This study aimed to explore the potential implication in initial

This study aimed to explore the potential implication in initial adherence or host specificity of the specific sequences. In the SSH library, we obtained 115 unique fragments that were specific to the bovine strain. These fragments include sequences with homology to genes or pathogenicity islands (PAIs) present only in other specific E. coli pathotypes

(e.g. VTEC) or other species (e.g. Klebsiella, Nitromonas), which are not known to be present in EHEC strains of serogroup O26. This heterogeneity supports the hypothesis of a horizontal acquisition of genomic regions from other pathogenic bacteria (Brzuszkiewicz et al., 2009; Juhas et al., 2009; Kelly et al., 2009). Moreover, it reflects the genomic plasticity of EHEC and/or E. coli strains. This finding supports the hypothesis Alpelisib concentration of Mokady et al. (2005), suggesting that this variation in the genome contents of E. coli could indicate that its evolutionary strategy tends to create a mixed assortment

of virulence factors coming from various pathogenic strains. This combination leads to a unique set of such factors, which helps the bacteria to better survive. The PAI ICL3 locus, first described by Shen et al. (2004) in the VTEC O113:H21 E. coli CL3, was found in 11.3% of the tested EHEC and EPEC strains of serogroup O26. These results are surprising when compared to those obtained by Girardeau et al. Forskolin solubility dmso (2009), suggesting that PAI ICL3 is unique to LEE-negative VTEC strains and that this locus thus provides a new marker for such strains. We have reported here that the locus could also be present in eae-positive strains belonging to a major serogroup involved in human diseases. Girardeau et al. (2009) have suggested that PAI ICL3 used to be present in most E. coli pathotypes but that many of these pathotypes have undergone extensive deletions [probably

via homologous recombination between insertion sequences (IS) elements, which removed almost the entire locus]. We can assume that our positive strains were not deleted for this locus. Another possible explanation is that these strains have recently Pyruvate dehydrogenase lipoamide kinase isozyme 1 acquired the PAI ICL3 locus via horizontal transfer, which hypothesis is supported by the fact that the PAI ICL3-positive strains are not closely related. Concerning host specificity, only one sequence appears to be statistically specific to human strains in comparison with bovine strains. Nevertheless, this sequence is only present in a few strains (7% of bovine strains and 33% of human strains) and therefore could not represent a host-specific marker. Moreover, three sequences were statistically associated with the pathotype (EHEC or EPEC), but these sequences were not present in more than half of the EPEC strains.

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