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Skin-resident memory CD4+ T cells enhance protection against Leishmania major infection.


ABSTRACT: Leishmaniasis causes a significant disease burden worldwide. Although Leishmania-infected patients become refractory to reinfection after disease resolution, effective immune protection has not yet been achieved by human vaccines. Although circulating Leishmania-specific T cells are known to play a critical role in immunity, the role of memory T cells present in peripheral tissues has not been explored. Here, we identify a population of skin-resident Leishmania-specific memory CD4+ T cells. These cells produce IFN-? and remain resident in the skin when transplanted by skin graft onto naive mice. They function to recruit circulating T cells to the skin in a CXCR3-dependent manner, resulting in better control of the parasites. Our findings are the first to demonstrate that CD4+ TRM cells form in response to a parasitic infection, and indicate that optimal protective immunity to Leishmania, and thus the success of a vaccine, may depend on generating both circulating and skin-resident memory T cells.

SUBMITTER: Glennie ND 

PROVIDER: S-EPMC4548053 | biostudies-literature | 2015 Aug

REPOSITORIES: biostudies-literature

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Skin-resident memory CD4+ T cells enhance protection against Leishmania major infection.

Glennie Nelson D ND   Yeramilli Venkata A VA   Beiting Daniel P DP   Volk Susan W SW   Weaver Casey T CT   Scott Phillip P  

The Journal of experimental medicine 20150727 9


Leishmaniasis causes a significant disease burden worldwide. Although Leishmania-infected patients become refractory to reinfection after disease resolution, effective immune protection has not yet been achieved by human vaccines. Although circulating Leishmania-specific T cells are known to play a critical role in immunity, the role of memory T cells present in peripheral tissues has not been explored. Here, we identify a population of skin-resident Leishmania-specific memory CD4+ T cells. Thes  ...[more]

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