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埃洛石纳米管作为万古霉素在藻酸盐基伤口敷料中的载体。

Halloysite nanotubes as carriers of vancomycin in alginate-based wound dressing.

作者信息

Kurczewska Joanna, Pecyna Paulina, Ratajczak Magdalena, Gajęcka Marzena, Schroeder Grzegorz

机构信息

Faculty of Chemistry, Adam Mickiewicz University in Poznań, Umultowska 89b, 61-614 Poznań, Poland.

Department of Genetics and Pharmaceutical Microbiology, Poznan University of Medical Sciences, Święcickiego 4, 60-781 Poznań, Poland.

出版信息

Saudi Pharm J. 2017 Sep;25(6):911-920. doi: 10.1016/j.jsps.2017.02.007. Epub 2017 Feb 16.

Abstract

The influence of an inorganic support - halloysite nanotubes - on the release rate and biological activity of the antibiotic encapsulated in alginate-based dressings was studied. The halloysite samples were loaded with approx. 10 wt.% of the antibiotic and then encapsulated in Alginate and Gelatin/Alginate gels. The material functionalized with aliphatic amine significantly extended the release of vancomycin from alginate-based gels as compared to that achieved when silica was used. After 24 h, the released amounts of the antibiotic immobilized at silica reached 70%, while for the drug immobilized at halloysite the released amount of vancomycin reached 44% for Alginate discs. The addition of gelatin resulted in even more prolonged sustained release of the drug. The antibiotic was released from the system with a double barrier with Higuchi kinetic model and Fickian diffusion mechanism. Only the immobilized drug encapsulated in Alginate gel demonstrated very good antimicrobial activity against various bacteria. The inhibition zones were greater than those of the standard discs for the staphylococci and enterococci bacteria tested. The addition of gelatin adversely affected the biological activity of the system. The inhibition zones were smaller than those of the reference samples. A reduction in the drug dose by half had no significant effect on changing the release rate and microbiological activity. The toxicity studies of the material with immobilized drug were carried out with and . The material studied had no effect on the living organisms used in the bioassays. The proposed system with a double barrier demonstrated high storage stability.

摘要

研究了无机载体——埃洛石纳米管——对藻酸盐基敷料中封装抗生素释放速率和生物活性的影响。埃洛石样品负载了约10 wt.%的抗生素,然后封装在藻酸盐和明胶/藻酸盐凝胶中。与使用二氧化硅时相比,用脂肪胺功能化的材料显著延长了万古霉素从藻酸盐基凝胶中的释放。24小时后,固定在二氧化硅上的抗生素释放量达到70%,而对于固定在埃洛石上的药物,藻酸盐圆盘上万古霉素的释放量达到44%。明胶的加入导致药物的缓释时间更长。抗生素通过具有Higuchi动力学模型和菲克扩散机制的双屏障从系统中释放。只有封装在藻酸盐凝胶中的固定化药物对各种细菌表现出非常好的抗菌活性。对于所测试的葡萄球菌和肠球菌,抑菌圈大于标准圆盘。明胶的加入对系统的生物活性有不利影响。抑菌圈小于参考样品。药物剂量减半对改变释放速率和微生物活性没有显著影响。对固定化药物材料进行了毒性研究。所研究的材料对生物测定中使用的生物体没有影响。所提出的双屏障系统显示出高储存稳定性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9590/5605850/1aabddb8c0a4/gr1.jpg

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