Reversible Defects in Natural Killer and Memory Cd8 T Cell Lineages in Interleukin 15–Deficient Mice

نویسندگان

  • Mary K. Kennedy
  • Moira Glaccum
  • Sandra N. Brown
  • Eric A. Butz
  • Joanne L. Viney
  • Monica Embers
  • Naoto Matsuki
  • Keith Charrier
  • Lisa Sedger
  • Cynthia R. Willis
  • Kenneth Brasel
  • Philip J. Morrissey
  • Kim Stocking
  • JoAnn C. L. Schuh
  • Sebastian Joyce
  • Jacques J. Peschon
چکیده

C57BL/6 mice genetically deficient in interleukin 15 (IL-15(-/-) mice) were generated by gene targeting. IL-15(-/-) mice displayed marked reductions in numbers of thymic and peripheral natural killer (NK) T cells, memory phenotype CD8(+) T cells, and distinct subpopulations of intestinal intraepithelial lymphocytes (IELs). The reduction but not absence of these populations in IL-15(-/-) mice likely reflects an important role for IL-15 for expansion and/or survival of these cells. IL-15(-/-) mice lacked NK cells, as assessed by both immunophenotyping and functional criteria, indicating an obligate role for IL-15 in the development and functional maturation of NK cells. Specific defects associated with IL-15 deficiency were reversed by in vivo administration of exogenous IL-15. Despite their immunological defects, IL-15(-/-) mice remained healthy when maintained under specific pathogen-free conditions. However, IL-15(-/-) mice are likely to have compromised host defense responses to various pathogens, as they were unable to mount a protective response to challenge with vaccinia virus. These data reveal critical roles for IL-15 in the development of specific lymphoid lineages. Moreover, the ability to rescue lymphoid defects in IL-15(-/-) mice by IL-15 administration represents a powerful means by which to further elucidate the biological roles of this cytokine.

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عنوان ژورنال:
  • The Journal of Experimental Medicine

دوره 191  شماره 

صفحات  -

تاریخ انتشار 2000