细胞生物学
再生(生物学)
骨膜
巨噬细胞
干细胞
藤黄蛋白C
骨免疫学
细胞外基质
免疫学
骨愈合
生物
解剖
受体
体外
生物化学
激活剂(遗传学)
兰克尔
作者
Qian Ren,Wenhui Xing,Bo Jiang,Heng Feng,Xuye Hu,Jinlong Suo,Lijun Wang,Weiguo Zou
标识
DOI:10.1038/s41418-024-01429-9
摘要
Abstract During the early stage of tissue injury, macrophages play important roles in the activation of stem cells for further regeneration. However, the regulation of macrophages during bone regeneration remains unclear. Here, the extracellular matrix (ECM) tenascin-C (TNC) is found to express in the periosteum and recruit inflammatory macrophages. TNC-deficiency in the periosteum delays bone repair. Transplantation of macrophages derived from injured periosteum is able to rescue the decreased skeletal stem cells and impaired bone regeneration caused by TNC deficiency. The cell communication analysis identifies ITGA7 as a TNC receptor contributing to the recruitment of inflammatory macrophages. TNC expression declines in aged mice and the exogenous delivery of TNC significantly promotes bone regeneration after aging through the recruitment of macrophages. Taken together, this study reveals the regulation of macrophage recruitment and its function in the activation of skeletal stem cells after bone injury, providing a strategy to accelerate bone regeneration by TNC delivery.
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