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本文引用的文献

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Evaluation of potential factors contributing to microbiological treatment failure in Streptococcus pyogenes pharyngitis.化脓性链球菌性咽炎微生物治疗失败潜在因素的评估。
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Biofilms, antimicrobial resistance, and airway infection.生物膜、抗菌药物耐药性与气道感染
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Biofilms: microbial life on surfaces.生物膜:表面的微生物群落。
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Practice guidelines for the diagnosis and management of group A streptococcal pharyngitis. Infectious Diseases Society of America.A组链球菌性咽炎诊断和管理实践指南。美国传染病学会。
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A component of innate immunity prevents bacterial biofilm development.先天性免疫的一个组成部分可阻止细菌生物膜的形成。
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Biofilm bacteria: formation and comparative susceptibility to antibiotics.生物膜细菌:形成及对抗生素的敏感性比较
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Detection of differential gene expression in biofilm-forming versus planktonic populations of Staphylococcus aureus using micro-representational-difference analysis.使用微代表性差异分析检测金黄色葡萄球菌生物膜形成群体与浮游群体中的差异基因表达。
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Growth rate and biofilm thickness of Streptococcus sobrinus and Streptococcus mutans on hydroxapatite.变形链球菌和远缘链球菌在羟基磷灰石上的生长速率及生物膜厚度
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Riddle of biofilm resistance.生物膜抗性之谜。
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A组链球菌生物膜的形成:与治疗失败是否有关?

Biofilm formation by group a streptococci: is there a relationship with treatment failure?

作者信息

Conley Joslyn, Olson Merle E, Cook Linda S, Ceri Howard, Phan Van, Davies H Dele

机构信息

Department of Community Health Sciences, University of Calgary, Calgary, Canada.

出版信息

J Clin Microbiol. 2003 Sep;41(9):4043-8. doi: 10.1128/JCM.41.9.4043-4048.2003.

DOI:10.1128/JCM.41.9.4043-4048.2003
PMID:12958223
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC193794/
Abstract

Group A streptococcus (GAS) is the primary cause of bacterial pharyngitis in children and adults. Up to one-third of patients treated for GAS pharyngitis fail to respond to antibiotic therapy. The objective of this cohort study was to evaluate GAS biofilm formation as a mechanism for antibiotic treatment failure using previously collected GAS isolates and penicillin treatment outcome data. The minimum biofilm eradication concentration (MBEC) assay device was used to determine the biofilm-forming capabilities, efficiencies, and antibiotic susceptibilities of GAS isolates. The MBECs and MICs of several antibiotics for GAS were determined. All 99 GAS isolates available for this study formed biofilms, with various efficiencies. Antibiotic MBECs were consistently higher than MICs for all of the GAS isolates. MBECs indicated penicillin insensitivity in 60% of GAS isolates, producing the first report of in vitro GAS insensitivity to penicillin. Using MBECs to predict penicillin treatment failure had better sensitivity (56%) but lower specificity (36%) than the sensitivity (0%) and specificity (100%) when MICs were used. However, the positive predictive value of the MBEC was superior to that of the MIC (56 versus 0%), while the negative predictive values (42 and 47%) were similar. More studies are needed to understand the roles of biofilms and the MBEC assay in predicting GAS treatment failure. In addition, further investigations are necessary to determine if non-biofilm-forming strains of GAS exist and the roles of in vivo monospecies and multispecies biofilms in streptococcal pharyngitis treatment failure.

摘要

A组链球菌(GAS)是儿童和成人细菌性咽炎的主要病因。接受GAS咽炎治疗的患者中,多达三分之一对抗生素治疗无反应。这项队列研究的目的是利用先前收集的GAS分离株和青霉素治疗结果数据,评估GAS生物膜形成作为抗生素治疗失败的一种机制。使用最低生物膜清除浓度(MBEC)测定装置来确定GAS分离株的生物膜形成能力、效率和抗生素敏感性。测定了几种抗生素对GAS的MBEC和MIC。本研究可用的所有99株GAS分离株均形成了生物膜,效率各不相同。所有GAS分离株的抗生素MBEC始终高于MIC。MBEC表明60%的GAS分离株对青霉素不敏感,这是首次关于体外GAS对青霉素不敏感的报道。与使用MIC时的敏感性(0%)和特异性(100%)相比,使用MBEC预测青霉素治疗失败具有更好的敏感性(56%)但特异性较低(36%)。然而,MBEC的阳性预测值优于MIC(56%对0%),而阴性预测值(42%和47%)相似。需要更多的研究来了解生物膜和MBEC测定在预测GAS治疗失败中的作用。此外,有必要进一步研究是否存在不形成生物膜的GAS菌株,以及体内单物种和多物种生物膜在链球菌性咽炎治疗失败中的作用。