Discordant effects ofex-vivoJAK inhibition on inflammatory responses in colonic compared to ileal mucosa

Abstract

AbstractBackground & aimsJanus kinase (JAK) inhibitors modulating JAK-STAT (signal transducers and activators of transcription) signaling pathway, are used for the treatment of patients with inflammatory bowel diseases (IBD). We aimed to identify the molecular effects of JAK inhibition in the human intestinal mucosa, considering the IBD location and phenotype.MethodsColonic and ileal explants from patients with ulcerative colitis (UC), Crohn’s disease (CD), or non-IBD controls (NC) were treatedex-vivowith the JAK inhibitor, tofacitinib. Phosphorylated STAT (p-STAT) levels were assessed by Western blot and Immunofluorescence. Inflammatory genes expression was assessed with Nanostring nCounter system. Human intestinal organoids were used to assess JAK inhibitors’ effects on p-STATs and iNOS expression.ResultsExplants were collected from 68 patients (NC=28; UC=20; CD=20). JAK inhibition reduced p-STAT1/3/5 expression in all explants. While p-STAT inhibition rates varied among patients (10%-88%), higher inhibition rates were observed in colonic compared to ileal explants. Significant alterations in 120 of 255 inflammatory genes were observed in colonic explants, while only 30 were observed in ileal NC explants. In colonic explants from UC, significant alterations were observed in 5 genes, includingSTAT1andNOS2. Various JAK inhibitors reduced IFN-γ-induced increase in p-STAT1 and iNOS expression in organoids.ConclusionsA site-specific anti-inflammatory effect of JAK inhibition by tofacitinib was noticed, whereby the colon was more robustly affected than the ileum.Ex-vivoresponse to tofacitinib is individual. JAK inhibition may attenuate inflammation by decreasing iNOS expression.Ex-vivomucosal platforms may be a valuable resource for studying drug impact and evaluating personalized treatment effects.