Author: ["Colby Zaph","Jude Uzonna","Stephen M Beverley","Phillip Scott"]
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Abstract
Infection with Leishmania major induces a protective immune response and long-term resistance to reinfection, which is thought to depend upon persistent parasites. Here we demonstrate that although effector CD4+ T cells are lost in the absence of parasites, central memory CD4+ T cells are maintained. Upon secondary infection, these central memory T cells become tissue-homing effector T cells and mediate protection. Thus, immunity to L. major is mediated by at least two distinct populations of CD4+ T cells: short-lived pathogen-dependent effector cells and long-lived pathogen-independent central memory cells. These data suggest that central memory T cells should be the targets for nonlive vaccines against infectious diseases requiring cell-mediated immunity.
Cite this article
Zaph, C., Uzonna, J., Beverley, S. et al. Central memory T cells mediate long-term immunity to Leishmania major in the absence of persistent parasites. Nat Med 10, 1104–1110 (2004). https://doi.org/10.1038/nm1108