Virulence of enterohemorrhagic Escherichia coli O91:H21 clinical isolates in an orally infected mouse model.

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Infect Immun. 1993 September; 61(9): 3832-3842

Virulence of enterohemorrhagic Escherichia coli O91:H21 clinical isolates in an orally infected mouse model.

S W Lindgren, A R Melton and A D O'Brien

Department of Microbiology, Uniformed Services University of the Health Sciences, Bethesda, Maryland 20814-4799.

ABSTRACT

Escherichia coli K-12 strains producing high levels of Shiga-liketoxin type II (SLT-II) but not SLT-I were previously shown tobe virulent in an orally infected, streptomycin-treated mousemodel. In this investigation, we tested the virulence of severalSLT-II-producing enterohemorrhagic E. coli (EHEC) isolates frompatients with hemorrhagic colitis or hemolytic uremic syndrome.All of the strains tested were able to colonize the mouse intestine.However, only two strains were consistently virulent for mice:O91:H21 strain B2F1 (Strr), which was previously shown to carrytwo copies of slt-II-related toxins, and O91:H21 strain H414-36/89(Strr), which was found in this study to contain three genesfrom the slt-II group. The oral 50% lethal doses of strainsB2F1 (Strr) and H414-36/89 (Strr) when fed to streptomycin-treatedmice were less than 10 bacteria. Histological sections frommoribund mice fed the O91:H21 strains demonstrated extensiverenal tubular necrosis; however, hematological results werenot consistent with a diagnosis of hemolytic uremic syndrome.The central role of SLT in the virulence of the O91:H21 EHECstrains was supported by the finding that streptomycin-treatedmice preinoculated with monoclonal antibody specific for SLT-IIsurvived oral challenge with either B2F1 (Strr) or H414-36/89(Strr). The basis for the variation in virulence among the SLT-II-producingEHEC strains tested was not determined. However, a correlationbetween the capacity of an EHEC strain to grow in small intestinalmucus and lethality in the streptomycin-treated mice was observed.

Infect Immun. 1993 September; 61(9): 3832-3842

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