mSphere (Jul 2024)

Genomic analysis and identification of a novel superantigen, SargEY, in Staphylococcus argenteus isolated from atopic dermatitis lesions

  • Fatkhanuddin Aziz,
  • Junzo Hisatsune,
  • Hisaya K. Ono,
  • Junko Kajimura,
  • Liansheng Yu,
  • Kanako Masuda,
  • Hiroki Kitagawa,
  • Yusuke Sato'o,
  • Koji Yahara,
  • Mika Yamaoka,
  • Akio Nakane,
  • Hiroshi Kawasaki,
  • Shoko Obata,
  • Ayano Fukushima-Nomura,
  • Yoshihiro Ito,
  • Meiji Soe Aung,
  • Masayuki Amagai,
  • Siti Isrina Oktavia Salasia,
  • Hiroki Ohge,
  • Yoichiro Kusunoki,
  • Motoyuki Sugai

DOI
https://doi.org/10.1128/msphere.00505-24
Journal volume & issue
Vol. 9, no. 7

Abstract

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ABSTRACT During surveillance of Staphylococcus aureus in lesions from patients with atopic dermatitis (AD), we isolated Staphylococcus argenteus, a species registered in 2011 as a new member of the genus Staphylococcus and previously considered a lineage of S. aureus. Genome sequence comparisons between S. argenteus isolates and representative S. aureus clinical isolates from various origins revealed that the S. argenteus genome from AD patients closely resembles that of S. aureus causing skin infections. We previously reported that 17%–22% of S. aureus isolated from skin infections produce staphylococcal enterotoxin Y (SEY), which predominantly induces T-cell proliferation via the T-cell receptor (TCR) Vα pathway. Complete genome sequencing of S. argenteus isolates revealed a gene encoding a protein similar to superantigen SEY, designated as SargEY, on its chromosome. Population structure analysis of S. argenteus revealed that these isolates are ST2250 lineage, which was the only lineage positive for the SEY-like gene among S. argenteus. Recombinant SargEY demonstrated immunological cross-reactivity with anti-SEY serum. SargEY could induce proliferation of human CD4+ and CD8+ T cells, as well as production of TNF-α and IFN-γ. SargEY showed emetic activity in a marmoset monkey model. SargEY and SET (a phylogenetically close but uncharacterized SE) revealed their dependency on TCR Vα in inducing human T-cell proliferation. Additionally, TCR sequencing revealed other previously undescribed Vα repertoires induced by SEH. SargEY and SEY may play roles in exacerbating the respective toxin-producing strains in AD.IMPORTANCEStaphylococcus aureus is frequently isolated from active lesions of atopic dermatitis (AD) patients. We reported that 17%–22% of S. aureus isolated from AD patients produced a novel superantigen staphylococcal enterotoxin Y (SEY). Unlike many S. aureus superantigens that activate T cells via T-cell receptor (TCR) Vß, SEY activates T cells via TCR Vα and stimulates cytokine secretion. Staphylococcus argenteus was isolated from AD patients during the surveillance for S. aureus. Phylogenetic comparison of the genome indicated that the isolate was very similar to S. aureus causing skin infections. The isolate encoded a SEY-like protein, designated SargEY, which, like SEY, activated T cells via the TCR Vα. ST2250 is the only lineage positive for SargEY gene. ST2250 S. argenteus harboring a superantigen SargEY gene may be a novel staphylococcal clone that infects human skin and is involved in the exacerbation of AD.

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