血管生成
再生(生物学)
细胞生物学
巨噬细胞
骨髓
祖细胞
化学
癌症研究
免疫学
生物
干细胞
生物化学
体外
作者
Yukihiro Kohara,Riko Kitazawa,Ryuma Haraguchi,Yuuki Imai,Sohei Kitazawa
出处
期刊:Bone
[Elsevier]
日期:2021-09-14
卷期号:154: 116200-116200
被引量:13
标识
DOI:10.1016/j.bone.2021.116200
摘要
Macrophages are progenitors of osteoclasts as well as regulators of bone metabolism. Macrophages mediate not only bone formation by osteoblasts under physiological conditions, but also bone regeneration after fracture. The mechanisms of macrophages regulation of bone formation and regeneration remain unclear, however. Here, we demonstrate that the liposome-encapsulated Clodronate (Clod-lip) injected mouse model with cortical bone defect induced by drill-hole injury and targeted depletion of phagocytic macrophages exhibits impaired angiogenesis of type H vessels that couple angiogenesis and osteogenesis. Moreover, we identify Tgfbi (encoding TGFBI), Plau (encoding uPA) and Tgfb1 (encoding TGF-β1), through RNA-seq analysis, as genes of macrophage-secreted factors mediating angiogenesis and wound healing. The relevant mRNA was highly expressed in bone marrow-derived macrophages among bone cells, as determined through qRT-PCR. Finally, we disclose that treatment with uPA inhibitor or TGF-β receptor I, receptor II inhibitor impairs bone regeneration after injury, confirming the importance of uPA and TGF-β1 during bone regeneration. Our findings reveal a novel mechanism of bone regeneration mediated by macrophages.
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