Publication | Open Access
In Vivo Role of Flt3 Ligand and Dendritic Cells in NK Cell Homeostasis
65
Citations
42
References
2010
Year
Nk Cell HomeostasisImmunologyImmunologic MechanismImmune SystemImmunotherapyNatural Killer CellsVivo RoleMature Nk CellsCell SignalingFlt3 LigandAutoimmunityT Cell ImmunityNk Cell DevelopmentCell BiologyTumor MicroenvironmentImmune Cell DevelopmentDendritic Cell BiologyCellular Immune ResponseMedicine
IL-15 is required for NK cell development and homeostasis in vivo. Because IL-15 is presented in trans via its high-affinity IL-15Ralpha-chain to cells expressing the IL-15Rbetagamma complex, we postulated that certain IL-15-bearing cells must be required for NK cell homeostasis. Using IL-15(WT/WT) and IL-15(-/-) mice, bone marrow chimeras with normal cellularity, and a selective depletion of CD11c(hi) dendritic cells (DCs), we demonstrate that ablation of the resting CD11c(hi) DC population results in a highly significant decrease in the absolute number of mature NK cells. In contrast, administration of Flt3 ligand increases the CD11c(hi) DC population, which, when expressing IL-15, significantly expands mature NK cells via enhanced survival and proliferation. In summary, a CD11c(hi) DC population expressing IL-15 is required to maintain NK cell homeostasis under conditions of normal cellularity and also is required to mediate Flt3 ligand-induced NK cell expansion in vivo.
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