4.8 Article

Structure and mechanism of Staphylococcus aureus TarM, the wall teichoic acid α-glycosyltransferase

Publisher

NATL ACAD SCIENCES
DOI: 10.1073/pnas.1418084112

Keywords

glycosyltransferase; wall teichoic acid; cell wall; crystal structure; bacterial pathogenicity

Funding

  1. Centro de Biologia Estructural del Mercosur/CCP4 workshop (Montevideo, Uruguay)
  2. Canadian Institutes of Health Research
  3. Michael Smith Foundation for Health Research Fellowship program
  4. Howard Hughes Medical Institute International Scholar program
  5. British Columbia Knowledge Development Fund
  6. Cystic Fibrosis Canada
  7. FWF Austrian Science Fund
  8. Deutsche Forschungsgemeinschaft

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Unique to Gram-positive bacteria, wall teichoic acids are anionic glycopolymers cross-stitched to a thick layer of peptidoglycan. The polyol phosphate subunits of these glycopolymers are decorated with GlcNAc sugars that are involved in phage binding, genetic exchange, host antibody response, resistance, and virulence. The search for the enzymes responsible for GlcNAcylation in Staphylococcus aureus has recently identified TarM and TarS with respective alpha-and beta-(1-4) glycosyltransferase activities. The stereochemistry of the GlcNAc attachment is important in balancing biological processes, such that the interplay of TarM and TarS is likely important for bacterial pathogenicity and survival. Here we present the crystal structure of TarM in an unusual ternary-like complex consisting of a polymeric acceptor substrate analog, UDP from a hydrolyzed donor, and an alpha-glyceryl-GlcNAc product formed in situ. These structures support an internal nucleophilic substitution-like mechanism, lend new mechanistic insight into the glycosylation of glycopolymers, and reveal a trimerization domain with a likely role in acceptor substrate scaffolding.

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