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用于骨再生的生物活性和可生物降解的二氧化硅生物材料。

Bioactive and biodegradable silica biomaterial for bone regeneration.

作者信息

Wang Shunfeng, Wang Xiaohong, Draenert Florian G, Albert Olga, Schröder Heinz C, Mailänder Volker, Mitov Gergo, Müller Werner E G

机构信息

ERC Advanced Investigator Grant Research Group at the Institute for Physiological Chemistry, University Medical Center of the Johannes Gutenberg University, Duesbergweg 6, D-55128 Mainz, Germany.

ERC Advanced Investigator Grant Research Group at the Institute for Physiological Chemistry, University Medical Center of the Johannes Gutenberg University, Duesbergweg 6, D-55128 Mainz, Germany; National Research Center for Geoanalysis, Chinese Academy of Geological Sciences, 26 Baiwanzhuang Dajie, CN-Beijing 100037, China.

出版信息

Bone. 2014 Oct;67:292-304. doi: 10.1016/j.bone.2014.07.025. Epub 2014 Aug 1.

Abstract

Biosilica, a biocompatible, natural inorganic polymer that is formed by an enzymatic, silicatein-mediated reaction in siliceous sponges to build up their inorganic skeleton, has been shown to be morphogenetically active and to induce mineralization of human osteoblast-like cells (SaOS-2) in vitro. In the present study, we prepared beads (microspheres) by encapsulation of β-tricalcium phosphate [β-TCP], either alone (control) or supplemented with silica or silicatein, into the biodegradable copolymer poly(d,l-lactide-co-glycolide) [PLGA]. Under the conditions used, ≈5% β-TCP, ≈9% silica, and 0.32μg/mg of silicatein were entrapped into the PLGA microspheres (diameter≈800μm). Determination of the biocompatibility of the β-TCP microspheres, supplemented with silica or silicatein, revealed no toxicity in the MTT based cell viability assay using SaOS-2 cells. The adherence of SaOS-2 cells to the surface of silica-containing microspheres was higher than for microspheres, containing only β-TCP. In addition, the silica-containing β-TCP microspheres and even more pronounced, a 1:1 mixture of microspheres containing β-TCP and silica, and β-TCP and silicatein, were found to strongly enhance the mineral deposition by SaOS-2 cells. Using these microspheres, first animal experiments with silica/biosilica were performed in female, adult New Zealand White rabbits to study the effect of the inorganic polymer on bone regeneration in vivo. The microspheres were implanted into 5mm thick holes, drilled into the femur of the animals, applying a bilateral comparison study design (3 test groups with 4-8 animals each). The control implant on one of the two hind legs contained microspheres with only β-TCP, while the test implant on the corresponding leg consisted either of microspheres containing β-TCP and silica, or a 1:1 mixture of microspheres, supplemented with β-TCP and silica, and β-TCP and silicatein. The results revealed that tissue/bone sections of silica containing implants and implants, composed of a 1:1 mixture of silica-containing microspheres and silicatein-containing microspheres, show an enhanced regeneration of bone tissue around the microspheres, compared to the control implants containing only β-TCP. The formation of new bone induced by the microspheres is also evident from measurements of the stiffness/reduced Young's modulus of the regenerated bone tissue. The reduced Young's modulus of the regenerating bone tissue around the implants was markedly higher for the silica-containing microspheres (1.1MPa), and even more for the 1:1 mixture of the silica- and silicatein-containing microspheres (1.4MPa), compared to the β-TCP microsphere controls (0.4MPa). We propose that based on their morphogenetic activity on bone-forming cells in vitro and the results of the animal experiments presented here, silica/biosilica-based scaffolds are promising materials for bone repair/regeneration.

摘要

生物二氧化硅是一种生物相容性天然无机聚合物,由硅质海绵中的酶促、硅酸蛋白介导反应形成,用于构建其无机骨架。研究表明,生物二氧化硅具有形态发生活性,并能在体外诱导人成骨样细胞(SaOS-2)矿化。在本研究中,我们通过将β-磷酸三钙[β-TCP]单独(对照)或添加二氧化硅或硅酸蛋白包裹于可生物降解共聚物聚(d,l-丙交酯-共-乙交酯)[PLGA]中来制备珠子(微球)。在所使用的条件下,约5%的β-TCP、约9%的二氧化硅和0.32μg/mg的硅酸蛋白被包封于PLGA微球(直径约800μm)中。对添加了二氧化硅或硅酸蛋白的β-TCP微球的生物相容性进行测定,发现在使用SaOS-2细胞的基于MTT的细胞活力测定中无毒性。SaOS-2细胞对含二氧化硅微球表面的黏附性高于仅含β-TCP的微球。此外,发现含二氧化硅的β-TCP微球,更明显的是含β-TCP和二氧化硅的微球以及含β-TCP和硅酸蛋白的微球按1:1混合后,能强烈增强SaOS-2细胞的矿物质沉积。使用这些微球,首次在成年雌性新西兰白兔身上进行了关于二氧化硅/生物二氧化硅的动物实验,以研究这种无机聚合物对体内骨再生的影响。将微球植入动物股骨上钻出的5mm厚的孔中,采用双侧对照研究设计(3个试验组,每组4 - 8只动物)。两条后腿之一的对照植入物包含仅含β-TCP的微球,而相应腿上的试验植入物由含β-TCP和二氧化硅的微球组成,或由含β-TCP和二氧化硅以及含β-TCP和硅酸蛋白的微球按1:1混合而成。结果显示,与仅含β-TCP的对照植入物相比,含二氧化硅植入物以及由含二氧化硅微球和含硅酸蛋白微球按1:1混合而成的植入物的组织/骨切片显示微球周围骨组织再生增强。再生骨组织的刚度/降低的杨氏模量测量结果也表明微球诱导了新骨形成。与β-TCP微球对照组(0.4MPa)相比,含二氧化硅微球周围再生骨组织的降低的杨氏模量明显更高(1.1MPa),含二氧化硅和硅酸蛋白微球按1:1混合的情况更高(1.4MPa)。我们认为,基于其对体外成骨细胞的形态发生活性以及此处呈现的动物实验结果,基于二氧化硅/生物二氧化硅的支架是用于骨修复/再生的有前景的材料。

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