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Identification and biosynthesis of thymidine hypermodifications in the genomic DNA of widespread bacterial viruses

  • Yan Jiun Lee
  • , Nan Dai
  • , Shannon E. Walsh
  • , Stephanie Müller
  • , Morgan E. Fraser
  • , Kathryn M. Kauffman
  • , Chudi Guan
  • , Ivan R. Corrêa
  • , Peter R. Weigele
  • New England Biolabs

Research output: Contribution to journalArticlepeer-review

64 Scopus citations

Abstract

Certain viruses of bacteria (bacteriophages) enzymatically hypermodify their DNA to protect their genetic material from host restriction endonuclease-mediated cleavage. Historically, it has been known that virion DNAs from the Delftia phage ΦW-14 and the Bacillus phage SP10 contain the hypermodified pyrimidines α-putrescinylthymidine and α-glutamylthymidine, respectively. These bases derive from the modification of 5-hydroxymethyl-2′-deoxyuridine (5-hmdU) in newly replicated phage DNA via a pyrophosphorylated intermediate. Like ΦW-14 and SP10, the Pseudomonas phage M6 and the Salmonella phage ViI encode kinase homologs predicted to phosphorylate 5-hmdU DNA but have uncharacterized nucleotide content [Iyer et al. (2013) Nucleic Acids Res 41:7635–7655]. We report here the discovery and characterization of two bases, 5-(2-aminoethoxy)methyluridine (5-NeOmdU) and 5-(2-aminoethyl)uridine (5-NedU), in the virion DNA of ViI and M6 phages, respectively. Furthermore, we show that recombinant expression of five gene products encoded by phage ViI is sufficient to reconstitute the formation of 5-NeOmdU in vitro. These findings point to an unexplored diversity of DNA modifications and the underlying biochemistry of their formation.

Original languageEnglish
Pages (from-to)E3116-E3125
JournalProceedings of the National Academy of Sciences of the United States of America
Volume115
Issue number14
DOIs
StatePublished - Apr 3 2018

Keywords

  • Bacteriophage
  • DNA modification
  • Hypermodification
  • Pyrimidine

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