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利用命运报告小鼠绘制稳态和自身免疫性神经炎症中免疫细胞产生粒细胞-巨噬细胞集落刺激因子的情况。

GM-CSF production by immune cells in steady state and autoimmune neuroinflammation mapped using fate reporting mice.

作者信息

Azizi Gholamreza, Rasouli Javad, Naziri Hamed, Gonzalez Michael V, Garifallou James, Zhang Guang-Xian, Ciric Bogoljub, Rostami Abdolmohamad

出版信息

bioRxiv. 2025 Apr 26:2025.04.23.650273. doi: 10.1101/2025.04.23.650273.

Abstract

The full GM-CSF expression spectrum in immune cells remains unclear, while CD4□ T cells are the primary source. Using novel GM-CSF reporter/fate reporter transgenic mice, we tracked ongoing and past (YFP ) GM-CSF expression in various immune cells. GM-CSF was produced by diverse immune cells, including CD4 , CD8 , γδ T, NK, B, and CD11b cells, with expression patterns varying by cell type and organ with liver CD4 T cells and NK cells showing the highest expression history in both naïve and mice with EAE. GM-CSF expression was transient and permanently lost in most cells over time. In a mouse model of multiple sclerosis, effector memory CD4□ T cells were the dominant CNS GM-CSF source, with higher expression than in other organs. CD4 YFP T cells, strongly expressing CXCR6, produced multiple cytokines. Transcriptomic analysis showed distinct gene expression profiles in effector memory CD4 T cells compared to naïve cells. YFP□ Tregs represent functionally distinct subsets mirroring effector Th cells, expressing cytokines associated with Th lineages, especially during neuroinflammation. These findings identified distinct GM-CSF cellular sources across organs, highlighting a transient tissue microenvironment influence on GM-CSF production linked to CXCR6 expression.

摘要

免疫细胞中GM-CSF的完整表达谱尚不清楚,而CD4⁺ T细胞是主要来源。我们使用新型GM-CSF报告基因/命运报告基因转基因小鼠,追踪了各种免疫细胞中正在进行的和过去的(YFP⁺)GM-CSF表达。GM-CSF由多种免疫细胞产生,包括CD4⁺、CD8⁺、γδ T、NK、B和CD11b⁺细胞,其表达模式因细胞类型和器官而异,肝脏中的CD4⁺ T细胞和NK细胞在未免疫小鼠和患有实验性自身免疫性脑脊髓炎(EAE)的小鼠中均显示出最高的表达历史。随着时间的推移,GM-CSF表达是短暂的,并且在大多数细胞中会永久丧失。在多发性硬化症小鼠模型中,效应记忆CD4⁺ T细胞是中枢神经系统GM-CSF的主要来源,其表达高于其他器官。强烈表达CXCR6的CD4⁺ YFP⁺ T细胞可产生多种细胞因子。转录组分析显示,与幼稚细胞相比,效应记忆CD4⁺ T细胞具有不同的基因表达谱。YFP⁺调节性T细胞(Tregs)代表功能上不同的亚群,反映效应性Th细胞,表达与Th谱系相关的细胞因子,尤其是在神经炎症期间。这些发现确定了不同器官中GM-CSF的不同细胞来源,突出了短暂的组织微环境对与CXCR6表达相关的GM-CSF产生的影响。

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