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Biomimetic matrix mediated room temperature synthesis and characterization of nano-hydroxyapatite towards targeted drug delivery

机译:仿生基质介导的室温合成与纳米羟基磷灰石朝向靶向药物递送的

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The nucleation and growth of hydroxyapatite is closely associated with the extracellular matrix environment. Bovine serum albumin, collagen and polyvinyl alcohol were used to mimic the extracellular matrix. An attempt to understand the role of these matrices on the synthesis and function of hydroxyapatite has been made. XRD, FT-IR, XPS, TG-DTA, SEM and TEM confirmed the formation of hydroxyapatite synthesized by the biomimetic route. Further, the role of the organic matrix in controlling the nucleation and growth of hydroxyapatite particles at the nano level is understood by in-depth analysis of the XPS spectra. The in vitro release of the anti-cancer drug methotrexate in aqueous solution was studied, and the in vitro release profile was assayed by elution in phosphate buffered saline with pH 7.4 and pH 5 at 37 degrees C. The percentage of loading and release profiles of the drug were evaluated. The results show that the use of the matrix increased the drug release efficiency from 44.5% to 66% at pH 7.4 and 78% to 98.92% at pH 5. These results suggest that the synthesized hydroxyapatite can be used as a pH responsive vehicle for delivering drugs. Further, the release profile was predicted by the Higuchi and Peppas models. The results suggest that the release mechanism is governed by Fickian diffusion for the initial 8 h followed by anomalous transport for longer times. The cytocompatibility of the materials was evaluated by in vitro cytotoxicity tests. Both MTT and live/dead assay observations indicated that the material had no adverse impact on cell proliferation. The results imply that these composites are bioactive with good cytocompatibility. Although all the matrices showed good results, the one with polyvinyl alcohol exhibited higher biocompatibility and drug release efficiency. A plausible explanation is proposed for the enhanced drug delivery efficiency of these materials.
机译:羟基磷灰石的成核和生长与细胞外基质环境密切相关。牛血清白蛋白,胶原和聚乙烯醇用于模拟细胞外基质。试图了解这些基质对羟基磷灰石合成和功能的作用。 XRD,FT-IR,XPS,TG-DTA,SEM和TEM证实了由仿生途径合成的羟基磷灰石的形成。此外,通过对XPS光谱的深入分析,理解有机基质在控制纳米水平下羟基磷灰石颗粒的成核和生长的作用。研究了水溶液中抗癌药物甲氨蝶呤的体外释放,并通过在pH 7.4和pH5的磷酸盐缓冲盐水中洗脱,在37摄氏度下进行体外释放曲线。装载和释放型材的百分比评估药物。结果表明,在pH7.4和6.4%和78%至98.92%的pH 5时,使用基质的使用将药物释放效率从44.5%增加到66.92%增加到78%至98.92%。这些结果表明合成的羟基磷灰石可用作pH响应型车辆进行送达药物。此外,HIGUCHI和PEPPAS模型预测了释放曲线。结果表明,释放机制由Fickian扩散管辖,使初始8 H,然后是长时间的异常运输。通过体外细胞毒性试验评估材料的细胞组分。 MTT和Live / Dead测定观察结果表明,该材料对细胞增殖没有不利影响。结果意味着这些复合材料具有良好的细胞组合性的生物活性。尽管所有基质表现出良好的结果,但具有聚乙烯醇的效果较高,呈较高的生物相容性和药物释放效率。提出了一种可合理的解释,用于增强这些材料的药物输送效率。

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  • 来源
    《RSC Advances 》 |2016年第67期| 共16页
  • 作者单位

    Acad Sci &

    Innovat Res AcSIR New Delhi India;

    Acad Sci &

    Innovat Res AcSIR New Delhi India;

    Acad Sci &

    Innovat Res AcSIR New Delhi India;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 化学 ;
  • 关键词

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