首页> 外文期刊>RSC Advances >Role of a nitrogenous bisphosphonate (local delivery) incorporated vitreous coating (with/without polymer) on surgical grade SS316L implant material to improve fixation at the damaged tissue site
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Role of a nitrogenous bisphosphonate (local delivery) incorporated vitreous coating (with/without polymer) on surgical grade SS316L implant material to improve fixation at the damaged tissue site

机译:在手术级SS316L植入材料上掺入含双膦酸的氮(局部递送)玻璃涂层(有/无聚合物)在改善受损组织部位固定方面的作用

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摘要

Nitrogenous bisphosphonate, alendronate sodium (AS) was incorporated in the bilayered (layer 1, impervious and layer 2, porous) vitreous coating of phosphate free bioactive glass (PFBG) coated on surgical grade SS316L blocks, for a possible treatment of peri implant bone loss as a consequence of implantation at the fracture site, by local delivery. The presence of the drug in the pores (dia: 0.5-8 mm) of layer 2 was confirmed by SEM-EDX analysis. To control the drug release and thereby improve the efficacy of the system, the drug loaded vitreous layer was further coated with a thin layer (thickness: 1-2 mm) of poly(D, L-lactic-co-glycolic acid, PLGA). Irrespective of the polymer coating, the drug release kinetics were diffusion controlled from a porous matrix and the drug was fluorescently tagged and internalized by mouse macrophage cells (RAW 264.7) which was analysed by flow cytometry (FACS), followed by assessing the time dependent inhibitory action of the above drug on the osteoclastogenic cytokine, TNF alpha of the RAW 264.7 cell line, demonstrated by ELISA (enzyme-linked immunosorbent assay), and the same was confirmed and correlated by the time dependent growth inhibition of the transfected (from RAW 264.7 cell line) osteoclast cells by quantitative TRAP staining. The in vivo animal trial exhibited angiogenesis and initiation of bone remodelling in a New Zealand white rabbit model during the study period of 90 days, with or without a polymer coating and this mutual comparison has been highlighted in all the in vitro characterisation results too. In summary, an attempt has been made herewith to establish the versatility of alendronate sodium to promote improved fixation of the PFBG coated SS316L load bearing implants at the damaged tissue site, exhibiting an overall better response in the case of its polymer coated counterpart via an extended release profile, leading to a higher possibility of bone regeneration.
机译:将含氮的双膦酸盐,阿仑膦酸钠(AS)掺入无磷生物活性玻璃(PFBG)的双层(第1层,不渗透层和第2层,多孔)玻璃体涂层中,该玻璃涂层涂覆在手术级SS316L块上,可能用于治疗种植体周围骨丢失由于在局部植入而植入骨折部位。通过SEM-EDX分析确认了在层2的孔(直径:0.5-8mm)中药物的存在。为了控制药物释放并由此改善系统的功效,在载有药物的玻璃体层上进一步涂覆了一层聚(D,L-乳酸-乙醇酸,PLGA)薄层(厚度:1-2 mm) 。不论聚合物包衣如何,药物释放动力学都是从多孔基质扩散控制的,并且通过小鼠巨噬细胞(RAW 264.7)进行荧光标记和内化,然后通过流式细胞术(FACS)进行分析,然后评估时间依赖性抑制作用。 ELISA(酶联免疫吸附试验)证实了上述药物对破骨细胞生成细胞因子RAW 264.7细胞系的TNFα的作用,并且通过转染的时间依赖性生长抑制作用证实了上述药物的相关性(与RAW 264.7比较)细胞系)破骨细胞通过定量TRAP染色。这项体内动物试验在90天的研究期内,无论有无聚合物涂层,在新西兰白兔模型中均显示出血管生成和骨骼重塑的开始,并且这种相互比较在所有体外表征结果中也得到了强调。总而言之,已尝试建立阿仑膦酸钠的多功能性,以促进改进的PFBG涂层的SS316L负重植入物在受损组织部位的固定,在其聚合物涂层对应物通过延长的情况下表现出总体上更好的响应释放曲线,导致骨骼再生的可能性更高。

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