Leyton Denisse L, Sloan Joan, Hill Rebecca E, Doughty Steven, Hartland Elizabeth L
Department of Microbiology, School of Biomedical Sciences, Monash University, Clayton 3800, Victoria, Australia.
Infect Immun. 2003 Nov;71(11):6307-19. doi: 10.1128/IAI.71.11.6307-6319.2003.
Enterohemorrhagic Escherichia coli (EHEC) is a prominent, food-borne cause of diarrhea, bloody diarrhea, and the hemolytic uremic syndrome in industrialized countries. Most strains of EHEC carry the locus for enterocyte effacement (LEE) pathogenicity island, but a proportion of isolates from patients with severe disease do not carry LEE and very little is known about virulence factors in these organisms. LEE-negative strains of EHEC typically express Shiga toxin 2 and carry a large plasmid that encodes the production of EHEC hemolysin. In this study, we determined the nucleotide sequence of the transfer region of pO113, the large hemolysin plasmid from LEE-negative EHEC O113:H21 (EH41). This 63.9-kb region showed a high degree of similarity with the transfer region of R64, and pO113 was capable of self-transmission at low frequencies. Unlike R64 and the related dot/icm system of Legionella pneumophila, however, pO113 was unable to mobilize RSF1010. In addition, the pO113 transfer region encoded a novel high-molecular-weight serine protease autotransporter of Enterobacteriaceae (SPATE) protein, termed EpeA. Like other SPATEs, EpeA exhibited protease activity and mucinase activity, but expression was not associated with a cytopathic effect on epithelial cells. Analysis of a second high-molecular-weight secreted protein revealed that pO113 also encodes EspP, a cytopathic SPATE identified previously in EHEC O157:H7. The nucleotide sequences encoding the predicted beta-domains of espP and epeA were identical and also shared significant homology with a third SPATE protein, EspI. Both espP and epeA were detected in several LEE-negative clinical isolates of EHEC and thus may contribute to the pathogenesis of this subset of EHEC.
肠出血性大肠杆菌(EHEC)是工业化国家中引起腹泻、血性腹泻和溶血尿毒综合征的一种主要食源性病原体。大多数EHEC菌株携带肠细胞脱落位点(LEE)致病岛,但一部分重症患者分离株不携带LEE,对这些菌株中的毒力因子了解甚少。LEE阴性的EHEC菌株通常表达志贺毒素2,并携带一个编码EHEC溶血素产生的大质粒。在本研究中,我们测定了来自LEE阴性EHEC O113:H21(EH41)的大溶血素质粒pO113转移区域的核苷酸序列。这个63.9 kb的区域与R64的转移区域高度相似,并且pO113能够以低频率自我转移。然而,与R64以及嗜肺军团菌相关的dot/icm系统不同,pO113无法动员RSF1010。此外,pO113转移区域编码一种新型的肠杆菌科高分子量丝氨酸蛋白酶自转运蛋白(SPATE),称为EpeA。与其他SPATE一样,EpeA表现出蛋白酶活性和粘蛋白酶活性,但表达与对上皮细胞的细胞病变效应无关。对另一种高分子量分泌蛋白的分析表明,pO113还编码EspP,一种先前在EHEC O157:H7中鉴定出的具有细胞病变作用的SPATE。编码espP和epeA预测β结构域的核苷酸序列相同,并且与第三种SPATE蛋白EspI也有显著同源性。espP和epeA在几种LEE阴性的EHEC临床分离株中均被检测到,因此可能在这一亚群EHEC的发病机制中起作用。