| Literature DB >> 33910010 |
Yoshihiro Ito1, Takashi Sasaki2, Youxian Li3, Takeshi Tanoue4, Yuki Sugiura5, Ashwin N Skelly6, Wataru Suda7, Yusuke Kawashima8, Nobuyuki Okahashi3, Eiichiro Watanabe3, Hiroto Horikawa9, Aiko Shiohama10, Rina Kurokawa7, Eiryo Kawakami11, Hachiro Iseki3, Hiroshi Kawasaki12, Yoichiro Iwakura13, Atsushi Shiota14, Liansheng Yu15, Junzo Hisatsune15, Haruhiko Koseki16, Motoyuki Sugai15, Makoto Arita3, Osamu Ohara17, Takeshi Matsui18, Makoto Suematsu5, Masahira Hattori7, Koji Atarashi4, Masayuki Amagai19, Kenya Honda20.
Abstract
Host-microbe interactions orchestrate skin homeostasis, the dysregulation of which has been implicated in chronic inflammatory conditions such as atopic dermatitis and psoriasis. Here, we show that Staphylococcus cohnii is a skin commensal capable of beneficially inhibiting skin inflammation. We find that Tmem79-/- mice spontaneously develop interleukin-17 (IL-17)-producing T-cell-driven skin inflammation. Comparative skin microbiome analysis reveals that the disease activity index is negatively associated with S. cohnii. Inoculation with S. cohnii strains isolated from either mouse or human skin microbiota significantly prevents and ameliorates dermatitis in Tmem79-/- mice without affecting pathobiont burden. S. cohnii colonization is accompanied by activation of host glucocorticoid-related pathways and induction of anti-inflammatory genes in the skin and is therefore effective at suppressing inflammation in diverse pathobiont-independent dermatitis models, including chemically induced, type 17, and type 2 immune-driven models. As such, S. cohnii strains have great potential as effective live biotherapeutics for skin inflammation.Entities:
Keywords: atopic dermatitis; biotherapy; psoriasis; skin microbiome
Mesh:
Year: 2021 PMID: 33910010 DOI: 10.1016/j.celrep.2021.109052
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423