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海藻酸钠微球共包载抗 BMP2 单克隆抗体和间充质干细胞用于骨组织工程。

Co-encapsulation of anti-BMP2 monoclonal antibody and mesenchymal stem cells in alginate microspheres for bone tissue engineering.

机构信息

Center for Craniofacial Molecular Biology, Ostrow School of Dentistry of USC, University of Southern California, Los Angeles, CA 90089, USA.

出版信息

Biomaterials. 2013 Sep;34(28):6572-9. doi: 10.1016/j.biomaterials.2013.05.048. Epub 2013 Jun 14.

Abstract

Recently, it has been shown that tethered anti-BMP2 monoclonal antibodies (mAbs) can trap BMP ligands and thus provide BMP inductive signals for osteo-differentiation of progenitor cells. The objectives of this study were to: (1) develop a co-delivery system based on murine anti-BMP2 mAb-loaded alginate microspheres encapsulating human bone marrow mesenchymal stem cells (hBMMSCs); and (2) investigate osteogenic differentiation of encapsulated stem cells in alginate microspheres in vitro and in vivo. Alginate microspheres of 1 ± 0.1 mm diameter were fabricated with 2 × 10(6) hBMMSCs per mL of alginate. Critical-size calvarial defects (5 mm diameter) were created in immune-compromised mice and alginate microspheres preloaded with anti-BMP mAb encapsulating hBMMSCs were transplanted into defect sites. Alginate microspheres pre-loaded with isotype-matched non-specific antibody were used as the negative control. After 8 weeks, micro CT and histologic analyses were used to analyze bone formation. In vitro analysis demonstrated that anti-BMP2 mAbs tethered BMP2 ligands that can activate the BMP receptors on hBMMSCs. The co-delivery system described herein, significantly enhanced hBMMSC-mediated osteogenesis, as confirmed by the presence of BMP signal pathway-activated osteoblast determinants Runx2 and ALP. Our results highlight the importance of engineering the microenvironment for stem cells, and particularly the value of presenting inductive signals for osteo-differentiation of hBMMSCs by tethering BMP ligands using mAbs. This strategy of engineering the microenvironment with captured BMP signals is a promising modality for repair and regeneration of craniofacial, axial and appendicular bone defects.

摘要

最近的研究表明,连接的抗 BMP2 单克隆抗体(mAbs)可以捕获 BMP 配体,从而为前体细胞的成骨分化提供 BMP 诱导信号。本研究的目的是:(1)开发一种基于载有人骨髓间充质干细胞(hBMMSCs)的鼠抗 BMP2 mAb 负载的海藻酸钠微球的共递送系统;(2)研究封装在海藻酸钠微球中的干细胞在体外和体内的成骨分化。采用 2×10(6)个 hBMMSCs/mL 的海藻酸钠制备粒径为 1±0.1mm 的海藻酸钠微球。在免疫缺陷小鼠中制作临界尺寸颅骨缺损(5mm 直径),并将预先加载抗 BMP mAb 封装 hBMMSCs 的海藻酸钠微球移植到缺损部位。将预载有同型匹配非特异性抗体的海藻酸钠微球作为阴性对照。8 周后,采用 micro CT 和组织学分析来分析骨形成。体外分析表明,连接的抗 BMP2 mAbs 可以捕获 BMP2 配体,从而激活 hBMMSCs 上的 BMP 受体。本文所述的共递送系统显著增强了 hBMMSC 介导的成骨作用,这可以通过存在 BMP 信号通路激活的成骨决定因子 Runx2 和 ALP 得到证实。我们的结果强调了为干细胞工程微环境的重要性,特别是通过使用 mAbs 连接 BMP 配体来呈现诱导 hBMMSCs 成骨分化的信号的重要性。这种捕获 BMP 信号的工程微环境策略是修复和再生颅面、轴骨和附肢骨缺损的一种很有前途的方法。

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