Xing Junchao, Mei Tieniu, Luo Keyu, Li Zhiqiang, Yang Aijun, Li Zhilin, Xie Zhao, Zhang Zehua, Dong Shiwu, Hou Tianyong, Xu Jianzhong, Luo Fei
Department of Orthopedics, National & Regional United Engineering Laboratory of Tissue Engineering, Southwest Hospital, the Third Military Medical University, Chongqing, China; Center of Regenerative and Reconstructive Engineering Technology in Chongqing City, Chongqing, China; Tissue Engineering Laboratory of Chongqing City, Chongqing, China.
Department of Orthopedics, National & Regional United Engineering Laboratory of Tissue Engineering, Southwest Hospital, the Third Military Medical University, Chongqing, China; Center of Regenerative and Reconstructive Engineering Technology in Chongqing City, Chongqing, China; Tissue Engineering Laboratory of Chongqing City, Chongqing, China; Department of Spine, Lanzhou General Hospital, Lanzhou Command of CPLA, Lanzhou 730050, China.
Acta Biomater. 2017 Apr 15;53:470-482. doi: 10.1016/j.actbio.2017.02.016. Epub 2017 Feb 11.
Easily accessible and effective bone grafts are in urgent need in clinic. The selective cell retention (SCR) strategy, by which osteogenesis-related cells and factors are enriched from bone marrow into bio-scaffolds, holds great promise. However, the retention efficacy is limited by the relatively low densities of osteogenesis-related cells and factors in marrow; in addition, a lack of satisfactory surface modifiers for scaffolds further exacerbates the dilemma. To address this issue, a multi-layered construct consisting of a recombinant fibronectin/cadherin chimera was established via a layer-by-layer self-assembly technique (LBL-rFN/CDH) and used to modify demineralised bone matrix (DBM) scaffolds. The modification was proven stable and effective. By the mechanisms of physical interception and more importantly, chemical recognition (fibronectin/integrins), the LBL-rFN/CDH modification significantly improved the retention efficacy and selectivity for osteogenesis-related cells, e.g., monocytes, mesenchymal stem cells (MSCs) and hematopoietic stem cells (HSCs), and bioactive factors, e.g., bFGF, BMP-2 and SDF-1α. Moreover, the resulting composite (designated as DBM-LBL-rFN/CDH) not only exhibited a strong MSC-recruiting capacity after SCR, but also provided favourable microenvironments for the proliferation and osteogenic differentiation of MSCs. Eventually, bone repair was evidently improved. Collectively, DBM-LBL-rFN/CDH presented a suitable biomaterial for SCR and a promising solution for tremendous need for bone grafts.
There is an urgent need for effective bone grafts. With the potential of integrating osteogenicity, osteoinductivity and osteoconductivity, selective cell retention (SCR) technology brings hope for developing ideal grafts. However, it is constrained by low efficacy and selectivity. Thus, we modified demineralized bone matrix with nano-scaled and multi-layered recombinant fibronectin/cadherin chimera (DBM-rFN/CDH-LBL), and evaluate its effects on SCR and bone repair. DBM-rFN/CDH-LBL significantly improved the efficacy and selectivity of SCR via physical interception and chemical recognition. The post-enriched DBM-rFN/CDH-LBL provided favourable microenvironments to facilitate the migration, proliferation and osteogenic differentiation of MSCs, thus accelerating bone repair. Conclusively, DBM-rFN/CDH-LBL presents a novel biomaterial with advantages including high cost-effectiveness, more convenience for storage and transport and can be rapidly constructed intraoperatively.
临床上迫切需要易于获取且有效的骨移植材料。选择性细胞滞留(SCR)策略,即从骨髓中富集与骨生成相关的细胞和因子到生物支架中,具有很大的潜力。然而,滞留效果受到骨髓中与骨生成相关的细胞和因子相对低密度的限制;此外,缺乏令人满意的支架表面改性剂进一步加剧了这一困境。为了解决这个问题,通过层层自组装技术(LBL-rFN/CDH)构建了一种由重组纤连蛋白/钙黏蛋白嵌合体组成的多层结构,并用于修饰脱矿骨基质(DBM)支架。这种修饰被证明是稳定且有效的。通过物理截留机制,更重要的是化学识别(纤连蛋白/整合素),LBL-rFN/CDH修饰显著提高了对与骨生成相关的细胞(如单核细胞、间充质干细胞(MSCs)和造血干细胞(HSCs))以及生物活性因子(如bFGF、BMP-2和SDF-1α)的滞留效果和选择性。此外,所得复合材料(命名为DBM-LBL-rFN/CDH)不仅在SCR后表现出强大的招募MSC的能力,还为MSC的增殖和成骨分化提供了有利的微环境。最终,骨修复得到明显改善。总的来说,DBM-LBL-rFN/CDH是一种适合SCR的生物材料,为骨移植的迫切需求提供了一个有前景的解决方案。
迫切需要有效的骨移植材料。选择性细胞滞留(SCR)技术具有整合成骨性、骨诱导性和骨传导性的潜力,为开发理想的移植材料带来了希望。然而,它受到低效率和低选择性的限制。因此,我们用纳米级多层重组纤连蛋白/钙黏蛋白嵌合体修饰脱矿骨基质(DBM-rFN/CDH-LBL),并评估其对SCR和骨修复的影响。DBM-rFN/CDH-LBL通过物理截留和化学识别显著提高了SCR的效率和选择性。富集后的DBM-rFN/CDH-LBL提供了有利的微环境,促进了MSC的迁移、增殖和成骨分化,从而加速了骨修复。总之,DBM-rFN/CDH-LBL是一种新型生物材料,具有成本效益高、储存和运输更方便以及可在术中快速构建等优点。
