IL-2 receptor signaling is essential for the development of Klrg1+ terminally differentiated T regulatory cells.

نویسندگان

  • Guoyan Cheng
  • Xiaomei Yuan
  • Matthew S Tsai
  • Eckhard R Podack
  • Aixin Yu
  • Thomas R Malek
چکیده

Thymic-derived natural T regulatory cells (Tregs) are characterized by functional and phenotypic heterogeneity. Recently, a small fraction of peripheral Tregs has been shown to express Klrg1, but it remains unclear as to what extent Klrg1 defines a unique Treg subset. In this study, we show that Klrg1(+) Tregs represent a terminally differentiated Treg subset derived from Klrg1(-) Tregs. This subset is a recent Ag-responsive and highly activated short-lived Treg population that expresses enhanced levels of Treg suppressive molecules and that preferentially resides within mucosal tissues. The development of Klrg1(+) Tregs also requires extensive IL-2R signaling. This activity represents a distinct function for IL-2, independent from its contribution to Treg homeostasis and competitive fitness. These and other properties are analogous to terminally differentiated short-lived CD8(+) T effector cells. Our findings suggest that an important pathway driving Ag-activated conventional T lymphocytes also operates for Tregs.

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عنوان ژورنال:
  • Journal of immunology

دوره 189 4  شماره 

صفحات  -

تاریخ انتشار 2012