生物
肥大细胞
炎症
受体
冲程(发动机)
神经科学
桅杆(植物学)
免疫学
遗传学
机械工程
工程类
作者
Ruchita Kothari,Mostafa Abdulrahim,Hyun Jong Oh,David M. Capuzzi,Collin Kilgore,Sumil K. Nair,Yaowu Zhang,Nathachit Limjunyawong,Sarbjit S. Saini,Jennifer E. Kim,Justin M. Caplan,Francisco Gabriel Salgado-González,Christopher M. Jackson,Chetan Bettegowda,Judy Huang,Bhanu Priya Ganesh,Chunfeng Tan,Raymond C. Koehler,Rafael J. Tamargo,Louise D. McCullough
出处
期刊:Cell
[Cell Press]
日期:2025-07-24
卷期号:188 (20): 5499-5515.e20
被引量:11
标识
DOI:10.1016/j.cell.2025.06.045
摘要
The immune environment surrounding the brain plays a fundamental role in monitoring signs of injury. Insults, including ischemic stroke, can disrupt this balance and incite an exaggerated inflammatory response, yet the underlying mechanism remains unclear. Here, we show that the mast-cell-specific receptor Mrgprb2 regulates post-stroke brain inflammation from the meninges. Mrgprb2 causes meningeal mast cell degranulation after stroke, releasing immune mediators. This process recruits skull bone marrow neutrophils into the dura and further promotes neutrophil migration from the dura into the brain by cleaving the chemorepellent semaphorin 3a. We demonstrate that the human ortholog, MRGPRX2, is expressed in human meningeal mast cells and is activated by upregulation of the neuropeptide substance P following stroke. Pharmacologically inhibiting Mrgprb2 reduces post-stroke inflammation and improves neurological outcomes in mice, providing a druggable target. Collectively, our study identifies Mrgprb2 as a critical meningeal gatekeeper for immune migration from skull bone marrow reservoirs into the brain.
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