Modulating the phenotype and function of bone marrow-derived macrophages via mandible and femur osteoblasts

再生(生物学) 免疫系统 细胞生物学 骨髓 表型 颅面 骨愈合 生物 骨免疫学 免疫学 移植 巨噬细胞 骨细胞 癌症研究 解剖 受体 医学 体外 内科学 遗传学 基因 激活剂(遗传学) 兰克尔
作者
Li Li,Yijuan Liu,Xueshen Qian,Ling Zhou,Yujie Fan,Xue Yang,Luo Kai,Yuling Chen
出处
期刊:International Immunopharmacology [Elsevier BV]
卷期号:132: 112000-112000 被引量:1
标识
DOI:10.1016/j.intimp.2024.112000
摘要

Various studies have been investigated the phenotypic and functional distinctions of craniofacial and long bone cells involved in bone regeneration. However, the process of bone tissue regeneration after bone grafting involves complicated interactions between different cell types at the donor-recipient site. Additionally, differences in alterations of the immune microenvironment at the recipient site remained to be explored. Osteoblasts (OBs) and macrophages (MØ) play essential roles in the bone restoration and regeneration processes in the bone and immune systems, respectively. The modulation of MØ on OBs has been extensively explored in the literature, whereas limited research has been conducted on the influence of OBs on the MØ phenotype and function. In the present study, OBs from the mandible and femur (MOBs and FOBs, respectively) promoted cranial defect regeneration in rats, with better outcomes noted in the MOBs-treated group. After MOBs transplantation, a significant inflammatory response was induced, accompanied by an early increase in IL-10 secretion. And then, there was an upregulation in M2-MØ-related cell markers and inflammatory factor expression. Condition media (CM) of OBs mildly inhibited apoptosis in MØ, enhanced their migration and phagocytic functions, and concurrently increased iNOS and Arg1 expression, with MOB-CM demonstrating more pronounced effects compared to FOB-CM. In conclusion, our investigation showed that MOBs and FOBs have the ability to modulate MØ phenotype and function, with MOBs exhibiting a stronger regulatory potential. These findings provide a new direction for improving therapeutic strategies for bone regeneration in autologous bone grafts from the perspective of the immune microenvironment.
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