhild  Petra Reinke  Hans‐Dieter Volk  Carmen Scheibenbogen
Affiliation:1. Institute of Medical Immunology, Charité Universit?tsmedizin Berlin, Campus Mitte, Berlin, Germany;2. Department of Hematology and Oncology, Charité Universit?tsmedizin Berlin, Campus Benjamin Franklin, Berlin, Germany;3. Department of Nephrology and Internal Intensive Care, Charité Universit?tsmedizin Berlin, Campus Virchow Clinic, Berlin, Germany;4. Berlin‐Brandenburg Center for Regenerative Therapy (BCRT), Charité Universit?tsmedizin Berlin, Berlin, Germany
Abstract:EBV infection leads to life‐long viral persistence. Although EBV infection can result in chronic disease and malignant transformation, most carriers remain disease‐free as a result of effective control by T cells. EBV‐specific IFN‐γ‐producing T cells could be demonstrated in acute and chronic infection as well as during latency. Recent studies, however, provide evidence that assessing IFN‐γ alone is insufficient to assess the quantity and quality of a T‐cell response. Using overlapping peptide pools of latent EBV nuclear antigen 1 and lytic BZLF‐1 protein and multicolor flow cytometry, we demonstrate that the majority of ex vivo EBV‐reactive T cells in healthy virus carriers are indeed IL‐2‐ and/or TNF‐producing memory cells, the latter being significantly more frequent in BM. After in vitro expansion, a substantial number of EBV‐specific CD4+ and CD8+ T cells retained a CC‐chemokine receptor 7 (CCR7)‐positive memory phenotype. Based on their cytokine profiles, six different EBV‐specific T‐cell subsets could be distinguished with TNF‐single or TNF/IL‐2‐double producing cells expressing the highest CCR7 levels resembling early‐differentiated memory T cells. Our study delineates the memory T‐cell profile of a protective immune response and provides a basis for analyzing T‐cell responses in EBV‐associated diseases.
Keywords:BM  EBV  Immune monitoring  Multifunctional T cells  T‐cell memory
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