[HTML][HTML] Resident Memory T Cells (TRM) Are Abundant in Human Lung: Diversity, Function, and Antigen Specificity

R Purwar, J Campbell, G Murphy, WG Richards… - PloS one, 2011 - journals.plos.org
R Purwar, J Campbell, G Murphy, WG Richards, RA Clark, TS Kupper
PloS one, 2011journals.plos.org
Recent studies have shown that tissue resident memory T cells (TRM) are critical to antiviral
host defense in peripheral tissues. This new appreciation of TRM that reside in epithelial
tissues and mediate host defense has been studied most extensively in skin: adult human
skin contains large numbers of functional TRM that express skin specific markers. Indeed,
more than twice as many T cells reside in skin as in peripheral blood. This T cell population
has a diverse T cell receptor repertoire, and can produce a broad array of cytokines. More …
Recent studies have shown that tissue resident memory T cells (TRM) are critical to antiviral host defense in peripheral tissues. This new appreciation of TRM that reside in epithelial tissues and mediate host defense has been studied most extensively in skin: adult human skin contains large numbers of functional TRM that express skin specific markers. Indeed, more than twice as many T cells reside in skin as in peripheral blood. This T cell population has a diverse T cell receptor repertoire, and can produce a broad array of cytokines. More recently, we have begun to examine other epithelial tissues for the presence of resident T cells. In the present study, we asked whether analogous populations of resident T cells could be found in human lung. We were able to demonstrate abundant resident T cells in human lung-more than 10 billion T cells were present. Lung T cells were largely of the effector memory T cell (TEM) phenotype, though small numbers of central memory T cells (TCM) and T regulatory cells (Treg) could be identified. Lung T cells had a diverse T cell receptor repertoire and subsets produced IL-17, IL-4, IFNγ, as well as TNFα. A significant number of lung TRM CD4+Th cells produced more than one cytokine, identifying them as “multifunctional” Th1 type cells. Finally, lung TRM, but not TRM resident to skin or T cells from blood, proliferated in response to influenza virus. This work suggests that normal human lung contains large numbers of TRM cells, and these cells are poised to respond to recall antigens previously encountered through lung mucosa. This population of T cells may contribute to the pathogenesis of asthma and other T cell mediated lung diseases.
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