Epithelial SLPI expression in severe inflammatory bowel disease relates to high IL-17 and neutrophil programming
Sandrine Nugteren, Beatriz Calado, Ytje Simons-Oosterhuis, Daniëlle H. Hulleman-van Haaften, Willem K. Smits, Renz C.W. Klomberg, Bastiaan Tuk, Mohammed Charrout, Dicky J. Lindenbergh-Kortleve, Michail Doukas, Mathijs A. Sanders, Gregory van Beek, Johanna C. Escher, Lissy de Ridder, Maria Fernanda Pascutti, Janneke N. Samsom
Sandrine Nugteren, Beatriz Calado, Ytje Simons-Oosterhuis, Daniëlle H. Hulleman-van Haaften, Willem K. Smits, Renz C.W. Klomberg, Bastiaan Tuk, Mohammed Charrout, Dicky J. Lindenbergh-Kortleve, Michail Doukas, Mathijs A. Sanders, Gregory van Beek, Johanna C. Escher, Lissy de Ridder, Maria Fernanda Pascutti, Janneke N. Samsom
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Research Article Gastroenterology Immunology

Epithelial SLPI expression in severe inflammatory bowel disease relates to high IL-17 and neutrophil programming

Abstract

Heterogeneity in disease severity and treatment response in inflammatory bowel disease (IBD) likely evolves from individual differences in host-microbiota-immune interactions. Histological evaluation of intestinal biopsies is central to diagnosis, but histological parameters that define underlying immune mechanisms are limited. We investigated histological features that distinguish individual patient immune profiles in therapy-naive pediatric IBD patients (age 6–18 years) using biopsy immunohistochemistry and transcriptomics and plasma proteomics across two cohorts. High colonic epithelial expression of secretory leukocyte protease inhibitor (SLPI), a microbiota-induced regulator of epithelial function, occurred in IBD patients with high clinical disease activity and more severe endoscopic and microscopic disease activity. SLPI expression was related to increased neutrophil infiltration, transcriptomic signatures of activation, and genes known to associate with therapeutic resistance. High SLPI colocalized with high densities of IL-17–secreting cells and was associated with high plasma concentrations of Th17-related immune proteins. Additionally, patients with high intestinal SLPI had an intrinsically different immunotype, in which circulating neutrophils exhibited altered transcription of genes involved in neutrophil granule formation, phagocytosis, oxidative phosphorylation, and interferon signaling. Thus, high colonic SLPI expression at diagnosis associates with severe IBD, increased IL-17A–neutrophil pathway responses, and altered transcriptomic wiring of circulating neutrophils.

Authors

Sandrine Nugteren, Beatriz Calado, Ytje Simons-Oosterhuis, Daniëlle H. Hulleman-van Haaften, Willem K. Smits, Renz C.W. Klomberg, Bastiaan Tuk, Mohammed Charrout, Dicky J. Lindenbergh-Kortleve, Michail Doukas, Mathijs A. Sanders, Gregory van Beek, Johanna C. Escher, Lissy de Ridder, Maria Fernanda Pascutti, Janneke N. Samsom

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Figure 2

SLPI expression is increased in colonic epithelium of therapy-naive pediatric patients with CD or UC compared with IBD-negative controls.

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SLPI expression is increased in colonic epithelium of therapy-naive pedi...
(A and B) SLPI RNA expression values from microarray data for intestinal biopsies from adult patients with CD or UC and controls. Data are derived from GSE16879 (Arijs 2009 cohort) (A) and GSE75214 (Arijs 2017 cohort) (B). Horizontal bars represent medians. Wilcoxon’s rank sum test. (C) SLPI mRNA expression measured by qPCR in macroscopically non-inflamed and macroscopically inflamed intestinal biopsies from pediatric CD (n = 21), UC (n = 19), and IBD-negative controls (IBD-neg, n = 9). Each data point represents one biopsy. Box plots display medians and first and third quartiles. Wilcoxon’s rank sum test. (D and E) SLPI protein expression detected by IHC in macroscopically non-inflamed and macroscopically inflamed intestinal biopsies from pediatric CD (n = 41), UC (n = 22), and IBD-negative controls (n = 15). (D) Representative images were acquired at ×20 magnification. (E) Intensity of intestinal epithelial SLPI staining scored semiquantitatively. Distribution of maximum SLPI scores and percentage of patients with each SLPI IHC score per group are shown. Fisher’s exact test. (F and G) Clinical characteristics per SLPI IHC score group using the SLPI IHC score for the colonic biopsy with the highest modified GHAS per patient. (F) Percentages of patients with CD (n = 40) versus UC (n = 22) and percentages of patients with no or mild clinical disease activity (n = 25) versus patients with moderate to severe clinical disease activity (n = 37). Pearson’s χ2 test. (G) SES-CD score in CD patients with a complete endoscopy (n = 31); UCEIS score in all UC patients (n = 22); and “total UCEIS” (the sum of the UCEIS of each colonic segment) in UC patients with a complete endoscopy (n = 21). The size of the circles represents the number of patients. Kruskal-Wallis rank sum test. For additional statistical comparisons, see Supplemental Table 2.