AI Article Synopsis

  • Pathogen shows versatility, causing various diseases and adapting to different hosts through genome modification and acquisition of mobile genetic elements.
  • Discovery of a novel variant of staphylococcal complement inhibitor (SCIN) in equine strains suggests it helps evade the host's immune system by blocking complement activation.
  • The new equine SCIN variant (eqSCIN) not only targets horses but also works across multiple species, indicating its role in the pathogen's adaptability and transmission between different hosts.

Article Abstract

is a versatile pathogen capable of causing a broad range of diseases in many different hosts. can adapt to its host through modification of its genome ( by acquisition and exchange of mobile genetic elements that encode host-specific virulence factors). Recently, the prophage φSaeq1 was discovered in strains from six different clonal lineages almost exclusively isolated from equids. Within this phage, we discovered a novel variant of staphylococcal complement inhibitor (SCIN), a secreted protein that interferes with activation of the human complement system, an important line of host defense. We here show that this equine variant of SCIN, eqSCIN, is a potent blocker of equine complement system activation and subsequent phagocytosis of bacteria by phagocytes. Mechanistic studies indicate that eqSCIN blocks equine complement activation by specific inhibition of the C3 convertase enzyme (C3bBb). Whereas SCIN-A from human isolates exclusively inhibits human complement, eqSCIN represents the first animal-adapted SCIN variant that functions in a broader range of hosts (horses, humans, and pigs). Binding analyses suggest that the human-specific activity of SCIN-A is related to amino acid differences on both sides of the SCIN-C3b interface. These data suggest that modification of this phage-encoded complement inhibitor plays a role in the host adaptation of and are important to understand how this pathogen transfers between different hosts.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5868266PMC
http://dx.doi.org/10.1074/jbc.RA117.000599DOI Listing

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