TFEB-mediated proinflammatory response in murine macrophages induced by acute Alpha7 nicotinic receptor activation

TFEB 生物 细胞生物学 胆碱能的 炎症 先天免疫系统 自噬 碱性螺旋-环-螺旋-亮氨酸拉链转录因子 免疫系统 转录因子 免疫学 神经科学 生物化学 DNA结合蛋白 基因 细胞凋亡
作者
Havisha H. Honwad,Mehran Najibi,Stuart D.M. Watts,Steven Watts,Accalia Fu,Balázs Koscsó,Milena Bogunovic,Javier E. Irazoqui
出处
期刊:Journal of Leukocyte Biology [Oxford University Press]
卷期号:117 (6) 被引量:1
标识
DOI:10.1093/jleuko/qiaf077
摘要

Transcription factors TFEB and TFE3 are crucial for regulating autophagy, lysosomal biogenesis, and lipid metabolism, and have significant roles in macrophage function and innate immunity. The alpha7 nicotinic acetylcholine receptor (α7nAChR), a ligand-gated Ca2+ channel known for its therapeutic potential in neurological and inflammatory disorders, has been implicated in modulating immune responses by modulating macrophage function. Stimulation of α7nAChR with chemical agonists has been claimed to activate TFEB in pancreatic acinar cells and neurons. However, the impact of α7nAChR activation on TFEB and TFE3 in macrophages remained unknown, posing an important question due to the potential implications for inflammation regulation. This study investigates the effects of acute α7nAChR activation on TFEB-mediated responses in murine macrophages using the specific agonist PNU-282987. We demonstrate that α7nAChR stimulation triggers TFEB nuclear translocation and lysosomal expansion. Surprisingly, PNU-282987 induces a broad proinflammatory gene signature without concomitant cytokine secretion, suggesting an uncoupling of gene expression from cytokine release. Mechanistically, TFEB activation requires the lysosomal Ca2+ exporter MCOLN1 and the Ca2+-dependent phosphatase PPP3/calcineurin. Additionally, PNU-282987 elevates reactive oxygen species (ROS) levels, and ROS are involved in TFEB activation by PNU-282987. Notably, even with α7nAChR deletion, compensatory ROS-mediated TFEB activation persists, suggesting the involvement of additional mechanisms of action for PNU-282987. Our findings reveal a novel α7nAChR-TFEB signaling axis in macrophages, offer new insights into the cholinergic regulation of immune responses, establish a baseline for comparison with disease states, and identify potential therapeutic targets for modulating inflammation.
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