4.5 Article

Characterization of a ViI-like Phage Specific to Escherichia coli O157:H7

Journal

VIROLOGY JOURNAL
Volume 8, Issue -, Pages -

Publisher

BMC
DOI: 10.1186/1743-422X-8-430

Keywords

E. coli O157:H7; hydroxymethyluracil; phage evolution; phage ecology; genome; proteome; bioinformatics; Vi antigen; O157 antigen; tail spike; T4 core genes

Categories

Funding

  1. PhageBiotics Foundation
  2. USDA/ARS
  3. National Cattlemen's Beef Association
  4. Evergreen Foundation
  5. NIH [2-R15GM063637-02, 2R15GM63637-3A1]
  6. Natural Sciences and Engineering Research Council of Canada

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Phage vB_EcoM_CBA120 (CBA120), isolated against Escherichia coli O157:H7 from a cattle feedlot, is morphologically very similar to the classic phage ViI of Salmonella enterica serovar Typhi. Until recently, little was known genetically or physiologically about the ViI-like phages, and none targeting E. coli have been described in the literature. The genome of CBA120 has been fully sequenced and is highly similar to those of both ViI and the Shigella phage AG3. The core set of structural and replication-related proteins of CBA120 are homologous to those from T-even phages, but generally are more closely related to those from T4-like phages of Vibrio, Aeromonas and cyanobacteria than those of the Enterobacteriaceae. The baseplate and method of adhesion to the host are, however, very different from those of either T4 or the cyanophages. None of the outer baseplate proteins are conserved. Instead of T4's long and short tail fibers, CBA120, like ViI, encodes tail spikes related to those normally seen on podoviruses. The 158 kb genome, like that of T4, is circularly permuted and terminally redundant, but unlike T4 CBA120 does not substitute hmdCyt for cytosine in its DNA. However, in contrast to other coliphages, CBA120 and related coliphages we have isolated cannot incorporate H-3-thymidine (H-3-dThd) into their DNA. Protein sequence comparisons cluster the putative thymidylate synthase of CBA120, ViI and AG3 much more closely with those of Delftia phage phi W-14, Bacillus subtilis phage SPO1, and Pseudomonas phage YuA, all known to produce and incorporate hydroxymethyluracil (hmdUra).

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