T-bet and Eomes instruct the development of two distinct natural killer cell lineages in the liver and in the bone marrow

نویسندگان

  • Cécile Daussy
  • Fabrice Faure
  • Katia Mayol
  • Sébastien Viel
  • Georg Gasteiger
  • Emily Charrier
  • Jacques Bienvenu
  • Thomas Henry
  • Emilie Debien
  • Uzma A. Hasan
  • Jacqueline Marvel
  • Keigyou Yoh
  • Satoru Takahashi
  • Immo Prinz
  • Simon de Bernard
  • Laurent Buffat
  • Thierry Walzer
چکیده

Trail(+)DX5(-)Eomes(-) natural killer (NK) cells arise in the mouse fetal liver and persist in the adult liver. Their relationships with Trail(-)DX5(+) NK cells remain controversial. We generated a novel Eomes-GFP reporter murine model to address this question. We found that Eomes(-) NK cells are not precursors of classical Eomes(+) NK cells but rather constitute a distinct lineage of innate lymphoid cells. Eomes(-) NK cells are strictly dependent on both T-bet and IL-15, similarly to NKT cells. We observed that, in the liver, expression of T-bet in progenitors represses Eomes expression and the development of Eomes(+) NK cells. Reciprocally, the bone marrow (BM) microenvironment restricts T-bet expression in developing NK cells. Ectopic expression of T-bet forces the development of Eomes(-) NK cells, demonstrating that repression of T-bet is essential for the development of Eomes(+) NK cells. Gene profile analyses show that Eomes(-) NK cells share part of their transcriptional program with NKT cells, including genes involved in liver homing and NK cell receptors. Moreover, Eomes(-) NK cells produce a broad range of cytokines, including IL-2 and TNF in vitro and in vivo, during immune responses against vaccinia virus. Thus, mutually exclusive expression of T-bet and Eomes drives the development of different NK cell lineages with complementary functions.

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عنوان ژورنال:

دوره 211  شماره 

صفحات  -

تاریخ انتشار 2014