4318720 Putative transketolase NC_008563 APECO1_2640   4318750

.4318720 Putative transketolase NC_008563 APECO1_2640   4318750..4319595 putative transcriptional regulatory NC_008563 APECO1_2639   4319796..4320701 putative transcriptional regulatory NC_008563 GW786034 nmr APECO1_2638   4320779..4322002 putative permease NC_008563 APECO1_2637   4322028..4322417 hypothetical protein NC_008563 APECO1_2636   4322434..4323390 catalyzes the reversible synthesis

of carbamate NC_008563     and ATP from carbamoyl phosphate and ADP   APECO1_2635 yahG 4323383..4324858 hypothetical protein NC_008563 APECO1_2634 yahF 4324804..4326363 hypothetical protein NC_008563 APECO1_2633 yahE 4326458..4327318 hypothetical protein NC_008563 APECO1_2632   4327324..4327992 putative isochorismatase hydrolase NC_008563

PAIs have been described in several well-known ExPEC strains, including E. coli strains 536, CFT073, J96, UTI189, RS218 and APEC O1. Indeed, CCI-779 manufacturer comparative analysis of the APEC O1 genome and other ExPEC genomes revealed that APEC and human ExPEC share more than 28 pathogenicity (genomic) islands [9, 25, 26, 31]. Among them, the genomic island encoding tkt1 was notable in that it was found among all sequenced ExPEC genomes. The multiplex PCR results of this study further demonstrated that a complete copy of this genomic island is significantly selleck chemicals llc associated with both avian and human ExPEC strains of phylogenetic group B2. These observations suggest that the tkt1 genomic island may contribute to the virulence/fitness of both avian and human ExPEC. Though Tkt1 shares 68% amino acid identity with TktA of a V. cholerae strain [13], it does not show any homology at the nucleotide level with tktA of E. coli MG1655. In E. coli K12, tktA encodes the

transketolase A, which is responsible for the major enzymatic activity of transketolase in E. coli. Transketolase is a link between glycolysis and the pentose phosphate pathway and is involved in the catabolism of pentose sugars, formation Paclitaxel concentration of D-ribose 5-phosphate, and provision of D-erythrose 4-phosphate which is a precursor of aromatic amino acids, aromatic vitamins and pyridoxine [32]. A previous study showed that the E. coli K12 mutant BJ502 that carries a mutation in tktA was unable to use L-arabinose or D-Xylose as the sole carbon source and required aromatic acids for growth on a minimal medium. The functional analysis in this study demonstrated that over-expression of Tkt1 in E. coli K12 mutant strain BJ502 could not recover its growth in M9 medium with L-arabinose as the sole carbon source; while over-expression of TktA could. These results suggest that tkt1 could not complement the tktA mutation in E. coli K12 and Tkt1 confers very little transketolase activity, if any. Most studies of bacterial pathogenesis have focused on classical virulence factors such as toxins, adhesins, iron uptake systems and factors that confer resistance to innate and adaptive immune mechanisms.

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