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采用人骨髓基质细胞和啮齿动物临界尺寸股骨缺损模型对 45S5、1393 和 0106-B1 生物活性玻璃成分的生物学特性进行体外和体内比较分析。

A comparative in vitro and in vivo analysis of the biological properties of the 45S5-, 1393-, and 0106-B1-bioactive glass compositions using human bone marrow-derived stromal cells and a rodent critical size femoral defect model.

机构信息

Department of Orthopaedics, Heidelberg University Hospital, Schlierbacher Landstraße 200a, 69118 Heidelberg, Germany.

Institute of Biomaterials, University of Erlangen-Nuremberg, Cauerstraße 6, 91058 Erlangen, Germany.

出版信息

Biomater Adv. 2023 Oct;153:213521. doi: 10.1016/j.bioadv.2023.213521. Epub 2023 Jun 13.

DOI:10.1016/j.bioadv.2023.213521
PMID:37356285
Abstract

Since the introduction of the 45S5-bioactive glass (BG), numerous new BG compositions have been developed. Compared to the 45S5-BG, 1393-BG shows favorable processing properties due to its low crystallization tendency and the 1393-BG-based borosilicate 0106-B1-BG exhibits improved angiogenic properties due to its boron content. Despite their close (chemical) relationship, the biological properties of the mentioned BG composition have not yet been comparatively examined. In this study, the effects of the BGs on proliferation, viability, osteogenic differentiation, and angiogenic factor production of human bone marrow-derived mesenchymal stromal cells were assessed. Scaffolds made of the BGs were introduced in a critical-sized femur defect model in rats in order to analyze their impact on bone defect regeneration. In vitro, 1393-BG and 0106-B1-BG outperformed 45S5-BG with regard to cell proliferation and viability. 1393-BG enhanced osteogenic differentiation; 0106-B1-BG promoted angiogenic factor production. In vivo, 0106-B1-BG and 45S5-BG outperformed 1393-BG in terms of angiogenic and osteoclastic response resulting in improved bone regeneration. In conclusion, the biological properties of BGs can be significantly modified by tuning their composition. Demonstrating favorable processing properties and an equally strong in vivo bone regeneration potential as 45S5-BG, 0106-B1-BG qualifies as a basis to incorporate other bioactive ions to improve its biological properties.

摘要

自 45S5-生物活性玻璃(BG)问世以来,已经开发出了许多新型的 BG 成分。与 45S5-BG 相比,1393-BG 的结晶倾向较低,具有更好的加工性能,而基于 1393-BG 的硼硅酸盐 0106-B1-BG 由于其硼含量而表现出更好的血管生成特性。尽管它们的(化学)关系密切,但尚未对这些 BG 成分的生物学特性进行比较研究。在这项研究中,评估了 BG 对人骨髓间充质基质细胞增殖、活力、成骨分化和血管生成因子产生的影响。将 BG 制成支架,引入大鼠股骨临界尺寸缺损模型中,以分析它们对骨缺损再生的影响。在体外,1393-BG 和 0106-B1-BG 在细胞增殖和活力方面优于 45S5-BG。1393-BG 增强了成骨分化;0106-B1-BG 促进了血管生成因子的产生。在体内,0106-B1-BG 和 45S5-BG 在血管生成和破骨细胞反应方面优于 1393-BG,从而促进了骨再生。总之,通过调整 BG 的成分,可以显著改变其生物学特性。0106-B1-BG 表现出良好的加工性能和与 45S5-BG 相当的体内骨再生潜力,可作为掺入其他生物活性离子以改善其生物学特性的基础。

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