4.7 Article

Programs for the persistence, vigilance and control of human CD8+ lung-resident memory T cells

Journal

NATURE IMMUNOLOGY
Volume 17, Issue 12, Pages 1467-1478

Publisher

NATURE PUBLISHING GROUP
DOI: 10.1038/ni.3589

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Funding

  1. Landsteiner Stichting voor Bloedtransfusie Research [1136]
  2. Netherlands Asthma Foundation [3.2.06.020]
  3. Alexander von Humboldt Foundation
  4. Netherlands organization for scientific research (NWO-ALW)

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Tissue-resident memory T cells (TRM cells) in the airways mediate protection against respiratory infection. We characterized TRM cells expressing integrin alpha(E) (CD103) that reside within the epithelial barrier of human lungs. These cells had specialized profiles of chemokine receptors and adhesion molecules, consistent with their unique localization. Lung TRM cells were poised for rapid responsiveness by constitutive expression of deployment-ready mRNA encoding effector molecules, but they also expressed many inhibitory regulators, suggestive of programmed restraint. A distinct set of transcription factors was active in CD103(+) TRM cells, including Notch. Genetic and pharmacological experiments with mice revealed that Notch activity was required for the maintenance of CD103(+) T-RM cells. We have thus identified specialized programs underlying the residence, persistence, vigilance and tight control of human lung TRM cells.

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