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The Role of Polydimethylsiloxane in the Molecular Structure of Silica Xerogels Intended for Drug Carriers

机译:聚二甲基硅氧烷在用于药物载体的硅胶干凝胶分子结构中的作用

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摘要

The aim of this study was to prepare and examine polymer/oxide xerogels with metronidazole (MT) as delivery systems for the local application of a drug to a bone. The nanoporous SiO2-CaO and PDMS-modified SiO2-CaO xerogel materials with different amounts of the polymer, polydimethylsiloxane (PDMS), were prepared by the sol-gel method.Characterization assays comprised the analysis of the composite materials by using Fourier transform infrared spectroscopy (FTIR), determining the specific surface area of solids (BET), using X-ray powder diffraction (XRD) and scanning electron microscope (SEM) techniques, and further monitoring in the ultraviolet and visible light regions (UV-Vis) of the in vitro release of the drug (metronidazole) over time. According to these results, the bioactive character and chemical stability of PDMS-modified silica xerogels have been proven.The release of MT from xerogels was strongly correlated with the composition of the matrix. In comparison with the pure oxide matrix, PDMS-modified matrices accelerated the release of the drug through its bigger pores, and additionally, on account of weaker interactions with the drug.The obtained results for the xerogel composites suggest that the metronidazole-loaded xerogels could be promising candidates for formulations in local delivery systems particularly to bone.
机译:这项研究的目的是准备和检查以甲硝唑(MT)为聚合物的药物/氧化物干凝胶,以将药物局部应用于骨骼。采用溶胶-凝胶法制备了纳米级SiO2-CaO和PDMS改性的SiO2-CaO干凝胶材料,并采用溶胶-凝胶法制备了聚二甲基硅氧烷(PDMS),表征实验包括傅立叶变换红外光谱法对复合材料的分析。 (FTIR),使用X射线粉末衍射(XRD)和扫描电子显微镜(SEM)技术确定固体的比表面积(BET),并进一步监测其的紫外和可见光区域(UV-Vis)随着时间的推移体外释放药物(甲硝唑)。根据这些结果,已经证明了PDMS改性的二氧化硅干凝胶的生物活性特征和化学稳定性。湿凝胶中MT的释放与基质的组成密切相关。与纯氧化物基质相比,PDMS改性的基质通过其较大的孔促进了药物的释放,此外,由于与药物的相互作用较弱。所得干凝胶复合材料的结果表明,装有甲硝唑的干凝胶可以有望成为局部递送系统(特别是骨)中制剂的有前途的候选人。

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