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The efficacy of topical agents in the treatment of bacterial biofilms: an in vivo sheep study and an in vitro study.

机译:局部药剂在治疗细菌生物膜中的功效:体内绵羊研究和体外研究。

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摘要

Introduction: Recent evidence has demonstrated the presence of bacterial biofilms on the mucosa of patients with Chronic Rhinosinusitis (CRS), suggesting their role in the pathogenesis of the condition. This thesis contains two separate studies. The studies investigated novel topical therapies by using previously established in vitro and in vivo biofilm growth and detection methods. In the first study, several different proposed anti-biofilm agents were evaluated in a sheep biofilm model, each with varying degrees of immediate and short-term success against Staphylococcus aureus biofilms. A second study was conducted to determine the in vitro anti-bacterial and anti-biofilm properties of Chitosan/Dextran (CD) gel, a novel chitosan-based product with remarkable mucosal healing and haemostatic properties. Methods: Three alternative anti-biofilm treatments: Mupirocin, CAZS (Citric Acid Zwitterionic Acid) and Gallium Nitrate were evaluated in a prospective randomized controlled single-blinded trial using a previously established sheep biofilm model of CRS. The sheep mucosal samples were analyzed for presence of S. aureus biofilms using BacLight staining and CLSM, and the degree of biofilm involvement was determined using FISH (Fluorescence In-Situ Hybridization). The MIC/MBC values for CD gel and its constituents were determined by macro-dilution methods described by Jorgensen et al.[1]. Established in vitro biofilms grown from common CRS pathogens (ATCC strains and clinical isolates) were subjected to treatment by CD gel and its components (chitosan and dextran). A 96-well micro-titre crystal-violet staining method described by O’Toole and Kolter [2] was used to determine the anti-biofilm profile of CD gel against several bacterial strains with known biofilm-forming capacity. Results: Following 8 days of inoculation with S. aureus, all treatment groups in the sheep biofilm model showed a statistically significant reduction in biofilm surface coverage compared to no treatment. Importantly, sheep frontal sinuses treated with twice-daily mupirocin flushes for 5 days showed almost negligible biofilm growth after the follow-up period of 8 days (0.84% ± 1.25% surface area coverage per visual field). The overall data from the in vitro studies suggest that CD gel has marked anti-microbial activity against planktonic and biofilm-forming bacteria. It was inhibitory and bacteriocidal at sub-clinical concentrations (25mg/mL) for all bacteria tested except for E. coli. When tested against a nutrient-free environment as well as a positive growth control, bacteria were essentially unable to grow in its presence. Conclusion: Recalcitrant CRS is a difficult condition to manage and its pathogenesis has been closely linked to the presence of bacterial biofilms. Using a standardized biofilm sheep model of CRS, regular treatment with mupirocin flushes over a 5 day period showed an almost complete eradication of biofilms as assessed by mucosal surface coverage, with sustained effects over the 8 day period of follow-up. Equally as efficacious in the in vitro setting, CD gel demonstrated potent anti-bacterial and anti-biofilm activity against a number of pathogenic organisms suspected of being involved in acute and chronic rhinosinusitis. CD gel’s favourable haemostatic and mucosal healing profile posits it as an ideal post-ESS packing material. These two topical agents therefore hold promise as effective treatment options in the management of CRS.
机译:简介:最近的证据表明,慢性鼻鼻窦炎(CRS)患者的粘膜上存在细菌生物膜,表明它们在该病的发病机理中发挥了作用。本文包含两个单独的研究。该研究通过使用先前建立的体外和体内生物膜生长和检测方法,研究了新型的局部疗法。在第一个研究中,在绵羊生物膜模型中评估了几种不同的拟议抗生物膜剂,每种抗生物膜剂对金黄色葡萄球菌生物膜的近期和短期成功率都不同。进行了第二项研究,以确定壳聚糖/右旋糖酐(CD)凝胶的体外抗菌和抗生物膜特性,这是一种新型的壳聚糖基产品,具有出色的粘膜愈合和止血性能。方法:在一项前瞻性随机对照单盲试验中,使用先前建立的CRS绵羊生物膜模型,评估了三种替代的抗生物膜治疗方法:莫匹罗星,CAZS(柠檬酸两性离子酸)和硝酸镓。使用BacLight染色和CLSM分析绵羊粘膜样品中金黄色葡萄球菌生物膜的存在,并使用FISH(荧光原位杂交)确定生物膜的参与程度。 CD凝胶及其成分的MIC / MBC值通过Jorgensen等人[1]所述的宏观稀释方法确定。从常见CRS病原体(ATCC菌株和临床分离株)生长的已建立的体外生物膜,通过CD凝胶及其成分(壳聚糖和右旋糖酐)进行处理。 O’Toole和Kolter [2]描述的96孔微滴定结晶紫染色方法用于确定CD凝胶对几种具有已知生物膜形成能力的细菌的抗生物膜特性。结果:接种金黄色葡萄球菌8天后,与未处理相比,绵羊生物膜模型中的所有处理组均显示出生物膜表面覆盖率的统计学显着降低。重要的是,在连续8天的随访期内,每天两次用莫匹罗星冲洗5天的绵羊额窦显示出几乎可以忽略的生物膜生长(每个视野的表面积为0.84%±1.25%)。体外研究的总体数据表明CD凝胶对浮游细菌和生物膜形成细菌具有显着的抗微生物活性。在亚临床浓度(25mg / mL)下,除大肠杆菌外,所有细菌均具有抑制和杀菌作用。当在无营养的环境以及阳性生长控制下进行测试时,细菌在存在时基本上无法生长。结论:顽固性CRS是一种难以控制的疾病,其发病机理与细菌生物膜的存在密切相关。使用标准化的生物膜绵羊CRS模型,在5天的时间内定期用莫匹罗星冲洗治疗,通过粘膜表面覆盖评估,生物膜几乎完全根除,并在8天的随访期内具有持续作用。在体外环境中,CD凝胶同样有效,对多种怀疑与急性和慢性鼻-鼻窦炎有关的病原生物具有有效的抗菌和抗生物膜活性。 CD凝胶具有良好的止血和粘膜愈合特性,是理想的ESS后包装材料。因此,这两种局部用药有望在CRS的治疗中作为有效的治疗选择。

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    Le Tong Ba;

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  • 年度 2010
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  • 正文语种 {"code":"en","name":"English","id":9}
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