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KMID : 0923620210210050033
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Immune Network
2021 Volume.21 No. 5 p.33 ~ p.33
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Induction of Unique STAT Heterodimers by IL-21 Provokes IL-1RI Expression on CD8+ T Cells, Resulting in Enhanced IL-1¥â Dependent Effector Function
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Kim Dong-Hyun
Kim Hee-Young
Lee Won-Woo
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Abstract
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IL-1¥â plays critical roles in the priming and effector phases of immune responses such as the differentiation, commitment, and memory formation of T cells. In this context, several reports have suggested that the IL-1¥â signal is crucial for CTL-mediated immune responses to viral infections and tumors. However, little is known regarding whether IL-1¥â acts directly on CD8+ T cells and what the molecular mechanisms underlying expression of IL-1 receptors (IL-1Rs) on CD8+ T cells and features of IL-1R+CD8+ T cells are. Here, we provide evidence that the expression of IL-1R type I (IL-1RI), the functional receptor of IL-1¥â, is preferentially induced by IL-21 on TCR-stimulated CD8+ T cells. Further, IL-1¥â enhances the effector function of CD8+ T cells expressing IL-21-induced IL-1RI by increasing cytokine production and release of cytotoxic granules containing granzyme B. The IL-21-IL-1RI-IL-1¥â axis is involved in an augmented effector function through regulation of transcription factors BATF, Blimp-1, and IRF4. Moreover, this axis confers a unique effector function to CD8+ T cells compared to conventional type 1 cytotoxic T cells differentiated with IL-12. Chemical inhibitor and immunoprecipitation assay demonstrated that IL-21 induces a unique pattern of STAT activation with the formation of both STAT1:STAT3 and STAT3:STAT5 heterodimers, which are critical for the induction of IL-1RI on TCR-stimulated CD8+ T cells. Taken together, we propose that induction of a novel subset of IL-1RI-expressing CD8+ T cells by IL-21 may be beneficial to the protective immune response against viral infections and is therefore important to consider for vaccine design.
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KEYWORD
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IL-1 Receptor, IL-1 Beta, IL-21, Cytotoxic T Lymphocyte, STAT transcription factors, Tc1 cells
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