The dura sinus-resident immune cells can influence the process of central neural system (CNS) diseases by communicating with central nerve cells. In clinical, Tregs are also frequently impaired in depression. However, the significance of this relationship remains unknown. In the present study, we found a significant increase in dural Treg populations in mouse models of depression, whereas depleting them by neutralizing antibodies injection could exacerbate depressive phenotypes. Through RNA sequencing, we identified that the antidepressant effects of dural Tregs are at least in part through the production of amphiregulin, increasing the expression of its receptor EGFR in medial prefrontal cortex (mPFC) pyramidal neurons. Furthermore, dural Tregs expressed high levels of ST2, and their expansion in depressed mice depended on astrocyte-derived IL33 secretion. Our study shows that dural Treg signaling can be enhanced by treatment with fluoxetine, highlighting that dural Tregs can be utilized as a potential target cell in major depressive disorder (MDD).
Dural Tregs driven by astrocytic IL-33 mitigate depression through the EGFR signals in mPFC neurons.
受星形胶质细胞 IL-33 驱动的硬脑膜调节性 T 细胞通过 mPFC 神经元中的 EGFR 信号减轻抑郁症
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作者:Yao Hang, Liu Yang, Wang Yueping, Xue You, Jiang Siyuan, Sun Xin, Ji Minjun, Xu Zhipeng, Ding Jianhua, Hu Gang, Lu Ming
| 期刊: | Cell Death and Differentiation | 影响因子: | 15.400 |
| 时间: | 2025 | 起止号: | 2025 May;32(5):926-943 |
| doi: | 10.1038/s41418-024-01421-3 | 靶点: | EGFR |
| 研究方向: | 信号转导、神经科学、细胞生物学 | 疾病类型: | 抑郁症 |
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