Center of Sports Medicine, Department of Sports Medicine, Huashan Hospital, Fudan University, Shanghai 200040, People's Republic of China.
Int J Nanomedicine. 2019 Jul 4;14:4881-4893. doi: 10.2147/IJN.S210687. eCollection 2019.
This study was designed to evaluate the in vitro and in vivo biocompatibility and osteointegration of plasma-sprayed hydroxyapatite (HA)-coated polyethylene terephthalate (PET) ligaments encapsulated with a simvastatin (SV)-chitosan (CS) composite.
This study compared the in vitro and in vivo bone responses to three different PET ligaments: SV/CS/PET-HA, CS/PET-HA and PET-HA. A field emission scanning electron microscope was used to characterize the morphology, and the in vitro SV release profile was analyzed. MC3T3 cells were cocultured with SV/CS/PET-HA, CS/PET-HA and PET-HA to test their biocompatibility using CCK-8 tests. Osteogenic differentiation was investigated by the expression of marker genes using qPCR. Osteointegration was performed by implanting the PET ligaments into the proximal tibia bone tunnels of male Sprague-Dawley rats for 3 weeks and 6 weeks. The bone-implant interface was evaluated by micro-computed tomography (micro-CT) and histological analysis.
The characteristic nanoporous structures mainly formed on the surface of the plasma-sprayed HA particles in the SV/CS/PET-HA and CS/PET-HA groups. The SV release test showed that the sustained release of simvastatin lasted for 25 days in the SV/CS/PET-HA group. The in vitro studies demonstrated that the SV/CS/PET-HA ligaments induced osteogenic differentiation in the MC3T3 cells, with higher mRNA expression levels of collagen-1, bone morphogenetic protein-2, osteocalcin and alkaline phosphatase than those in the CS/PET-HA and PET-HA ligament groups. The in vivo tests showed that both micro-CT analysis (bone mineral density and bone volume per total volume) and histological analysis (bone implant contact and interface area) revealed significantly higher peri-implant bone formation and less interface area in the SV/CS/PET-HA group than in the other groups.
The SV-CS composite nanoporous structure was associated with the improved biocompatibility and osteogenic differentiation in vitro and enhanced osteointegration process in vivo of plasma-sprayed HA-coated PET ligaments.
本研究旨在评估包被辛伐他汀(SV)-壳聚糖(CS)复合材料的等离子喷涂羟基磷灰石(HA)涂层的聚乙烯 terephthalate(PET)韧带的体外和体内生物相容性和骨整合。
本研究比较了三种不同的 PET 韧带的体外和体内骨反应:SV/CS/PET-HA、CS/PET-HA 和 PET-HA。使用场发射扫描电子显微镜(FESEM)对形态进行了表征,并分析了体外 SV 释放曲线。通过 CCK-8 试验检测 SV/CS/PET-HA、CS/PET-HA 和 PET-HA 与 MC3T3 细胞的共培养物的生物相容性。通过 qPCR 检测标记基因的表达研究成骨分化。通过将 PET 韧带植入雄性 Sprague-Dawley 大鼠的胫骨近端骨隧道中 3 周和 6 周来进行骨整合。通过微计算机断层扫描(micro-CT)和组织学分析评估骨-植入物界面。
SV/CS/PET-HA 和 CS/PET-HA 组中,等离子喷涂 HA 颗粒表面主要形成特征性纳米多孔结构。SV 释放试验表明,SV/CS/PET-HA 组中辛伐他汀的持续释放可持续 25 天。体外研究表明,SV/CS/PET-HA 韧带在 MC3T3 细胞中诱导成骨分化,其胶原-1、骨形态发生蛋白-2、骨钙素和碱性磷酸酶的 mRNA 表达水平均高于 CS/PET-HA 和 PET-HA 韧带组。体内试验表明,微 CT 分析(骨矿物质密度和骨体积/总体积)和组织学分析(骨植入物接触和界面面积)均显示,SV/CS/PET-HA 组的植入物周围骨形成明显更高,界面面积明显更小。
SV-CS 复合纳米多孔结构与体外提高的生物相容性和成骨分化以及体内等离子喷涂 HA 涂层的 PET 韧带增强的骨整合过程有关。
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