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首页> 外文期刊>Journal of Inclusion Phenomena and Macrocyclic Chemistry >Anew controlled release system of chlorhexidine and chlorhexidine:/ted inclusion compounds based on porous silica
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Anew controlled release system of chlorhexidine and chlorhexidine:/ted inclusion compounds based on porous silica

机译:基于多孔二氧化硅的洗必泰和洗必泰:/泰德包合物的新型控释系统

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The purpose of this study was to prepare and characterize a controlled release system based on porous silica loaded with chlorhexidine (Cx) and its inclusion compounds in β-cyclodextrin (βcd), and to evaluate its antimicrobial activity. Acetate chlorhexidine (CxA), gluconate chlorhexidine (CxG), βcd:hlorhexidine acetate 2:1 (βcd:CxA) and βcdxhlorhexidine gluconate 2:1 (βcd:CxG) were incorporated into porous silica. Drug loading was characterized by FTIR, powder X-ray diffraction, thermal analysis and BET, and was shown to be in an amorphous state and porous matrix. The kinetics release parameter of the drug was established, which showed that the Cx systems release profile followed zero order release until 400 h and Higuchi model release until 750 h, after the burst effect at the first 8 h. Chlorhexidine therapeutic range was reached near first hour for all systems. The chlorhexidine porous silica system was biologically active against Enterococcus faecalis and Candida albicans in vitro. The systems showed an efficient Cx controlled release modulated by the presence of the β-cyclodextrin and by the porous silica matrices, providing effective antimicrobial activity.
机译:这项研究的目的是基于载有洗必泰(Cx)及其在β-环糊精(βcd)中的包合物的多孔二氧化硅制备并表征控释系统,并评估其抗菌活性。将乙酸氯己定(CxA),葡萄糖酸氯己定(CxG),乙酸βcd:氯己定己酸酯2:1(βcd:CxA)和βcdx氯己定葡糖苷2:1(βcd:CxG)掺入多孔二氧化硅中。通过FTIR,粉末X射线衍射,热分析和BET对药物载量进行表征,并显示为无定形状态和多孔基质。建立了药物的动力学释放参数,该参数表明在最初的8 h爆发效应后,Cx系统的释放曲线遵循零阶释放直至400 h,Higuchi模型释放直至750 h。所有系统在接近第一个小时的时候都达到了洗必泰的治疗范围。氯己定多孔二氧化硅系统在体外对粪肠球菌和白色念珠菌具有生物活性。该系统显示出有效的Cx控释,其受β-环糊精的存在和多孔二氧化硅基质的调节,提供了有效的抗菌活性。

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