| Literature DB >> 34253575 |
Eirini Giannoudaki1,2, Anna M Stefanska1,2, Hazel Lawler1,2, Gemma Leon1,2, Yasmina E Hernandez Santana1,2, Najma Hassan1,2, Shane E Russell1,2, Rachel Horan1,2, Cheryl Sweeney3, Roger S Preston4, Alberto Mantovani5,6,7, Cecilia Garlanda5,6, Padraic G Fallon1,2, Patrick T Walsh8,2.
Abstract
SIGIRR has been described as a negative regulator of several IL-1R/TLR family members and has been implicated in several inflammatory disease conditions. However, it is unknown whether it can suppress IL-36 family cytokines, which are members of the broader IL-1 superfamily that have emerged as critical orchestrators of psoriatic inflammation in both humans and mice. In this study, we demonstrate that SIGIRR is downregulated in psoriatic lesions in humans and mice, and this correlates with increased expression of IL-36 family cytokines. Using Sigirr -/- mice, we identify, for the first time (to our knowledge), SIGIRR as a negative regulator of IL-36 responses in the skin. Mechanistically, we identify dendritic cells and keratinocytes as the primary cell subsets in which IL-36 proinflammatory responses are regulated by SIGIRR. Both cell types displayed elevated IL-36 responsiveness in absence of SIGIRR activity, characterized by enhanced expression of neutrophil chemoattractants, leading to increased neutrophil infiltration to the inflamed skin. Blockade of IL-36R signaling ameliorated exacerbated psoriasiform inflammation in Sigirr-/- mice and inhibited neutrophil infiltration. These data identify SIGIRR activity as an important regulatory node in suppressing IL-36-dependent psoriatic inflammation in humans and mice.Entities:
Year: 2021 PMID: 34253575 DOI: 10.4049/jimmunol.2100237
Source DB: PubMed Journal: J Immunol ISSN: 0022-1767 Impact factor: 5.422