MIRIKIZUMAB-INDUCED TRANSCRIPTOME CHANGES in ULCERATIVE COLITIS PATIENT BIOPSIES at WEEK 12 ARE MAINTAINED THROUGH WEEK 52

Travis Johnson, Boyd Steere, Pengyue Zhang, Yong Zang, Richard Higgs, Catherine Milch, Walter Reinisch, Julian Panés, Kun Huang, Geert D'Haens, Venkatesh Krishnan

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Abstract

Introduction:Mirikizumab, an anti-IL-23p19 monoclonal antibody, demonstrated efficacy in phase 2 and 3 randomized clinical trials of patients with moderate-To-severe ulcerative colitis (UC). Previous results have shown that 12 weeks of mirikizumab treatment down-regulated transcripts associated with UC disease activity and tumor necrosis factor inhibitor resistance. We assessed Week-52 gene expression from Week-12 responders receiving mirikizumab or placebo.Methods:In the phase 2 AMAC study (NCT02589665), mirikizumab-Treated patients achieving Week-12 clinical response were re-randomized to mirikizumab 200 mg subcutaneous every 4 or 12 weeks through Week 52 (N=31). Week-12 placebo responders continued placebo through Week 52 (N=7). The limma R package clustered transcript changes in colonic mucosa biopsies from baseline to Week 12 into differentially expressed genes (DEGs). Among DEGs, similarly expressed genes (DEGSEGs) maintaining Week-12 expression through Week 52 were identified.Results:Of 89 DEGSEGs, 63 (70.8%) were present only in mirikizumab induction responders, 5 (5.6%) in placebo responders, and 21 (23.6%) in both. Week-12 magnitudes and Week-52 consistency of transcript changes were greater in mirikizumab than in placebo responders (log2FC>1). DEGSEG clusters (from 84 DEGSEGs identified in mirikizumab and mirikizumab/placebo responders) correlated to modified Mayo score (26/84 with Pearson correlation coefficient [PCC]>0.5) and Robarts Histopathology Index (55/84 with PCC>0.5), sustained through Week 52.Discussion:Mirikizumab responders had broader, more sustained transcriptional changes of greater magnitudes at Week 52 versus placebo. Mirikizumab responder DEGSEGs suggest a distinct molecular healing pathway associated with mirikizumab IL-23 inhibition. The cluster's correlation with disease activity illustrates relationships between clinical, endoscopic, and molecular healing in UC.
Original languageEnglish
Article numberCTG-23-0112
JournalClinical and translational gastroenterology
Early online date2023
DOIs
Publication statusE-pub ahead of print - 2023

Keywords

  • Mirikizumab
  • differential gene expression
  • transcriptome
  • ulcerative colitis

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