Interleukin-27 signalling induces stem cell antigen-1 expression in T lymphocytes in vivo.

白细胞介素-27信号传导在体内诱导T淋巴细胞中干细胞抗原-1的表达

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作者:Liu Zhihao, Wu Lisha, Zhu Jing, Zhu Xiaotong, Zhu Jianmin, Liu Jin-Qing, Zhang Jianchao, Davis Jonathan P, Varikuti Sanjay, Satoskar Abhay R, Zhou Jie, Li Ming-Song, Bai Xue-Feng
Stem cell antigen-1 (Sca-1/Ly6A/E) is a cell surface glycoprotein that is often used as a biomarker for stem cells and cell stemness. However, it is not clear what factors can directly induce the expression of Sca-1/Ly6A/E in T lymphocytes in vivo, and if induction of Sca-1 is associated with T cell stemness. In this study, we show that interleukin-27 (IL-27), a member of the IL-12 family of cytokines, directly induces Sca-1 expression in T cells in vivo. We found that mice-deficient for IL-27 (either P28 or EBI3) or its signalling (IL-27Rα) had profound reduction of Sca-1 expression in naive (CD62L(+)  CD44(-) ), memory (CD62L(+)  CD44(+) ) and effector (CD62L(-)  CD44(+) ) T cells. In contrast, in vivo delivery of IL-27 using adeno-associated viral vectors strongly induced the expression of Sca-1 in naive and memory/effector T-cell populations in an IL-27 receptor- or signal transducer and activator of transcription 1-dependent manner. Interestingly, IL-27-induced Sca-1(+) T cells do not express or up-regulate classic stem cell-associated genes such as Nanog, Oct4, Sox2 and Ctnnb1. However, IL-27-induced Sca-1(+) T cells had increased expression of effector/memory-associated transcription factor T-bet, Eomes and Blimp1. Hence, IL-27 signalling directly induces the expression of Sca-1/Ly6A/E expression in T cells. Direct expansion of Sca-1(+)  CD62L(+)  CD44(-) T memory stem cells may explain why IL-27 enhances T-cell memory.

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