Musculoskeletal traumatic injuries (MTI) involve soft tissue lesions adjacent to a bone fracture leading to fibrous nonunion. The impact of MTI on the inflammatory response to fracture and on the immunomodulation of skeletal stem/progenitor cells (SSPCs) remains unknown. Here, we used single-nucleus transcriptomic analyses to describe the immune cell dynamics after bone fracture and identified distinct macrophage subsets with successive pro-inflammatory, pro-repair and anti-inflammatory profiles. Concurrently, SSPCs transition via a pro- and anti-inflammatory fibrogenic phase of differentiation prior to osteochondrogenic differentiation. In a preclinical MTI mouse model, the injury response of immune cells and SSPCs is disrupted leading to a prolonged pro-inflammatory phase and delayed resolution of inflammation. Macrophage depletion improves bone regeneration in MTI demonstrating macrophage involvement in fibrous nonunion. Finally, pharmacological inhibition of macrophages using the CSF1R inhibitor Pexidartinib ameliorates healing. These findings reveal the coordinated immune response of macrophages and skeletal stem/progenitor cells as a driver of bone healing and as a primary target for the treatment of trauma-associated fibrosis.
Multimodal analyses of immune cells during bone repair identify macrophages as a therapeutic target in musculoskeletal trauma.
对骨修复过程中免疫细胞的多模态分析表明,巨噬细胞是肌肉骨骼创伤的治疗靶点
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作者:Hachemi Yasmine, Perrin Simon, Ethel Maria, Julien Anais, Vettese Julia, Geisler Blandine, Göritz Christian, Colnot Céline
| 期刊: | Bone Research | 影响因子: | 15.000 |
| 时间: | 2024 | 起止号: | 2024 Sep 29; 12(1):56 |
| doi: | 10.1038/s41413-024-00347-3 | 研究方向: | 细胞生物学 |
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