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新型无水载体中微结构磷酸钙的体内性能。

In vivo performance of microstructured calcium phosphate formulated in novel water-free carriers.

机构信息

Xpand Biotechnology BV, MB Bilthoven, The Netherlands.

出版信息

Acta Biomater. 2012 Jul;8(7):2759-69. doi: 10.1016/j.actbio.2012.04.007. Epub 2012 Apr 7.

DOI:10.1016/j.actbio.2012.04.007
PMID:22487931
Abstract

Osteoinductive calcium phosphate (CaP) ceramics can be combined with polymeric carriers to make shapeable bone substitutes as an alternative to autologous bone; however, carriers containing water may degrade the ceramic surface microstructure, which is crucial to bone formation. In this study five novel tricalcium phosphate (TCP) formulations were designed from water-free polymeric binders and osteoinductive TCP granules of different particle sizes (500-1000 μm for moldable putty forms, and 150-500 μm for flowable paste forms). The performance of these novel TCP formulations was studied and compared with control TCP granules alone (both 150-500 and 500-1000 μm). In vitro the five TCP formulations were characterized by their carrier dissolution times and TCP mineralization kinetic profiles in simulated body fluid. In vivo the formulations were implanted in the dorsal muscle and a unicortical femoral defect (Ø=5 mm) of dogs for 12 weeks. The TCP formulation based on a xanthan gum-glycerol carrier exhibited fast carrier dissolution (1 h) and TCP mineralization (7 days) in vitro, but induced inflammation and showed little ectopic bone formation. This carrier chemistry was thus found to disrupt the early cellular response related to osteoinduction by microstructured TCP. TCP formulations based on carboxymethyl cellulose-glycerol and Polyoxyl 15-hydroxystearate-Pluronic(®) F127 allowed the in vitro surface mineralization of TCP by day 7 and produced the highest level of orthotopic bone bridging and ectopic bone formation, which was equivalent to the control. These results demonstrate that water-free carriers can preserve the chemistry, microstructure, and performance of osteoinductive CaP ceramics.

摘要

具有成骨诱导性的磷酸钙 (CaP) 陶瓷可以与聚合物载体结合,制成可塑的骨替代物,以替代自体骨;然而,含有水的载体可能会降解陶瓷表面的微观结构,这对骨形成至关重要。在这项研究中,从无水聚合物粘合剂和不同粒径的具有成骨诱导性的 TCP 颗粒(500-1000μm 用于可模塑腻子形式,150-500μm 用于可流动糊剂形式)中设计了五种新型的磷酸三钙 (TCP) 配方。研究了这些新型 TCP 配方的性能,并与单独的对照 TCP 颗粒(150-500μm 和 500-1000μm)进行了比较。体外,通过载体溶解时间和模拟体液中 TCP 矿化动力学曲线对五种 TCP 配方进行了表征。体内,将这些配方植入狗的背肌和单皮质股骨缺损(Ø=5mm)中 12 周。基于黄原胶-甘油载体的 TCP 配方在体外具有快速的载体溶解(1 小时)和 TCP 矿化(7 天),但会引起炎症,异位骨形成很少。因此,发现这种载体化学物质破坏了与微结构 TCP 相关的成骨诱导的早期细胞反应。基于羧甲基纤维素-甘油和聚氧乙烯 15-羟基硬脂酸酯-泊洛沙姆(®)F127 的 TCP 配方允许 TCP 在第 7 天表面矿化,并产生最高水平的原位骨桥接和异位骨形成,与对照物相当。这些结果表明,无水载体可以保持具有成骨诱导性的 CaP 陶瓷的化学性质、微观结构和性能。

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