Regulation of memory CD4+ T-cell generation by intrinsic and extrinsic IL-27 signaling during malaria infection.

IF 4.8 4区 医学 Q2 IMMUNOLOGY International immunology Pub Date : 2024-11-14 DOI:10.1093/intimm/dxae039
Sanjaadorj Tsogtsaikhan, Shin-Ichi Inoue, Ganchimeg Bayarsaikhan, Maria Lourdes Macalinao, Daisuke Kimura, Mana Miyakoda, Masahiro Yamamoto, Hiromitsu Hara, Hiroki Yoshida, Katsuyuki Yui
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Abstract

The generation and maintenance of memory T cells are regulated by various factors, including cytokines. Previous studies have shown that IL-27 is produced during the early acute phase of Plasmodium chabaudi chabaudi AS (Pcc) infection and inhibits the development of Th1-type memory CD4+ T cells. However, whether IL-27 acts directly on its receptor on Plasmodium-specific CD4+ T cells or indirectly via its receptor on other immune cells remains unclear. We aimed to determine the role of IL-27 receptor signaling in different immune cell types in regulating the generation and phenotype of memory CD4+ T cells during Plasmodium infection. We utilized Plasmodium-specific T-cell antigen receptor (TCR) transgenic mice, PbT-II, and Il27rα-/- mice to assess the direct and indirect effects of IL-27 signaling on memory CD4+ T-cell generation. Mice were transferred with PbT-II or Il27rα-/- PbT-II cells and infected with Pcc. Conditional knockout mice lacking the IL-27 receptor in T cells or dendritic cells were employed to discern the specific immune cell types involved in IL-27 receptor signaling. High levels of memory in PbT-II cells with Th1-shift occurred only when both PbT-II and host cells lacked the IL-27 receptor, suggesting the predominant inhibitory role of IL-27 signaling in both cell types. Furthermore, IL-27 receptor signaling in T cells limited the number of memory CD4+ T cells, while signaling in both T and dendritic cells contributed to the Th1 dominance of memory CD4+ T cells. These findings underscore the complex cytokine signaling network regulating memory CD4+ T cells during Plasmodium infection.

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在疟疾感染过程中,IL-27 的内在和外在信号调节记忆 CD4+ T 细胞的生成。
记忆 T 细胞的生成和维持受多种因素(包括细胞因子)的调控。先前的研究表明,IL-27 在沙鲍迪疟原虫(Pcc)感染的早期急性期产生,并抑制 Th1 型记忆 CD4+ T 细胞的发育。然而,IL-27是直接作用于其在疟原虫特异性CD4+ T细胞上的受体,还是间接通过其在其他免疫细胞上的受体发挥作用,目前仍不清楚。我们的目的是确定在疟原虫感染期间,IL-27 受体信号在不同免疫细胞类型中调节记忆 CD4+ T 细胞的生成和表型的作用。我们利用疟原虫特异性 TCR 转基因小鼠 PbT-II 和 Il27rα-/- 小鼠来评估 IL-27 信号传导对记忆 CD4+ T 细胞生成的直接和间接影响。用 PbT-II 或 Il27rα-/- PbT-II 细胞转移小鼠并用 Pcc 感染。利用T细胞或树突状细胞中缺乏IL-27受体的条件性基因敲除小鼠来确定参与IL-27受体信号转导的特定免疫细胞类型。只有当 PbT-II 细胞和宿主细胞都缺乏 IL-27 受体时,PbT-II 细胞才会出现高水平的 Th1 转移记忆,这表明 IL-27 信号在两种细胞类型中都起着主要的抑制作用。此外,T细胞中的IL-27受体信号限制了记忆CD4+ T细胞的数量,而T细胞和树突状细胞中的信号则导致记忆CD4+ T细胞的Th1优势。这些发现强调了在疟原虫感染期间调节记忆CD4+ T细胞的复杂细胞因子信号网络。
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来源期刊
International immunology
International immunology 医学-免疫学
CiteScore
9.30
自引率
2.30%
发文量
51
审稿时长
6-12 weeks
期刊介绍: International Immunology is an online only (from Jan 2018) journal that publishes basic research and clinical studies from all areas of immunology and includes research conducted in laboratories throughout the world.
期刊最新文献
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