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Publication : Skin-resident CD4+ T cells protect against Leishmania major by recruiting and activating inflammatory monocytes.

First Author  Glennie ND Year  2017
Journal  PLoS Pathog Volume  13
Issue  4 Pages  e1006349
PubMed ID  28419151 Mgi Jnum  J:245720
Mgi Id  MGI:5915858 Doi  10.1371/journal.ppat.1006349
Citation  Glennie ND, et al. (2017) Skin-resident CD4+ T cells protect against Leishmania major by recruiting and activating inflammatory monocytes. PLoS Pathog 13(4):e1006349
abstractText  Tissue-resident memory T cells are required for establishing protective immunity against a variety of different pathogens, although the mechanisms mediating protection by CD4+ resident memory T cells are still being defined. In this study we addressed this issue with a population of protective skin-resident, IFNgamma-producing CD4+ memory T cells generated following Leishmania major infection. We previously found that resident memory T cells recruit circulating effector T cells to enhance immunity. Here we show that resident memory CD4+ T cells mediate the delayed-hypersensitivity response observed in immune mice and provide protection without circulating T cells. This protection occurs rapidly after challenge, and requires the recruitment and activation of inflammatory monocytes, which limit parasites by production of both reactive oxygen species and nitric oxide. Overall, these data highlight a novel role for tissue-resident memory cells in recruiting and activating inflammatory monocytes, and underscore the central role that skin-resident T cells play in immunity to cutaneous leishmaniasis.
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