IL-15 trans-presentation promotes human NK cell development and differentiation in vivo

Open Access
Authors
  • N.D. Huntington
  • N. Legrand
  • N.L. Alves
  • B. Jaron
  • K. Weijer
  • A. Plet
  • E. Corcuff
  • E. Mortier
  • Y. Jacques
  • H. Spits
  • J.P. Di Santo
Publication date 2009
Journal Journal of Experimental Medicine
Volume | Issue number 206 | 1
Pages (from-to) 25-34
Organisations
  • Faculty of Medicine (AMC-UvA)
Abstract
The in vivo requirements for human natural killer (NK) cell development and differentiation into cytotoxic effectors expressing inhibitory receptors for self-major histocompatability complex class I (MHC-I; killer Ig-like receptors [KIRs]) remain undefined. Here, we dissect the role of interleukin (IL)-15 in human NK cell development using Rag2(-/-)gamma c(-/-) mice transplanted with human hematopoietic stem cells. Human NK cell reconstitution was intrinsically low in this model because of the poor reactivity to mouse IL-15. Although exogenous human IL-15 (hIL-15) alone made little improvement, IL-15 coupled to IL-15 receptor alpha (IL-15R alpha) significantly augmented human NK cells. IL-15-IL-15R alpha complexes induced extensive NK cell proliferation and differentiation, resulting in accumulation of CD16(+)KIR(+)NK cells, which was not uniquely dependent on enhanced survival or preferential responsiveness of this subset to IL-15. Human NK cell differentiation in vivo required hIL-15 and progressed in a linear fashion from CD56(hi)CD(16)(-)KIR(-) to CD56(lo)CD16(+)KIR(-), and finally to CD56(lo)CD16(+)KIR(+). These data provide the first evidence that IL-15 trans-presentation regulates human NK cell homeostasis. Use of hIL-15 receptor agonists generates a robust humanized immune system model to study human NK cells in vivo. IL-15 receptor agonists may provide therapeutic tools to improve NK cell reconstitution after bone marrow transplants, enhance graft versus leukemia
Document type Article
Published at https://doi.org/10.1084/jem.20082013
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