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由分层 MBG 支架时空递呈的 IL-8 和 BMP-2 驱动的快速引导骨再生。

Rapid initiation of guided bone regeneration driven by spatiotemporal delivery of IL-8 and BMP-2 from hierarchical MBG-based scaffold.

机构信息

Engineering Research Center for Biomaterials of Ministry of Education, East China University of Science and Technology, Shanghai, 200237, PR China; Key Laboratory for Ultrafine Materials of Ministry of Education, East China University of Science and Technology, Shanghai, 200237, PR China.

Engineering Research Center for Biomaterials of Ministry of Education, East China University of Science and Technology, Shanghai, 200237, PR China; The State Key Laboratory of Bioreactor Engineering, East China University of Science and Technology, Shanghai, 200237, PR China.

出版信息

Biomaterials. 2019 Mar;196:122-137. doi: 10.1016/j.biomaterials.2017.11.011. Epub 2017 Nov 17.

Abstract

Initiation of endogenous repair mechanisms, including key steps of stem cell recruitment and cartilage intermediate formation in endochondral ossification, is vital to regeneration of large bone defects. To biomimetically promote a rapid initiation and ensuing osteogenic stimulation, exogenous chemokine IL-8 and growth factor BMP-2 were orchestrated in a mesoporous bioactive glass (MBG)-based spatiotemporal delivery system, to achieve a rapid release of IL-8 followed by a long-term sustained release of BMP-2. The synergistic effect of IL-8 and BMP-2 on initiation stage of bone healing and underlying mechanism were thoroughly investigated in vitro and in vivo. Intriguingly, apart from its superiority in stem cell recruitment to BMP-2, IL-8 not only endowed a histological "prep-state" of endochondral ossification by up-regulating chondrogenic genes and inducing the formation of extensive cartilage tissues, facilitating rapid bone transformation by BMP-2, but also triggered a cellular "prep-state" with high expression of BMP receptors, enhancing the osteoinductivity of BMP-2. With the spatiotemporal delivery system, orchestrated signal stimuli of IL-8 and BMP-2 induced a rapid initiation including efficient stem cell recruitment and a "chondrogenic/osteogenic balance" at the first stage of endochondral ossification, and the scaffold facilitated sufficient osteoconductivity, together resulting in early extensive bone mineralization and an advanced regeneration throughout the repair of large bone defect. We believe this new idea could provide insights toward designing bone-repairing biomaterials with higher regenerative efficiency.

摘要

启动内源性修复机制,包括在软骨内骨化中干细胞募集和软骨中间形成的关键步骤,对于大骨缺损的再生至关重要。为了仿生学地促进快速启动和随后的成骨刺激,外源性趋化因子 IL-8 和生长因子 BMP-2 在介孔生物活性玻璃(MBG)基时空递送系统中进行了协调,以实现 IL-8 的快速释放,随后是 BMP-2 的长期持续释放。IL-8 和 BMP-2 对骨愈合起始阶段的协同作用及其潜在机制在体外和体内进行了深入研究。有趣的是,除了在干细胞募集方面优于 BMP-2 外,IL-8 不仅通过上调软骨形成基因和诱导广泛的软骨组织形成来赋予软骨内骨化的组织学“预备状态”,从而促进 BMP-2 快速骨转化,而且还引发了一种具有高 BMP 受体表达的细胞“预备状态”,增强了 BMP-2 的成骨诱导性。通过时空递送系统,协调的 IL-8 和 BMP-2 信号刺激在软骨内骨化的第一阶段诱导了快速启动,包括有效的干细胞募集和“软骨形成/成骨平衡”,支架促进了足够的骨传导性,共同导致早期广泛的骨矿化和整个大骨缺损修复过程中的先进再生。我们相信,这个新理念可以为设计具有更高再生效率的骨修复生物材料提供思路。

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