IL-27 promotes Treg cell expression of CD122 and fitness at homeostasis

2025 Proceedings of the National Academy of Sciences 0 citations

Abstract

Regulatory T (Treg) cells express high levels of the IL-27R, and in the setting of infection and autoimmunity, the cytokine IL-27 promotes Treg cell activities that mitigate tissue pathology. However, IL-27 appears dispensable for Treg cell development and maintenance as lineage-specific depletion of the IL-27R on Treg cells does not impact these populations at steady state. In contrast, when mice were generated in which the Treg compartment comprised a mix of IL-27R-sufficient and -deficient Treg cells, those that lacked IL-27R were at a competitive disadvantage. Aging experiments illustrate that IL-27R-deficient Treg cells are preferentially eroded, and this defect was associated with reduced expression of CD122, the β chain of the IL-2/15R. Moreover, blockade of CD122 led to a similar loss of Treg cells, and in vitro and in vivo studies highlight that IL-27 promotes Treg cell expression of CD122 and improves responsiveness to IL-2/15. These datasets reveal that homeostatic IL-27 signals provide a competitive advantage that shapes the composition of the Treg cell pool by modulating responsiveness to growth factors.

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Year
2025
Type
article
Volume
122
Issue
50
Pages
e2519141122-e2519141122
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0
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Zachary Lanzar, Daniel L. Aldridge, Elisa Cruz-Morales et al. (2025). IL-27 promotes Treg cell expression of CD122 and fitness at homeostasis. Proceedings of the National Academy of Sciences , 122 (50) , e2519141122-e2519141122. https://doi.org/10.1073/pnas.2519141122

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DOI
10.1073/pnas.2519141122