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尿路致病性Dr/Afa⁺大肠杆菌的Dra/AfaE黏附素介导孕鼠死亡。

Dra/AfaE adhesin of uropathogenic Dr/Afa+ Escherichia coli mediates mortality in pregnant rats.

作者信息

Wroblewska-Seniuk K, Selvarangan R, Hart A, Pladzyk R, Goluszko P, Jafari A, du Merle L, Nowicki S, Yallampalli C, Le Bouguénec C, Nowicki B

机构信息

Department of Obstetrics and Gynecology, Meharry University, Nashville, TN 37208, USA.

出版信息

Infect Immun. 2005 Nov;73(11):7597-601. doi: 10.1128/IAI.73.11.7597-7601.2005.

Abstract

Escherichia coli bearing adhesins of the Dr/Afa family frequently causes urogenital infections during pregnancy in humans and has been associated with mortality in pregnant rats. Two components of the adhesin, Dra/AfaE and Dra/AfaD, considered virulence factors, are responsible for bacterial binding and internalization. We hypothesize that gestational mortality caused by Dr/Afa+ E. coli is mediated by one of these two proteins, Dra/AfaE or Dra/AfaD. In this study, using afaE and/or afaD mutants, we investigated the role of the afaE and afaD genes in the mortality of pregnant rats from intrauterine infection. Sprague-Dawley rats, on the 17th day of pregnancy, were infected with the E. coli afaE+ afaD and afaE afaD+ mutants. The clinical E. coli strain (afaE+ afaD+) and the afaE afaD double mutant were used as positive and negative controls, respectively. The mortality rate was evaluated 24 h after infection. The highest maternal mortality was observed in the group infected with the afaE+ afaD+ strain, followed by the group infected with the afaE+ afaD strain. The mortality was dose dependent. The afaE afaD double mutant did not cause maternal mortality, even with the highest infection dose. The in vivo studies corresponded with the invasion assay, where the afaE+ strains were the most invasive (afaE+ afaD strain > afaE+ afaD+ strain), while the afaE mutant strains (afaE afaD+ and afaE afaD strains) seemed to be noninvasive. This study shows for the first time that the afaE gene coding for the AfaE subunit of Dr/Afa adhesin is involved in the lethal outcome of gestational infection in rats. This lethal effect associated with AfaE correlates with the invasiveness of afaE+ E. coli strains in vitro.

摘要

携带Dr/Afa家族黏附素的大肠杆菌经常在人类孕期引发泌尿生殖系统感染,并且与孕鼠死亡有关。黏附素的两个组分,Dra/AfaE和Dra/AfaD,被认为是毒力因子,负责细菌的黏附和内化。我们推测由Dr/Afa+大肠杆菌引起的孕期死亡是由这两种蛋白质之一,Dra/AfaE或Dra/AfaD介导的。在本研究中,我们使用afaE和/或afaD突变体,研究了afaE和afaD基因在孕鼠因宫内感染导致的死亡中的作用。在妊娠第17天的斯普拉格-道利大鼠被感染了大肠杆菌afaE+ afaD和afaE afaD+突变体。临床大肠杆菌菌株(afaE+ afaD+)和afaE afaD双突变体分别用作阳性和阴性对照。在感染后24小时评估死亡率。在感染afaE+ afaD+菌株的组中观察到最高的母体死亡率,其次是感染afaE+ afaD菌株的组。死亡率呈剂量依赖性。即使使用最高感染剂量,afaE afaD双突变体也不会导致母体死亡。体内研究与侵袭试验结果一致,其中afaE+菌株侵袭性最强(afaE+ afaD菌株> afaE+ afaD+菌株),而afaE突变菌株(afaE afaD+和afaE afaD菌株)似乎无侵袭性。本研究首次表明,编码Dr/Afa黏附素AfaE亚基的afaE基因参与了大鼠孕期感染的致死结局。这种与AfaE相关的致死效应与afaE+大肠杆菌菌株在体外的侵袭性相关。

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