Beschreibung:
<jats:title>Abstract</jats:title><jats:p>It is well known that regulatory T‐cells (Tregs) are required to prevent autoimmunity, but they may also have some less‐well understood immune‐stimulatory effects. In particular, in CD8<jats:sup>+</jats:sup> T‐cell responses Tregs select high‐affinity clones upon priming and promote memory by inhibiting inflammation‐dependent generation of short‐lived effector cells. In the current issue of the <jats:italic>European Journal of Immunology</jats:italic> [Eur. J. Immunol. 2023. 53: <jats:ext-link xmlns:xlink="http://www.w3.org/1999/xlink" xlink:href="https://onlinelibrary.wiley.com/doi/10.1002/eji.202149400">2149400</jats:ext-link>], Madi et al. report the surprising finding that human and murine FOXP3<jats:sup>+</jats:sup> Tregs are a physiologically relevant source of IL‐15, a homeostatic cytokine that promotes antigen‐independent maintenance of CD8<jats:sup>+</jats:sup> memory T‐cells. In mice that lack IL‐15 selectively in FOXP3<jats:sup>+</jats:sup>Tregs the authors show that the composition of the CD8<jats:sup>+</jats:sup> T‐cell memory pool is altered in the absence of Treg‐derived IL‐15, since a subset of terminally effector memory cells is drastically reduced. Otherwise Treg‐derived IL‐15 is dispensable for antiviral immune responses and the generation of anti‐viral CD8<jats:sup>+</jats:sup> memory T‐cells. These findings add to our understanding of the multifaceted role of Tregs in immune responses, and how IL‐15 derived from different cellular sources maintains anti‐viral T‐cell memory.</jats:p>