大肠杆菌所致复发性尿路感染的重要细菌特征。

Danish medical bulletin Pub Date : 2011-04-01
Karen Ejrnæs
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Primary infecting E. coli causing persistence or relapse of the infection were associated with phylogenetic group B2, whereas primary infecting E. coli followed by cure or reinfection were associated with group D (Paper II). Phylogenetic group B2 was associated with susceptibility to many of the tested antimicrobials, whereas group A was associated with resistance to many of these antimicrobials and multidrug resistant (MDR) strains, and group D with MDR strains. Phylogenetic group A and D were associated with carriage of IncH and IncI plasmids, respectively. Resistance patterns or plasmid profiles of the primary infecting E. coli were not associated with outcome during follow-up (cure, persistence, reinfection or relapse) (Paper II). Resistance to ampicillin, sulfamethizole, streptomycin and tetracycline was associated with a lower prevalence of some VFGs (sfa/focDE, agn43bCFT073, chuA, iroN, cnf1, hlyD, ibeA, malX, usp) and higher prevalence of other VFGs (afa/draBC, agn43aCFT073, iha, iutA, sat) but the aggregate VFG score did not differ among the resistant and susceptible strains of these antimicrobials (Paper III). Primary infecting E. coli causing persistence or relapse showed to have a higher biofilm formation capacity in vitro than those being followed by cure or reinfection (Paper II). This indicates that biofilm may be an important determinant for developing RUTI and may support the observation of IBCs. Primary infecting E. coli causing relapse or persistence had a higher aggregate VFG score and higher prevalence of hemolysis and of many of the VFGs than those followed by cure or reinfection. 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引用次数: 0

摘要

尿路感染(uti)是临床实践中最常见的细菌感染性疾病之一,发病率高,医疗费用高。大肠杆菌是导致80-90%社区获得性尿路感染和30-50%医院获得性尿路感染的最主要病原体。据报道,25%的妇女在急性尿路感染发作后6个月内出现复发性尿路感染,这是一个重大问题。本论文的目的是寻找大肠杆菌引起的尿路感染复发的重要细菌特征。本论文以三篇论文为基础。该研究基于来自236名瑞典妇女的大肠杆菌,这些妇女患有社区获得性症状性下尿路感染,来自1162名接受哌美西林或安慰剂三种不同剂量方案之一治疗的患者的大型研究。在首次访问和两次预定的随访中,对这些妇女进行了临床和细菌学评估。根据脉冲场凝胶电泳(PFGE)和培养结果,将所有原代感染大肠杆菌(初始分离株、预处理株)分为初始感染后治愈、持续、再感染或随访期间复发。在初次感染的大肠杆菌中,毒力因子基因(vfg)、系统发育群、生物膜形成、质粒和抗微生物药物耐药性的流行率与治愈或再感染的大肠杆菌中这些基因的流行率进行了比较。以往使用基于表型的分型方法或特异性较低的基于DNA的分型方法对RUTI进行的研究得出结论,RUTI主要归因于新菌株的再感染。然而,应用PFGE显示,77%的ruti是由原发感染大肠杆菌的复发引起的(论文1)。这可能支持最近的观察,即大肠杆菌可以在小鼠膀胱内侵入和复制,形成生物膜样细胞内细菌群落(IBCs),并建立静止的细胞内宿主,这可能代表ruti的稳定宿主。IBC的致病周期尚未在人类中进行研究;然而,最近在急性无并发症膀胱炎妇女的尿液中检测到脱落的IBC,支持IBC途径的存在和一些UTI妇女细胞内细菌生态位的发生。经三联PCR检测,大肠杆菌可分为a、B1、B2和D 4个主要的系统发育类群,其中B2类群在原代感染大肠杆菌中最占优势,其次为D、a和B1类群。所检测的29个vfg中,大多数与系统发生组B2相关,而只有少数vfg在系统发生组中分布更广泛(论文III)。原发感染大肠杆菌导致感染持续或复发与系统发生组B2相关,而原发感染大肠杆菌后治愈或再感染与D组相关(论文II)。系统发生组B2与许多所测试的抗菌素的敏感性相关。而A组与对许多这些抗菌剂和耐多药菌株的耐药性有关,D组与耐多药菌株有关。系统发育类群A和D分别与携带IncH和IncI质粒相关。原发感染大肠杆菌的耐药模式或质粒谱与随访期间的结果(治愈、持续、再感染或复发)无关(论文II)。对氨苄西林、磺胺甲唑、链霉素和四环素的耐药与一些vfg (sfa/focDE、agn43bCFT073、chuA、iroN、cnf1、hlyD、ibeA、malX、usp)的较低患病率和其他vfg (afa/draBC、agn43aCFT073、iha、iutA、但这些抗菌素的耐药菌株和敏感菌株之间的VFG总分没有差异(论文III)。与那些治愈或再感染的大肠杆菌相比,初次感染导致持续或复发的大肠杆菌在体外具有更高的生物膜形成能力(论文II)。这表明生物膜可能是RUTI发展的重要决定因素,并可能支持IBCs的观察。原发感染大肠杆菌导致复发或持续存在的患者,其VFG总分、溶血率和许多VFG发生率高于治愈或再感染后的患者。与持续或复发相关的vgf包括:粘附素(sfa/focDE, papAH),生物膜相关因子(agn43),铁摄取系统(chuA, fyuA, iroN),保护因子(kpsM II, kpsMII K2),毒素(cnf1, hlyD), CFT073致病性相关岛的标记物(malX)和细菌素样因子(usp)。没有特定的vfg组合可以预测持续性或复发(论文III)。 大肠杆菌中至少有一种性状(系统发育组B2、sfa/focDE、papAH、agn43、chuA、fyuA、iroN、kpsM II、kpsM II K2、traT、cnf1、hlyD、ibeA、malX、usp和溶血性)呈阳性,与没有这些性状的原发性感染大肠杆菌接受三天治疗或不考虑这些性状的原发性感染大肠杆菌接受七天治疗相比,具有显著更高的持续或复发的发生率(论文III)。我们的结果可能支持大肠杆菌在膀胱细胞内蓄水池的假设。认识到尿路致病性大肠杆菌是一种潜在的细胞内病原体,对我们目前的尿路感染治疗方案提出了挑战,并主张开发新的抗菌药物或治疗方案/策略。没有明确的毒力谱可以预测RUTI。然而,我们发现与持续性或复发相关的vfg可能是预防和治疗UTI的潜在目标。此外,我们确定了潜在的标记物,可用于选择更差异化和最佳的治疗。未来的研究必须探索这些vfg和其他推测的和新的vfg在尿路感染持续或复发中的作用,以及它们在IBC形成中的可能作用。确定vfg的功能和机制可以促进开发新的诊断工具、方案和药物,以预防和治疗RUTI。
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Bacterial characteristics of importance for recurrent urinary tract infections caused by Escherichia coli.

Urinary tract infections (UTIs) are among the most common bacterial infectious diseases encountered in clinical practice and account for significant morbidity and high medical costs. Escherichia coli is the most predominant pathogen causing 80-90% of community-acquired UTIs and 30-50% of nosocomially-acquired UTIs. Recurrent UTIs (RUTIs) are reported in 25% of women within 6 months of an acute UTI episode and pose a major problem. The aim of the present thesis was to look for bacterial characteristics of importance for recurrence of UTI caused by E. coli. The thesis is based on three papers. The study is based on E. coli from 236 Swedish women with community-acquired symptomatic lower UTI from a large study of 1162 patients treated with one of three different dosing regimens of pivmecillinam or placebo. The women were evaluated clinically and bacteriologically at the initial visit and at two scheduled follow-up visits. According to pulsed-field gel electrophoresis (PFGE) and culture results all primary infecting E. coli (initial isolates, pretherapy) were assigned into whether the initial infection was followed by cure, persistence, reinfection or relapse during follow-up. The prevalence of virulence factor genes (VFGs), phylogenetic groups, biofilm formation, plasmids and resistance to antimicrobials among primary infecting E. coli causing persistence or relapse at the follow-up visits were compared with the prevalence of these among E. coli followed by cure or reinfection. Previous studies of RUTI using phenotypically based typing methods or less specific DNA based typing methods have concluded, that RUTIs are mainly attributable to reinfection with new strains. However, applying PFGE showed that 77% of RUTIs were caused by a relapse with the primary infecting E. coli (Paper I). This may support the recent observation that E. coli can invade and replicate within the murine bladder forming biofilm-like intracellular bacterial communities (IBCs) and establish quiescent intracellular reservoirs that may represent stable reservoirs for RUTIs. The IBC pathogenic cycle has not been studied in humans; however, recently exfoliated IBCs were detected in urine from women with acute uncomplicated cystitis supporting the presence of the IBC pathway and occurrence of an intracellular bacterial niche in some women with UTI. Based on a triplex PCR E. coli can be divided into four main phylogenetic groups (A, B1, B2 and D). Phylogenetic group B2 was the most predominant group among the primary infecting E. coli followed by group D, A and B1. The majority of the tested 29 VFGs were associated with phylogenetic group B2, whereas only a few VFGs were more broadly distributed among the phylogenetic groups (Paper III). Primary infecting E. coli causing persistence or relapse of the infection were associated with phylogenetic group B2, whereas primary infecting E. coli followed by cure or reinfection were associated with group D (Paper II). Phylogenetic group B2 was associated with susceptibility to many of the tested antimicrobials, whereas group A was associated with resistance to many of these antimicrobials and multidrug resistant (MDR) strains, and group D with MDR strains. Phylogenetic group A and D were associated with carriage of IncH and IncI plasmids, respectively. Resistance patterns or plasmid profiles of the primary infecting E. coli were not associated with outcome during follow-up (cure, persistence, reinfection or relapse) (Paper II). Resistance to ampicillin, sulfamethizole, streptomycin and tetracycline was associated with a lower prevalence of some VFGs (sfa/focDE, agn43bCFT073, chuA, iroN, cnf1, hlyD, ibeA, malX, usp) and higher prevalence of other VFGs (afa/draBC, agn43aCFT073, iha, iutA, sat) but the aggregate VFG score did not differ among the resistant and susceptible strains of these antimicrobials (Paper III). Primary infecting E. coli causing persistence or relapse showed to have a higher biofilm formation capacity in vitro than those being followed by cure or reinfection (Paper II). This indicates that biofilm may be an important determinant for developing RUTI and may support the observation of IBCs. Primary infecting E. coli causing relapse or persistence had a higher aggregate VFG score and higher prevalence of hemolysis and of many of the VFGs than those followed by cure or reinfection. The VFGs associated with persistence or relapse included: adhesins (sfa/focDE, papAH), a biofilm related factor (agn43), iron-uptake systems (chuA, fyuA, iroN), protectins (kpsM II, kpsMII K2), toxins (cnf1, hlyD), a marker of a pathogenicity-associated island from CFT073 (malX), and a bacteriocin-like factor (usp). No specific combination of VFGs could predict persistence or relapse (Paper III). A regimen of three days pivmecillinam therapy for primary infecting E. coli positive for at least one of a number of traits (phylogenetic group B2, sfa/focDE, papAH, agn43, chuA, fyuA, iroN, kpsM II, kpsM II K2, traT, cnf1, hlyD, ibeA, malX, usp and being hemolytic) gave a significantly higher prevalence of persistence or relapse as opposed to primary infecting E. coli subjected to three days therapy with absence of these traits or primary infecting E. coli subjected to seven days therapy irrespective of these traits (Paper III). In conclusion, our results may support the hypothesis of an intracellular reservoir of E. coli in the bladder. The recognition of uropathogenic E. coli as a potential intracellular pathogen challenges our current treatment regimens of UTI and argues for the development of new antimicrobials or treatment regimens/strategies. No distinct virulence profile could predict RUTI. However, we found VFGs associated with persistence or relapse that may be potential targets for prevention and treatment of UTI. Furthermore we identified potential markers that may be used to select a more differentiated and optimal treatment. Future studies must explore the function of these VFGs and other putative and novel VFGs in relation to persistence or relapse of UTI and their possible role in IBC formation. Defining the repertoire and mechanism of VFGs could facilitate the development of new diagnostic tools, regimens and drugs for prevention and treatment of RUTI.

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Danish medical bulletin
Danish medical bulletin 医学-医学:内科
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Impact of new advances in sex research on psychoanalytic theory. Global Mental Health : Anthropological Perspectives Cancer rates after kidney transplantation. Need for thyroidectomy in patients treated with radioactive iodide for benign thyroid disease. Stagnation in body mass index in Denmark from 1997/1998 to 2004/2005, but with geographical diversity.
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