Targeting formyl peptide receptor 1 reduces brain inflammation and neurodegeneration

Li, Yulin; Li, Zhiguo; Zheng, Pei; Guan, Shuzhen; Li, Yan; Yao, Nan; Qi, Zhihui; Zhang, Xueyu; Su, Lei; Jing, Jing; Wu, Siting; Zhao, Xue; Wang, Meng; Böttcher, Chotima; Ljunggren, Hans-Gustaf; Paul, Friedemann; Van Kaer, Luc; Verkhratsky, Alexei; Shi, Fu-Dong

Targeting formyl peptide receptor 1 reduces brain inflammation and neurodegeneration

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Item Type:	Article
Title:	Targeting formyl peptide receptor 1 reduces brain inflammation and neurodegeneration
Creators Name:	Li, Yulin, Li, Zhiguo, Zheng, Pei, Guan, Shuzhen, Li, Yan, Yao, Nan, Qi, Zhihui, Zhang, Xueyu, Su, Lei, Jing, Jing, Wu, Siting, Zhao, Xue, Wang, Meng, Böttcher, Chotima, Ljunggren, Hans-Gustaf, Paul, Friedemann, Van Kaer, Luc, Verkhratsky, Alexei and Shi, Fu-Dong
Abstract:	Multiple sclerosis (MS) progresses through brain region–specific inflammation and degeneration, with poorly defined mechanisms. In individuals with MS, we identified increased expression of formyl peptide receptor 1 (FPR1) in central nervous system (CNS)–resident microglia and CNS-infiltrating macrophages. Blood amounts of N-formylated peptides, which are endogenous agonists of FPR1, correlated with disease progression in patients with MS. In MS mouse models, signaling through FPR1 promoted microglial mitochondrial dysfunction, causing axonal loss and apoptosis. FPR1-expressing microglia sustained the clonal expansion of myelin-reactive CD4+ T cells in the CNS. A CNS-penetrating small molecule FPR1 antagonist, T0080, mitigated autoimmune responses and axonal degeneration. Our study identifies FPR1 signaling as a potential mechanism for MS progression and suggests antagonizing FPR1 as a therapeutic approach.
Keywords:	Animal Disease Models, Apoptosis, Axons, Brain, CD4-Positive T-Lymphocytes, Disease Progression, Experimental Autoimmune Encephalomyelitis, Formyl Peptide Receptors, Inbred C57BL Mice, Macrophages, Microglia, Mitochondria, Multiple Sclerosis, Signal Transduction, Animals, Mice
Source:	Science
ISSN:	0036-8075
Publisher:	American Association for the Advancement of Science
Volume:	390
Number:	6774
Page Range:	eadq1177
Date:	13 November 2025
Additional Information:	The data under accession "CRA016153" will be available on 2025-12-24.
Official Publication:	https://doi.org/10.1126/science.adq1177
PubMed:	View item in PubMed
Related to:	URL URL Type https://ngdc.cncb.ac.cn/gsa/search?searchTerm=CRA016153 External Dataset https://github.com/codedeposition/Science2025 Software https://dx.doi.org/10.5517/ccdc.csd.cc24y49k External Dataset

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