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Characterization of AfaE adhesins produced by extraintestinal and intestinal human Escherichia coli isolates: PCR assays for detection of Afa adhesins that do or do not recognize Dr blood group antigens.

机译:肠道外和肠道人大肠杆菌分离物产生的AfaE粘附素的表征:PCR检测法,用于检测识别或不识别Dr血型抗原的Afa粘附素。

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摘要

Operons of the afa family are expressed by pathogenic Escherichia coli strains associated with intestinal and extraintestinal infections in humans and animals. The recently demonstrated heterogeneity of these operons (L. Lalioui, M. Jouve, P. Gounon, and C. Le Bouguénec, Infect. Immun. 67:5048-5059, 1999) was used to develop a new PCR assay for detecting all the operons of the afa family with a single genetic tool. This PCR approach was validated by investigating three collections of human E. coli isolates originating from the stools of infants with diarrhea (88 strains), the urine of patients with pyelonephritis (97 strains), and the blood of cancer patients (115 strains). The results obtained with this single test and those previously obtained with several PCR assays were closely correlated. The AfaE adhesins encoded by the afa operons are variable, particularly with respect to the primary sequence encoded by the afaE gene. The receptor binding specificities have not been determined for all of these adhesins; some recognize the Dr blood group antigen (Afa/Dr(+) adhesins) on the human decay-accelerating factor (DAF) as a receptor, and others (Afa/Dr(-) adhesins) do not. Thus, the afa operons detected in this study were characterized by subtyping the afaE gene using specific PCRs. In addition, the DAF-binding capacities of as-yet-uncharacterized AfaE adhesins were tested by various cellular approaches. The afaE8 subtype (Afa/Dr(-) adhesin) was found to predominate in afa-positive isolates from sepsis patients (75%); it was frequent in afa-positive pyelonephritis E. coli (55.5%) and absent from diarrhea-associated strains. In contrast, Afa/Dr(+) strains (regardless of the afaE subtype) were associated with both diarrhea (100%) and extraintestinal infections (44 and 25% in afa-positive pyelonephritis and sepsis strains, respectively). These data suggest that there is an association between the subtype of AfaE adhesin and the physiological site of the infection caused by afa-positive strains.
机译:afa家族的操纵子由与人和动物的肠和肠外感染有关的致病性大肠杆菌菌株表达。最近证明了这些操纵子的异质性(L. Lalioui,M。Jouve,P。Gounon和C. LeBouguénec,Infect。Immun。67:5048-5059,1999)被用于开发一种新的PCR检测方法,用于检测所有用单个遗传工具操纵afa家族的操纵子。通过研究三套人类大肠杆菌分离株来验证该PCR方法,这些分离株来自腹泻婴儿(88株)的粪便,肾盂肾炎患者的尿液(97株)和癌症患者的血液(115株)。通过该单一测试获得的结果与先前通过多种PCR分析获得的结果紧密相关。由afa操纵子编码的AfaE粘附素是可变的,特别是对于由afaE基因编码的一级序列而言。还没有确定所有这些粘附素的受体结合特异性。有些人认识到人类衰变促进因子(DAF)上的Dr血型抗原(Afa / Dr(+)粘附素)是受体,而其他人(Afa / Dr(-)粘附素)则不然。因此,本研究中检测到的afa操纵子的特征是使用特异性PCR对afaE基因进行亚型分析。另外,还通过各种细胞方法测试了尚未表征的AfaE粘附素的DAF结合能力。发现败血症患者的afa阳性分离株中afaE8亚型(Afa / Dr(-)粘附素)占主导(75%)。在Afa阳性肾盂肾炎(55.5%)中很常见,而在腹泻相关菌株中则没有。相反,Afa / Dr(+)菌株(与afaE亚型无关)与腹泻(100%)和肠外感染(在afa阳性肾盂肾炎和败血症菌株中分别占44%和25%)相关。这些数据表明,AfaE粘附素的亚型与由afa阳性菌株引起的感染的生理部位之间存在关联。

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