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聚乙烯吡咯烷酮碘-聚(ε-己内酯)共混物对大肠杆菌黏附的抗性

The resistance of polyvinylpyrrolidone-iodine-poly(-caprolactone) blends to adherence of Escherichia coli.

作者信息

Jones David S, Djokic Jasmina, Gorman Sean P

机构信息

Medical Devices Group, School of Pharmacy, The Queen's University of Belfast, Medical Biology Centre, 97 Lisburn Road, Belfast BT9 7BL, Northern Ireland, UK.

出版信息

Biomaterials. 2005 May;26(14):2013-20. doi: 10.1016/j.biomaterials.2004.06.001.

Abstract

In this study, the resistance of biodegradable biomaterials, composed of blends of poly(-caprolactone) (PCL) and the polymeric antimicrobial complex, polyvinylpyrrolidone-iodine (PVP-I) to the adherence of a clinical isolate of Escherichia coli is described. Blends of PCL composed of a range of high (50,000 g mol(-1)) to low (5000 g mol(-1)) molecular weight ratios of polymer and either devoid of or containing PVP-I (1% w/w) were prepared by solvent evaporation. Following incubation (4 h), there was no relationship between m. wt. ratio of PCL in films devoid of PVP-I and adherence of E. coli. Conversely, microbial adherence to PCL containing PVP-I decreased as the ratio of high:low m. wt. polymer was decreased and was approximately 1000 fold lower than that to comparator films devoid of PVP-I. Following periods of immersion of PVP-I containing PCL films under sink conditions in phosphate buffered saline, subsequent adherence of E. coli was substantially reduced for 2 days (40:60 m. wt. ratio) and 6 days (100:0 m. wt. ratio). Concurrent exposure of PCL and E. coli to sub-minimum inhibitory concentrations (sub-MIC) of PVP-I significantly reduced microbial adherence to the biomaterial; however, the molecular weight ratio of PCL did not affect this outcome. Pretreatment of PCL with similar sub-MIC of PVP-I prior to inclusion within the microbial adherence assay significantly decreased the subsequent adherence of E. coli. Greatest reduction in adherence was observed following treatment of PCL (40:60 m. wt. ratio) with 0.0156% w/w PVP-I. In conclusion, this study has illustrated the utility of PVP-I as a suitable therapeutic agent for incorporation within PCL as a novel biomaterial. Due to the combined antimicrobial and biodegradable properties, these biomaterials offer a promising strategy for the reduction in medical device related infection.

摘要

在本研究中,描述了由聚(ε-己内酯)(PCL)与聚合物抗菌复合物聚乙烯吡咯烷酮碘(PVP-I)的混合物组成的可生物降解生物材料对临床分离的大肠杆菌黏附的抗性。通过溶剂蒸发制备了一系列高分子量(50,000 g mol⁻¹)与低分子量(5000 g mol⁻¹)聚合物比例且不含或含有PVP-I(1% w/w)的PCL混合物。孵育(4小时)后,不含PVP-I的薄膜中PCL的分子量比与大肠杆菌的黏附之间没有关系。相反,随着高分子量:低分子量聚合物比例的降低,微生物对含PVP-I的PCL的黏附减少,且比不含PVP-I的对照薄膜低约1000倍。将含PVP-I的PCL薄膜在水槽条件下浸泡于磷酸盐缓冲盐水中一段时间后,大肠杆菌的后续黏附在2天(40:60分子量比例)和6天(100:0分子量比例)时显著降低。PCL和大肠杆菌同时暴露于PVP-I的亚最小抑菌浓度(亚MIC)下可显著降低微生物对生物材料的黏附;然而,PCL的分子量比不影响这一结果。在微生物黏附试验中加入PVP-I之前,用类似亚MIC的PVP-I对PCL进行预处理可显著降低大肠杆菌随后的黏附。在用0.0156% w/w PVP-I处理PCL(40:60分子量比例)后,观察到黏附减少最多。总之,本研究说明了PVP-I作为一种合适的治疗剂用于掺入PCL作为新型生物材料的实用性。由于其抗菌和可生物降解的综合特性,这些生物材料为减少与医疗器械相关的感染提供了一种有前景的策略。

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