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硼硅酸盐生物活性玻璃 0106-B1 具有良好的血管生成特性,与 45S5 生物玻璃相比,能增强体内类骨质的形成。

Favorable angiogenic properties of the borosilicate bioactive glass 0106-B1 result in enhanced in vivo osteoid formation compared to 45S5 Bioglass.

机构信息

Center of Orthopedics, Traumatology, and Spinal Cord Injury, Heidelberg University Hospital, Schlierbacher Landstraße 200a, 69118 Heidelberg, Germany.

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

出版信息

Biomater Sci. 2019 Dec 1;7(12):5161-5176. doi: 10.1039/c9bm01220f. Epub 2019 Oct 4.

Abstract

The 45S5-bioactive glass (BG) composition is the most commonly investigated amongst BG-based bone substitutes. By changing BG compositions and by addition of therapeutically active ions such as boron, the biological features of BGs can be tailored towards specific needs and possible drawbacks can be overcome. The borosilicate glass 0106-B1 (composition in wt%: 37.5 SiO, 22.6 CaO, 5.9 NaO, 4.0 PO, 12.0 KO, 5.5 MgO, 12.5 BO) has demonstrated pro-angiogenic properties. However, the osteogenic performance of the 0106-B1-BG and its influence on cell viability and proliferation in vitro as well as its osteogenic and angiogenic properties in vivo have not been investigated. Therefore, in this study, the impact of 0106-B1-BG and 45S5-BG on osteogenic differentiation, viability and proliferation on human mesenchymal stromal cells (MSCs) was assessed in vitro. Furthermore, MSC-seeded scaffolds made from both BG types were implanted subcutaneously in immunodeficient mice for 10 weeks. Osteoid formation was quantified by histomorphometry, vascularization was visualized by immunohistological staining. Additionally, the in vivo expression patterns of genes correlating with osteogenesis and angiogenesis were analyzed. In vitro, the impact of 45S5-BG and 0106-B1-BG on the proliferation, viability and osteogenic differentiation of MSCs was comparable. In vivo, scaffolds made from 0106-B1-BG significantly outperformed the 45S5-BG-based scaffolds regarding the amount and maturation of the osteoid. Furthermore, 0106-B1-BG-based scaffolds showed significantly increased angiogenic gene expression patterns. In conclusion, the beneficial angiogenic properties of 0106-B1-BG result in improved osteogenic properties in vivo, making the 0106-B1-BG a promising candidate for further investigation, e.g. in a bone defect model.

摘要

45S5-生物活性玻璃(BG)是最常被研究的 BG 基骨替代物。通过改变 BG 成分并添加治疗活性离子,如硼,可以针对特定需求定制 BG 的生物学特性,并克服可能的缺点。硼硅酸盐玻璃 0106-B1(按重量计的组成:37.5SiO,22.6CaO,5.9NaO,4.0PO,12.0KO,5.5MgO,12.5BO)已被证明具有促血管生成特性。然而,0106-B1-BG 的成骨性能及其对细胞活力和增殖的影响,以及其在体内的成骨和血管生成性能尚未得到研究。因此,在这项研究中,评估了 0106-B1-BG 和 45S5-BG 对人间充质基质细胞(MSCs)成骨分化、活力和增殖的影响。此外,将两种 BG 类型的 MSC 种子支架植入免疫缺陷小鼠皮下 10 周。通过组织形态计量学定量评估类骨质形成,通过免疫组织化学染色可视化血管化。此外,还分析了与成骨和血管生成相关的基因的体内表达模式。在体外,45S5-BG 和 0106-B1-BG 对 MSCs 的增殖、活力和成骨分化的影响相当。在体内,0106-B1-BG 支架在类骨质的数量和成熟度方面明显优于 45S5-BG 支架。此外,0106-B1-BG 支架表现出明显增加的血管生成基因表达模式。总之,0106-B1-BG 的有益的血管生成特性导致体内成骨性能的改善,使 0106-B1-BG 成为进一步研究的有前途的候选物,例如在骨缺损模型中。

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