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新型硅碳钙石生物陶瓷通过 MAPK 通路促进成骨作用引起的骨免疫反应。

Osteoimmune reaction caused by a novel silicocarnotite bioceramic promoting osteogenesis through the MAPK pathway.

机构信息

Department of Orthodontics, School and Hospital of Stomatology, Shanghai Engineering Research Center of Tooth Restoration and Regeneration, Tongji University, Shanghai 200072, China.

The Education Ministry Key Lab of Resource Chemistry and Shanghai Key Laboratory of Rare Earth Functional Materials, Shanghai Normal University, Shanghai 200234, China.

出版信息

Biomater Sci. 2022 May 31;10(11):2877-2891. doi: 10.1039/d2bm00125j.

Abstract

The host immune response to an implant is a key factor in determining the fate of bone grafts, which is thought to be a regulator of tissue regeneration. Figuring out the effects of the osteoimmune microenvironment on the osteogenesis of bone grafts can be a valuable strategy for their design and can further enhance the healing of bone defects. Our previous study demonstrated that the silicocarnotite (Ca(PO)SiO, CPS) bioceramic can significantly promote osteogenesis. The aim of this study is to investigate the immune reaction of CPS, the effects of the immune microenvironment on osteogenesis, and the related molecular mechanisms. Compared to hydroxyapatite (Ca(PO)(OH), HA), the results showed that CPS could downregulate the pro-inflammatory phenotype and upregulate the anti-inflammatory phenotype, showing the lower levels of TNF-α and increased expression of IL-10. We further found that CPS could regulate the expression of NPPA, EDN1, and MMP9 in RAW 264.7 by RNA sequencing, which may be related to its superiority in osteogenesis. The osteogenic differentiation of rat bone marrow mesenchymal stem cells (rBMSCs) was subsequently studied in a macrophage-conditioned medium pretreated with CPS, and the medium caused a significant promotion of the osteogenic differentiation of rBMSCs, demonstrating that CPS can generate a favorable immune microenvironment to promote rBMSCs differentiation. In terms of mechanism, CPS in the macrophage-conditioned medium promoted osteogenic differentiation through the MAPK pathway, including ERK1/2, JNK and P38. Our study demonstrated that osteogenic differentiation was influenced by the immune microenvironment generated the implant, and also presented an effective tool for studying the mechanisms of macrophage polarization as well as functions.

摘要

宿主对植入物的免疫反应是决定骨移植物命运的关键因素,被认为是组织再生的调节剂。了解骨免疫微环境对骨移植物成骨的影响,可以为其设计提供有价值的策略,并进一步增强骨缺损的愈合。我们之前的研究表明,硅碳磷灰石(Ca(PO)SiO,CPS)生物陶瓷可以显著促进成骨。本研究旨在研究 CPS 的免疫反应、免疫微环境对成骨的影响及其相关分子机制。与羟基磷灰石(Ca(PO)(OH),HA)相比,结果表明 CPS 可以下调促炎表型,上调抗炎表型,TNF-α 水平降低,IL-10 表达增加。我们进一步发现,CPS 通过 RNA 测序可以调节 RAW 264.7 中 NPPA、EDN1 和 MMP9 的表达,这可能与其在成骨方面的优势有关。随后在 CPS 预处理的巨噬细胞条件培养基中研究了大鼠骨髓间充质干细胞(rBMSCs)的成骨分化,结果表明该培养基显著促进了 rBMSCs 的成骨分化,表明 CPS 可以产生有利的免疫微环境促进 rBMSCs 的分化。在机制方面,巨噬细胞条件培养基中的 CPS 通过 MAPK 通路,包括 ERK1/2、JNK 和 P38,促进成骨分化。我们的研究表明,免疫微环境会影响植入物产生的成骨分化,并为研究巨噬细胞极化的机制和功能提供了一种有效的工具。

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