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涂覆抗生素的聚氨酯的抗菌活性:实现免微生物定植医疗设备的新方法。

Antimicrobial activity of polyurethanes coated with antibiotics: a new approach to the realization of medical devices exempt from microbial colonization.

作者信息

Piozzi A, Francolini I, Occhiaperti L, Venditti M, Marconi W

机构信息

Department of Chemistry, University La Sapienza, P.le Aldo Moro, Rome 00185, Italy.

出版信息

Int J Pharm. 2004 Aug 6;280(1-2):173-83. doi: 10.1016/j.ijpharm.2004.05.017.

Abstract

Intravascular devices are widely used for vascular access but are associated with substantial risk of development of devices-related bloodstream infection (DR-BSI), which causes a considerable increase of morbidity and mortality, prolonged hospitalisation and growing medical costs. Since conventional treatment of DR-BSI fails in a significant number of cases, resulting in removal of the device, new approaches are needed to prevent bacterial colonization. In this paper, two antibiotics, rifampin and amoxicillin, have been adsorbed on polyurethanes exhibiting acidic or basic properties. The influence of the type of antibiotic-polymer interaction on the amount of adsorbed antibiotic and on the release kinetics was studied. It was seen that the antibiotic-polymer affinity increases both with the introduction in the polymer side-chain of functional groups and with the matrix hydrophilicity. The antimicrobial activity of the treated polymers, evaluated in vitro by the Kirby-Bauer test, depends on the amount of antibiotic adsorbed, on the strength of drug-matrix interaction and on the water swelling of the polymers. The inhibition zone of bacterial growth lasts only a few hours for the amoxi-coated polymers while remains at least for five months for the rifampin-coated ones. The presence of serum proteins decreases by about 30% the inhibition zone diameter of these latest matrices after two months.

摘要

血管内装置被广泛用于血管通路,但与发生装置相关血流感染(DR-BSI)的重大风险相关,这会导致发病率和死亡率显著增加、住院时间延长以及医疗成本不断上升。由于DR-BSI的传统治疗在大量病例中失败,导致装置被移除,因此需要新的方法来防止细菌定植。在本文中,两种抗生素,利福平和阿莫西林,已被吸附在具有酸性或碱性性质的聚氨酯上。研究了抗生素-聚合物相互作用类型对吸附抗生素量和释放动力学的影响。可以看出,抗生素-聚合物亲和力随着聚合物侧链中官能团的引入以及基质亲水性的增加而增加。通过 Kirby-Bauer 试验在体外评估的处理后聚合物的抗菌活性取决于吸附的抗生素量、药物-基质相互作用的强度以及聚合物的水溶胀性。对于阿莫西林包被的聚合物,细菌生长抑制区仅持续几个小时,而对于利福平包被的聚合物,至少持续五个月。两个月后,血清蛋白的存在使这些最新基质的抑制区直径减小约30%。

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