In Haemophilus ducreyi, inactivation of the gmhA gene has been shown to result in a truncated LOS and to reduce the BAY 57-1293 supplier ability of the organism to produce skin lesions in rabbits [59]. In addition, the ability of Salmonella this website enterica to kill Caenorhabditis elegans was impaired by insertional inactivation of the gmhA gene [60]. Mutation of another C. jejuni gene involved in synthesis of the LOS inner core, waaC, markedly impaired the ability of C. jejuni 81–176 to invade the intestinal cell line INT407 in vitro [61]. Strain NW was also missing a number of C. jejuni 11168 genes in complex loci involved in capsule synthesis and O-linked glycosylation of the flagellin protein. Extensive variation
in these loci has been reported in other microarray comparisons of C. jejuni strains [12]. Both flagella and capsule have C59 wnt price been reported to affect virulence in C. jejuni [18, 24]. The reason for the inability of strain D2586 to increase in virulence is not known, but a similar approach could be taken to examine gene content in comparison to strain 11168. The degree and complexity of the phenotypic changes we observed – increased fecal population
sizes, increased colonization of the jejunum, decreased time to develop severe disease, shift from watery to bloody diarrhea – suggest that the three evolving strains underwent genetic change at multiple loci, including loci that influence growth and loci that influence interaction with and damage to host tissues. We have no information on any specific genetic changes that led to these phenotypic changes at the present time; further studies on these strains will utilize gene expression microarrays to focus on the hypothesis that the changes in pathogenicity are tuclazepam due to changes in gene expression levels or patterns; experimental infection of C57BL/6 IL-10-/- mice with C. jejuni 11168 derivatives containing targeted gene knockouts will be used to determine whether corresponding genes contribute to virulence in C. jejuni 11168. Outcome of C. jejuni infection and host
immune response were influenced by diet Results from two of three trials (the previous experiment with mice kept on an ~12% fat diet and an ~6% fat diet throughout the experiment and the full, balanced design comparison (experiment 5, diet comparison) of the effect of diet on the outcome of C. jejuni infection) did not indicate that there was an effect of diet on survival, gross pathology, or histopathology in mice infected with unpassaged C. jejuni 11168. On the other hand, results from the diet comparison conducted in the final phase of experiment 2 (serial passage experiment) did indicate such an effect. In addition, there was a significant effect of diet on plasma IgA levels in the full, balanced design experiment (experiment 5, diet comparison).