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聚丙交酯-乙交酯-壳聚糖核壳纤维电纺支架中白细胞介素 4 和 TCP 的双重释放通过协同免疫调节和成骨作用增强骨再生。

Dual-Mode Release of IL-4 and TCP from a PGA-SF Core-Shell Electrospinning Scaffold for Enhanced Bone Regeneration through Synergistic Immunoregulation and Osteogenesis.

机构信息

Hospital of Stomatology, Guanghua School of Stomatology, Institute of Stomatology, Sun Yat-sen University, Guangdong Provincial Key Laboratory of Stomatology, Guangzhou 510275, China.

出版信息

ACS Appl Mater Interfaces. 2024 Oct 30;16(43):58148-58167. doi: 10.1021/acsami.4c08996. Epub 2024 Sep 16.

Abstract

The successful filling of bone defects remains challenging due to the incongruity between bone graft materials and the dynamic process of bone healing. Developing multifunctional materials matching the dynamic process of bone healing offers a viable solution to the current dilemma. Lines of evidence have shown that engineering osteoimmunomodulatory biomaterials can modulate the function of immune cells and thus promote bone regeneration. Herein, we utilized silk fibroin (SF) and polyglycolic acid (PGA) to create a PGA-SF core-shell fibrous scaffold, incorporating interleukin-4 (IL-4) and tricalcium phosphate (TCP) as a codelivery system (PGA/TCP-SF/IL-4), aiming to achieve an initial rapid release of IL-4 and sustained release of TCP. The PGA/TCP-SF/IL-4 scaffold mimicked the native bone structure and showed superior tenacity in the wetting regime. studies demonstrated that the PGA/TCP-SF/IL-4 scaffold significantly reduced the inflammatory response by upregulating the M2 macrophages, created a favorable microenvironment for osteogenesis, and facilitated osteogenic differentiation and mineralization. Implantation of the PGA/TCP-SF/IL-4 scaffold into the rat skull defect model notably increased the formation of new bones. IL-4 and TCP acted synergistically in attenuating inflammation and enhancing osteogenic differentiation. Overall, this multifunctional scaffold comprehensively considers the various demands in the bone defect region, which might have a significant potential for application in bone reconstruction.

摘要

由于骨移植物材料与骨愈合的动态过程之间存在不匹配,成功填充骨缺损仍然具有挑战性。开发与骨愈合的动态过程相匹配的多功能材料为解决当前的困境提供了可行的解决方案。有证据表明,工程化的骨免疫调节生物材料可以调节免疫细胞的功能,从而促进骨再生。在此,我们利用丝素蛋白(SF)和聚乙醇酸(PGA)构建了一种 PGA-SF 核壳纤维支架,将白细胞介素-4(IL-4)和磷酸三钙(TCP)作为共递送系统(PGA/TCP-SF/IL-4),旨在实现 IL-4 的快速初始释放和 TCP 的持续释放。PGA/TCP-SF/IL-4 支架模拟了天然骨结构,在润湿状态下具有优异的韧性。研究表明,PGA/TCP-SF/IL-4 支架通过上调 M2 巨噬细胞显著降低了炎症反应,为成骨创造了有利的微环境,并促进了成骨分化和矿化。将 PGA/TCP-SF/IL-4 支架植入大鼠颅骨缺损模型中显著增加了新骨的形成。IL-4 和 TCP 协同作用,减轻炎症反应,增强成骨分化。总的来说,这种多功能支架全面考虑了骨缺损区域的各种需求,在骨重建中可能具有重要的应用潜力。

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