Esophagus to Small Intestine

Clin Gastroenterol Hepatol. 2022;20(9):2059–73.e7

Magro F, Magalhães D, Patita M, Arroja B, Lago P, Rosa I, Tavares de Sousa H, Ministro P, Mocanu I, Vieira A, Castela J, Moleiro J, Roseira J, Cancela E, Sousa P, Portela F, Correia L, Santiago M, Dias S, Alves C, Afonso J, Danese S, Peyrin-Biroulet L, Dias CC; Portuguese Group of Studies in IBD (GEDII)

Subclinical persistent inflammation as risk factor for Crohn’s disease progression: Findings from a prospective real-world study of 2 years

Background and aims: Subclinical intestinal inflammation is common in Crohn’s disease. The authors aimed to explore its impact in the disease progression of infliximab (IFX)-treated patients and the usefulness of fecal calprotectin (FC) and C-reactive protein (CRP) as surrogate minimally invasive biomarkers.
Methods: The registry-based, prospective, observational, multicenter DIRECT study (study to investigate the correlation of fecal calprotectin with serum Drug levels and development of an antI-dRug antibodiEs among adult patients with inflammatory bowel disease reCeiving anti-TNF-alpha treatment or vedoluzimab treatment) followed IFX-treated Crohn’s disease patients for 2 years in a tertiary care setting. Persistent inflammation definition was based on FC (> 150 μg/g, > 250 μg/g, or > 350 μg/g) or serum CRP (> 3 μg/ml) concentrations over 2 consecutive or at least 3 visits. Patients were categorized according to a composite outcome reflecting disease progression that incorporated surgery; hospitalizations; new fistulae, abscess, or stricture; and treatment escalation.
Results: Of 322 DIRECT study patients, 180 asymptomatic, IFX treated on maintenance regimen were included in the analysis. Patients developing the composite end point (n = 96) presented higher median levels of FC (205 [interquartile range {IQR}, 98–515] μg/g; p = 0.045) but not of CRP (2.50 [IQR, 0.80–6.00] μg/ml; p = 0.895). Biomarker-defined persistent subclinical inflammation prevalence ranged from 24% to 81%. Considering FC > 250 μg/g in 2 consecutive visits, prevalence was 50%, odds of achieving the end point were increased 3-fold (odds ratio = 2.996, 95% confidence interval: 1.557–5.776), and time-to-outcome occurrence was significantly lower among subjects with persistent inflammation (median time, 11 months). Both clinical-related and treatment-related components were significantly associated with persistent inflammation. Definitions based on CRP > 3 μg/ml, FC > 150 μg/g, FC > 350 μg/g, double biomarkers (FC > 250 μg/g and/or CRP > 3 μg/ml), or more visits did not improve predictive ability.

Conclusions: Persistent inflammation, defined simply and readily by fecal calprotectin > 250 μg/g over 2 consecutive visits, was associated with a significantly higher risk and shorter time to occurrence of a composite outcome reflecting disease progression in asymptomatic infliximab-treated Crohn’s disease patients.

DOI: 10.1016/j.cgh.2021.12.004