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溶血、细胞毒素坏死因子1阳性和阴性大肠杆菌对人T24膀胱细胞的细胞毒性。

Cytotoxicity of hemolytic, cytotoxic necrotizing factor 1-positive and -negative Escherichia coli to human T24 bladder cells.

作者信息

Island M D, Cui X, Foxman B, Marrs C F, Stamm W E, Stapleton A E, Warren J W

机构信息

Division of Infectious Diseases, Department of Medicine, University of Maryland School of Medicine, Baltimore, Maryland, USA.

出版信息

Infect Immun. 1998 Jul;66(7):3384-9. doi: 10.1128/IAI.66.7.3384-3389.1998.

Abstract

Approximately one-half of Escherichia coli isolates from patients with cystitis or pyelonephritis produce the pore-forming cytotoxin hemolysin, a molecule with the capacity to lyse erythrocytes and a range of nucleated cell types. A second toxin, cytotoxic necrotizing factor 1 (CNF1), is found in approximately 70% of hemolytic, but rarely in nonhemolytic, isolates. To evaluate the potential interplay of these two toxins, we used epidemiological and molecular biologic techniques to compare the cytotoxicity of hemolytic, CNF1(+), and CNF1(-) cystitis strains toward human T24 bladder epithelial cells in vitro. A total of 29 isolates from two collections of cystitis-associated E. coli were evaluated by using methylene blue staining of bladder monolayers at 1-h intervals after inoculation with each strain. Most (20 of 29) isolates damaged or destroyed the T24 monolayer (less than 50% remaining) within 4 h after inoculation. As a group, CNF1(+) isolates from one collection (11 strains) were less cytotoxic at 4 h than the CNF1(-) strains in that collection (P = 0.009), but this pattern was not observed among isolates from the second collection (18 strains). To directly evaluate the role of CNF1 in cytotoxicity of hemolytic E. coli without the variables present in multiple clinical isolates, we constructed mutants defective in production of CNF1. Compared to the CNF1(+) parental isolates, no change in cytotoxicity was detected in these cnf1 mutants. Our results indicate that CNF1 does not have a detectable effect on the ability of hemolytic E. coli to damage human bladder cell monolayers in vitro.

摘要

从膀胱炎或肾盂肾炎患者中分离出的大肠杆菌,约有一半会产生形成孔道的细胞毒素溶血素,该分子能够裂解红细胞及一系列有核细胞类型。第二种毒素,即细胞毒性坏死因子1(CNF1),在约70%的溶血菌株中可检测到,但在非溶血菌株中很少见。为评估这两种毒素之间可能的相互作用,我们运用流行病学和分子生物学技术,在体外比较溶血、CNF1阳性和CNF1阴性膀胱炎菌株对人T24膀胱上皮细胞的细胞毒性。对接种每种菌株后每隔1小时的膀胱单层细胞进行亚甲蓝染色,以此评估来自两个膀胱炎相关大肠杆菌菌库的总共29株分离菌。大多数(29株中的20株)分离菌在接种后4小时内破坏或摧毁了T24单层细胞(剩余细胞少于50%)。作为一个整体,来自一个菌库的11株CNF1阳性分离菌在4小时时的细胞毒性低于该菌库中的CNF1阴性菌株(P = 0.009),但在来自第二个菌库的18株分离菌中未观察到这种模式。为在不存在多个临床分离株中所存在变量的情况下,直接评估CNF1在溶血大肠杆菌细胞毒性中的作用,我们构建了CNF1产生缺陷的突变体。与CNF1阳性亲本分离株相比,在这些cnf1突变体中未检测到细胞毒性的变化。我们的结果表明,CNF1对溶血大肠杆菌在体外损伤人膀胱细胞单层的能力没有可检测到的影响。

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