Efficacy of Chemokine Receptor Inhibition in Treating IL-36α-Induced Psoriasiform Inflammation.
James J CampbellKaren EbsworthLinda S ErtlJeffrey P McMahonYu WangSimon YauVenkat R MaliVicky ChhinaAlice KumamotoShirley LiuTon DangDale NewlandIsrael F CharoPenglie ZhangThomas J SchallRajinder SinghPublished in: Journal of immunology (Baltimore, Md. : 1950) (2019)
Several types of psoriasiform dermatitis are associated with increased IL-36 cytokine activity in the skin. A rare, but severe, psoriasis-like disorder, generalized pustular psoriasis (GPP), is linked to loss-of-function mutations in the gene encoding IL-36RA, an important negative regulator of IL-36 signaling. To understand the effects of IL-36 dysregulation in a mouse model, we studied skin inflammation induced by intradermal injections of preactivated IL-36α. We found the immune cells infiltrating IL-36α-injected mouse skin to be of dramatically different composition than those infiltrating imiquimod-treated skin. The IL-36α-induced leukocyte population comprised nearly equal numbers of CD4+ αβ T cells, neutrophils, and inflammatory dendritic cells, whereas the imiquimod-induced population comprised γδ T cells and neutrophils. Ligands for chemokine receptors CCR6 and CXCR2 are increased in both GPP and IL-36α-treated skin, which led us to test an optimized small-molecule antagonist (CCX624) targeting CCR6 and CXCR2 in the IL-36α model. CCX624 significantly reduced the T cell, neutrophil, and inflammatory dendritic cell infiltrates and was more effective than saturating levels of an anti-IL-17RA mAb at reducing inflammatory symptoms. These findings put CCR6 and CXCR2 forward as novel targets for a mechanistically distinct therapeutic approach for inflammatory skin diseases involving dysregulated IL-36 signaling, such as GPP.
Keyphrases
- dendritic cells
- oxidative stress
- small molecule
- regulatory t cells
- soft tissue
- mouse model
- rheumatoid arthritis
- wound healing
- gene expression
- diabetic rats
- transcription factor
- genome wide
- physical activity
- systemic lupus erythematosus
- early onset
- endothelial cells
- stress induced
- binding protein
- monoclonal antibody
- protein protein