The four clusters in the tree represented an almost equal amount of strains causing severe GSK621 clinical trial or mild symptoms of S. Typhimurium
infections. The probes on the array were designed primarily on basis of the S. Typhimurium LT2 sequence, but also some additional known genes from other serotypes such as S. Enteritidis and S. Typhi. The presence or absence of additional S. Typhimurium genes, which are not present in the LT2 sequence, could not be assessed in this study. It is possible that the presence or absence of such genes, not present in LT2, are responsible for the observed differences in the patient symptoms. Although this is not likely, as recent publications of sequenced S. Typhimurium strains showed few gene differences to the LT2 sequenced strain [28, 29]. Conclusion We investigated a collection of Salmonella strains for the presence of a wide range of known virulence genes, and detected no significant difference in the presence of these genes. The investigated strains were carefully selected, based on epidemiological
data, to represent strains causing severe symptoms of disease and strains causing mild symptoms of disease. Although the investigated strains had different genomic click here contents, this study found no evidence of a correlation between the genomic contents of the S. Typhimurium strains and the symptoms they caused in human cases of salmonellosis.
Based on the results of this study, an idea which immediately suggests itself is that the factors and defence mechanisms of the host immune system may play a fundamental role in the different outcomes of infection. Methods Patient interviews Data for the present study was obtained from PAK5 a prospective cohort study carried out in Denmark from September 2001 to December 2002 [30]. Cases were patients with a culture-confirmed S. Typhimurium infection, identified by the examination of samples submitted to Statens Serum Institut (SSI) from hospitals and general practitioners. Patients were invited to participate by their own physicians or the relevant hospital department. Individuals who agreed to participate were mailed a questionnaire and asked to complete the questionnaire immediately. Data was collected by a computer-assisted telephone interviewing system (CATI) whilst the subjects were looking at their questionnaire. This method facilitated data collection and allowed standardized probing about relevant exposures and outcomes. Data collected included information on clinical symptoms, treatment, medications (including antimicrobials) from one month before infection to one month after, underlying illnesses, foreign travel during the two weeks prior to OTX015 price inclusion and basic socioeconomic variables i.e. education, occupation and household income.