Abstract
BackgroundAnalysis of the Escherichia coli collection of reference strains (ECOR) for the presence of the gene locus clyA, which encodes the pore-forming protein ClyA (cytolysin A), revealed that a non-functional clyA locus is common among certain extraintestinal pathogenic E. coli (ExPEC). In fact, all 15 ECOR group B2 strains and several additionally examined extraintestinal pathogenic (uropathogenic (UPEC) and neonatal meningitis (NBM)) E. coli strains contained various ΔclyA alleles.ResultsThere are at least four different variants of ΔclyA, suggesting that such deletions in clyA have arisen at more than one occasion. On the basis of this occurrence of the truncated clyA genes, we considered that there may be a patho-adaptive selection for deletions in clyA in extraintestinal pathogenic E. coli. In E. coli K-12 the clyA gene has been viewed as “cryptic” since it is tightly silenced by the nucleoid structuring protein H-NS. We constructed a restored clyA+ locus in derivatives of the UPEC strain 536 for further investigation of this hypothesis and, in particular, how the gene would be expressed. Our results show that the level of clyA+ expression is highly increased in the UPEC derivatives in comparison with the non-pathogenic E. coli K-12. Transcription of the clyA+ gene was induced to even higher levels when the SfaX regulatory protein was overproduced. The derivative with a restored clyA+ locus displayed a somewhat slower growth than the parental UPEC strain 536 when a sub-inhibitory concentration of the antimicrobial peptide Polymyxin B was added to the growth medium.ConclusionsTaken together, our findings show that the clyA+ locus is expressed at an elevated level in the UPEC strain and we conclude that this is at least in part due to the effect of the SfaX/PapX transcriptional regulators.Electronic supplementary materialThe online version of this article (doi:10.1186/s12866-014-0216-4) contains supplementary material, which is available to authorized users.
Highlights
Analysis of the Escherichia coli collection of reference strains (ECOR) for the presence of the gene locus clyA, which encodes the pore-forming protein ClyA, revealed that a non-functional clyA locus is common among certain extraintestinal pathogenic E. coli (ExPEC)
A majority of Escherichia coli strains are benign residents of the intestinal tract of mammals, a minority of E. coli isolates are pathogenic and cause a variety of diseases ranging from diarrhea to urinary tract infections and to meningitis
One of the most characterized hemolysins is HlyA or α-hemolysin which is produced by uropathogenic E. coli (UPEC), several other types of hemolysins have been described for E. coli from different patho-groups [1]
Summary
Analysis of the Escherichia coli collection of reference strains (ECOR) for the presence of the gene locus clyA, which encodes the pore-forming protein ClyA (cytolysin A), revealed that a non-functional clyA locus is common among certain extraintestinal pathogenic E. coli (ExPEC). All 15 ECOR group B2 strains and several examined extraintestinal pathogenic (uropathogenic (UPEC) and neonatal meningitis (NBM)) E. coli strains contained various ΔclyA alleles. Considering the strict regulation of clyA in non-pathogenic E. coli laboratory strains it is of interest to understand how this gene locus functions in other E. coli isolates. The role of ClyA in Salmonella virulence was analyzed using the S. enterica serovars Brandenburg, Indiana, Panama, and Schwarzengrund; 21 different serotypes of the strains were examined and the presence of ClyA was suggested to be associated with virulence in these S. enterica serovars [11]
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