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Predictors of outcome in ulcerative colitis

Research output: Contribution to Journal/MagazineJournal articlepeer-review

  • Matti Waterman
  • Jo Knight
  • Amreen Dinani
  • Wei Xu
  • Joanne M. Stempak
  • Kenneth Croitoru
  • Geoffrey C. Nguyen
  • Zane Cohen
  • Robin S. McLeod
  • Gordon R. Greenberg
  • A. Hillary Steinhart
  • Mark S. Silverberg
<mark>Journal publication date</mark>09/2015
<mark>Journal</mark>Inflammatory Bowel Diseases
Issue number9
Number of pages9
Pages (from-to)2097-2105
Publication StatusPublished
<mark>Original language</mark>English


BACKGROUND: Approximately 80% of patients with ulcerative colitis (UC) have intermittently active disease and up to 20% will require a colectomy, but little data available on predictors of poor disease course. The aim of this study was to identify clinical and genetic markers that can predict prognosis.

METHODS: Medical records of patients with UC with ≥5 years of follow-up and available DNA and serum were retrospectively assessed. Immunochip was used to genotype loci associated with immune mediated inflammatory disorders (IMIDs), inflammatory bowel diseases, and other single nucleotide polypmorphisms previously associated with disease severity. Serum levels of pANCA, ASCA, CBir1, and OmpC were also evaluated. Requirement for colectomy, medication, and hospitalization were used to group patients into 3 prognostic groups.

RESULTS: Six hundred one patients with UC were classified as mild (n = 78), moderate (n = 273), or severe disease (n = 250). Proximal disease location frequencies at diagnosis were 13%, 21%, and 30% for mild, moderate, and severe UC, respectively (P = 0.001). Disease severity was associated with greater proximal extension rates on follow-up (P < 0.0001) and with shorter time to extension (P = 0.03) and to prednisone initiation (P = 0.0004). When comparing severe UC with mild and moderate UC together, diagnosis age >40 and proximal disease location were associated with severe UC (odds ratios = 1.94 and 2.12, respectively). None of the single nucleotide polypmorphisms or serum markers tested was associated with severe UC, proximal disease extension or colectomy.

CONCLUSIONS: Older age and proximal disease location at diagnosis, but not genetic and serum markers, were associated with a more severe course. Further work is required to identify biomarkers that will predict outcomes in UC.