4.6 Article

Tissue Distribution of Memory T and B Cells in Rhesus Monkeys following Influenza A Infection

Journal

JOURNAL OF IMMUNOLOGY
Volume 195, Issue 9, Pages 4378-4386

Publisher

AMER ASSOC IMMUNOLOGISTS
DOI: 10.4049/jimmunol.1501702

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Funding

  1. National Institutes of Health
  2. National Institute of Allergy and Infectious Diseases [Y1-AI-5026-01]
  3. Thailand Research Fund [BRG5880003]
  4. Ratchadapisek endowment

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Studies of influenza-specific immune responses in humans have largely assessed systemic responses involving serum Ab and peripheral blood T cell responses. However, recent evidence indicates that tissue-resident memory T (T-RM) cells play an important role in local murine intrapulmonary immunity. Rhesus monkeys were pulmonary exposed to 2009 pandemic H1N1 virus at days 0 and 28 and immune responses in different tissue compartments were measured. All animals were asymptomatic postinfection. Although only minimal memory immune responses were detected in peripheral blood, a high frequency of influenza nucleoprotein-specific memory T cells was detected in the lung at the contraction phase, 49-58 d after second virus inoculation. A substantial proportion of lung nucleoprotein-specific memory CD8(+) T cells expressed CD103 and CD69, phenotypic markers of T-RM cells. Lung CD103(+) and CD103(-) memory CD8(+) T cells expressed similar levels of IFN-gamma and IL-2. Unlike memory T cells, spontaneous Ab secreting cells and memory B cells specific to influenza hemagglutinin were primarily observed in the mediastinal lymph nodes. Little difference in systemic and local immune responses against influenza was observed between young adult (6-8 y) and old animals (18-28 y). Using a nonhuman primate model, we revealed substantial induction of local T and B cell responses following 2009 pandemic H1N1 infection. Our study identified a subset of influenza-specific lung memory T cells characterized as T-RM cells in rhesus monkeys. The rhesus monkey model may be useful to explore the role of TRM cells in local tissue protective immunity after rechallenge and vaccination.

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