AI Article Synopsis

  • A bacteriophage called phi MR11 was selected to target and treat Staphylococcus aureus infections, focusing on its gene 61 which produces a protein (gp61) with lytic properties.
  • Both the amidase and lysozyme domains of gp61 were shown to effectively lyse S. aureus, making it significant for phage therapy.
  • This research is notable as it identifies gp61 as the first tail-associated virion protein that functions as a lysin in a Staphylococcus aureus phage, which could enhance our understanding and application of phage therapy.

Article Abstract

A tailed bacteriophage, phi MR11 (siphovirus), was selected as a candidate therapeutic phage against Staphylococcus aureus infections. Gene 61, one of the 67 ORFs identified, is located in the morphogenic module. The gene product (gp61) has lytic domains homologous to CHAP (corresponding to an amidase function) at its N-terminus and lysozyme subfamily 2 (LYZ2) at its C-terminus. Each domain of gp61 was purified as a recombinant protein. Both the amidase [amino acids (aa) 1-150] and the lysozyme (aa 401-624) domains but not the linker domain (aa 151-400) caused efficient lysis of S. aureus. Immunoelectron microscopy localized gp61 to the tail tip of the phi MR11 phage. These data strongly suggest that gp61 is a tail-associated lytic factor involved in local cell-wall degradation, allowing the subsequent injection of phi MR11 DNA into the host cytoplasm. Staphylococcus aureus lysogenized with phi MR11 was also lysed by both proteins. Staphylococcus aureus strains on which phi MR11 phage can only produce spots but not plaques were also lysed by each protein, indicating that gp61 may be involved in 'lysis from without'. This is the first report of the presence of a tail-associated virion protein that acts as a lysin, in an S. aureus phage.

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Source
http://dx.doi.org/10.1111/j.1574-6968.2008.01152.xDOI Listing

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