Essential and non-overlapping IL-2Rα-dependent processes for thymic development and peripheral homeostasis of regulatory T cells

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作者
Kevin H. Toomer
Jen Bon Lui
Norman H. Altman
Yuguang Ban
Xi Chen
Thomas R. Malek
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[1] University of Miami,Department of Microbiology and Immunology, Miller School of Medicine
[2] University of Miami,Department of Pathology, Miller School of Medicine
[3] University of Miami,Sylvester Comprehensive Cancer Center, Miller School of Medicine
[4] University of Miami,Department of Public Health Sciences, Miller School of Medicine
[5] University of Miami,Diabetes Research Institute, Miller School of Medicine
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IL-2R signaling is essential for regulatory T cell (Treg) function. However, the precise contribution of IL-2 during Treg thymic development, peripheral homeostasis and lineage stability remains unclear. Here we show that IL-2R signaling is required by thymic Tregs at an early step for expansion and survival, and a later step for functional maturation. Using inducible, conditional deletion of CD25 in peripheral Tregs, we also find that IL-2R signaling is indispensable for Treg homeostasis, whereas Treg lineage stability is largely IL-2-independent. CD25 knockout peripheral Tregs have increased apoptosis, oxidative stress, signs of mitochondrial dysfunction, and reduced transcription of key enzymes of lipid and cholesterol biosynthetic pathways. A divergent IL-2R transcriptional signature is noted for thymic Tregs versus peripheral Tregs. These data indicate that IL-2R signaling in the thymus and the periphery leads to distinctive effects on Treg function, while peripheral Treg survival depends on a non-conventional mechanism of metabolic regulation.
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