Impairment of Gal-9 and Tim-3 crosstalk between Tregs and Th17 cells drives tobacco smoke-induced airway inflammation

IF 4.9 3区 医学 Q2 IMMUNOLOGY
Immunology Pub Date : 2024-06-03 DOI:10.1111/imm.13820
Shilin Qiu, Guang Zhou, Junyi Ke, Jianpeng Zhou, Hui Zhang, Zhitao Jin, Wenli Xie, Shu Huang, Zaiqin He, Huajiao Qin, Hui Huang, Qiuming Li, Hongchun Huang, Haijuan Tang, Yi Liang, Minchao Duan
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引用次数: 0

Abstract

Overexpression of T-cell immunoglobulin and mucin-domain containing-3 (TIM-3) on T cells has been observed in smokers. However, whether and how galectin-9 (Gal-9)/TIM-3 signal between T-regulatory cells (Tregs) and type 17 helper (Th17) cells contributes to tobacco smoke-induced airway inflammation remains unclear. Here, we aimed to explore the role of the Gal-9/TIM-3 signal between Tregs and Th17 cells during chronic tobacco smoke exposure. Tregs phenotype and the expression of TIM-3 on CD4+ T cells were detected in a mouse model of experimental emphysema. The role of TIM-3 in CD4+ T cells was explored in a HAVCR2−/− mouse model and in mice that received recombinant anti-TIM3. The crosstalk between Gal-9 and Tim-3 was evaluated by coculture Tregs with effector CD4+ T cells. We also invested the expression of Gal-9 in Tregs in patients with COPD. Our study revealed that chronic tobacco smoke exposure significantly reduces the frequency of Tregs in the lungs of mice and remarkably shapes the heterogeneity of Tregs by downregulating the expression of Gal-9. We observed a pro-inflammatory but restrained phenotypic transition of CD4+ T cells after tobacco smoke exposure, which was maintained by TIM-3. The restrained phenotype of CD4+ T cells was perturbed when TIM-3 was deleted or neutralised. Tregs from the lungs of mice with emphysema displayed a blunt ability to inhibit the differentiation and proliferation of Th17 cells. The inhibitory function of Tregs was partially restored by using recombinant Gal-9. The interaction between Gal-9 and TIM-3 inhibits the differentiation of Th17 cells and promotes apoptosis of CD4+ T cells, possibly by interfering with the expression of retinoic acid receptor-related orphan receptor gamma t. The expression of Gal-9 in Tregs was reduced in patients with COPD, which was associated with Th17 response and lung function. These findings present a new paradigm that impairment of Gal-9/Tim-3 crosstalk between Tregs and Th17 cells during chronic tobacco smoke exposure promotes tobacco smoke-induced airway/lung inflammation.

Abstract Image

Tregs和Th17细胞之间的Gal-9和Tim-3串联障碍是烟草烟雾诱导气道炎症的驱动因素。
在吸烟者体内观察到T细胞免疫球蛋白和含粘蛋白域-3(TIM-3)在T细胞上过度表达。然而,T调节细胞(Tregs)和17型辅助细胞(Th17)之间的Galectin-9(Gal-9)/TIM-3信号是否以及如何导致烟草烟雾诱导的气道炎症仍不清楚。在此,我们旨在探索在慢性烟草烟雾暴露过程中 Tregs 和 Th17 细胞之间的 Gal-9/TIM-3 信号的作用。在实验性肺气肿小鼠模型中检测了Tregs表型和CD4+ T细胞上TIM-3的表达。在HAVCR2-/-小鼠模型和接受重组抗TIM3的小鼠中探讨了TIM-3在CD4+ T细胞中的作用。通过Tregs与效应CD4+ T细胞的共培养,评估了Gal-9和TIM-3之间的相互影响。我们还研究了慢性阻塞性肺病患者Tregs中Gal-9的表达情况。我们的研究发现,慢性烟草烟雾暴露会显著降低小鼠肺部 Tregs 的频率,并通过下调 Gal-9 的表达显著改变 Tregs 的异质性。我们观察到,在烟草烟雾暴露后,CD4+ T细胞的表型发生了促炎症但受抑制的转变,而这种转变是由TIM-3维持的。当 TIM-3 被删除或中和时,CD4+ T 细胞的抑制表型会受到干扰。来自肺气肿小鼠肺部的Tregs显示出抑制Th17细胞分化和增殖的钝化能力。使用重组 Gal-9 可以部分恢复 Tregs 的抑制功能。Gal-9 和 TIM-3 之间的相互作用抑制了 Th17 细胞的分化,并促进了 CD4+ T 细胞的凋亡,这可能是通过干扰视黄酸受体相关孤儿受体 gamma t 的表达实现的。这些发现提出了一种新的范式,即在慢性烟草烟雾暴露过程中,Tregs和Th17细胞之间的Gal-9/Tim-3串联障碍会促进烟草烟雾诱发的气道/肺部炎症。
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来源期刊
Immunology
Immunology 医学-免疫学
CiteScore
11.90
自引率
1.60%
发文量
175
审稿时长
4-8 weeks
期刊介绍: Immunology is one of the longest-established immunology journals and is recognised as one of the leading journals in its field. We have global representation in authors, editors and reviewers. Immunology publishes papers describing original findings in all areas of cellular and molecular immunology. High-quality original articles describing mechanistic insights into fundamental aspects of the immune system are welcome. Topics of interest to the journal include: immune cell development, cancer immunology, systems immunology/omics and informatics, inflammation, immunometabolism, immunology of infection, microbiota and immunity, mucosal immunology, and neuroimmunology. The journal also publishes commissioned review articles on subjects of topical interest to immunologists, and commissions in-depth review series: themed sets of review articles which take a 360° view of select topics at the heart of immunological research.
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