Effect of Crohn’s Disease on Villous Length and CYP3A4 Expression in the Pediatric Small Intestine

Effect of Crohn’s Disease on Villous Length and CYP3A4 Expression in the Pediatric Small Intestine

Changes in absorptive capacity and first‐pass metabolism in the small intestine affect oral drug bioavailability. Characterization of such changes as a consequence of inflammation is important for developing physiologically‐based pharmacokinetic (PBPK) models for inflammatory bowel disease. We sough...

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Main Authors: Carrie A Vyhlidal, Brian D. Chapron, Atif Ahmed, Vivekanand Singh, Rebecca Casini, Valentina Shakhnovich
Format: Article
Language:English
Published: Wiley 2021-03-01
Series:Clinical and Translational Science
Online Access:https://doi.org/10.1111/cts.12938
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spelling doaj-7ce09dbdbf024a4eaf7d5bd7226990612021-03-25T15:37:47ZengWileyClinical and Translational Science1752-80541752-80622021-03-0114272973610.1111/cts.12938Effect of Crohn’s Disease on Villous Length and CYP3A4 Expression in the Pediatric Small IntestineCarrie A Vyhlidal0Brian D. Chapron1Atif Ahmed2Vivekanand Singh3Rebecca Casini4Valentina Shakhnovich5Division of Clinical Pharmacology, Toxicology and Therapeutic Innovation Children’s Mercy Kansas City Kansas City Missouri USADivision of Clinical Pharmacology, Toxicology and Therapeutic Innovation Children’s Mercy Kansas City Kansas City Missouri USADepartment of Pediatrics University of Missouri - Kansas City School of Medicine Kansas City Missouri USADivision of Pathology UT Southwestern Medical Center Dallas Texas USANorthShore University Health System Skokie Illinois USADivision of Clinical Pharmacology, Toxicology and Therapeutic Innovation Children’s Mercy Kansas City Kansas City Missouri USAChanges in absorptive capacity and first‐pass metabolism in the small intestine affect oral drug bioavailability. Characterization of such changes as a consequence of inflammation is important for developing physiologically‐based pharmacokinetic (PBPK) models for inflammatory bowel disease. We sought to elucidate the impact of small intestinal Crohn’s disease (CD) on villous length and CYP3A4 expression in children. Freshly frozen duodenal and terminal ileum (TI) biopsies from 107 children (1–19 years) with and without CD were evaluated for active inflammation. Villous length and CYP3A4 mRNA/protein expression were compared among regions of active and inactive inflammation in CD and controls. A twofold reduction in villous length was observed in inflamed duodena and ilia of children with CD, but in the absence of regional inflammation, villi in CD were comparable in length to controls. Expression of CYP3A4 mRNA correlated significantly with villous length in the TI (P = 0.0003), with a trend observed in the duodenum that did not reach statistical significance. In the presence of active inflammation, a significant decrease in CYP3A protein expression was confirmed in the duodenum, where protein expression also correlated significantly with villous length across diagnoses (P < 0.0001). Our findings suggest that previous observations of decreased CYP3A4 expression and function in inflamed intestine may not be due solely to downregulation by inflammatory cytokines, but also to villous blunting and subsequent loss of surface area for protein expression. This information is relevant for PBPK model development and could aid with dose adjustment decisions for oral CYP3A4 substrates administered during CD flare (e.g., budesonide).https://doi.org/10.1111/cts.12938
collection DOAJ
language English
format Article
sources DOAJ
author Carrie A Vyhlidal
Brian D. Chapron
Atif Ahmed
Vivekanand Singh
Rebecca Casini
Valentina Shakhnovich
spellingShingle Carrie A Vyhlidal
Brian D. Chapron
Atif Ahmed
Vivekanand Singh
Rebecca Casini
Valentina Shakhnovich
Effect of Crohn’s Disease on Villous Length and CYP3A4 Expression in the Pediatric Small Intestine
Clinical and Translational Science
author_facet Carrie A Vyhlidal
Brian D. Chapron
Atif Ahmed
Vivekanand Singh
Rebecca Casini
Valentina Shakhnovich
author_sort Carrie A Vyhlidal
title Effect of Crohn’s Disease on Villous Length and CYP3A4 Expression in the Pediatric Small Intestine
title_short Effect of Crohn’s Disease on Villous Length and CYP3A4 Expression in the Pediatric Small Intestine
title_full Effect of Crohn’s Disease on Villous Length and CYP3A4 Expression in the Pediatric Small Intestine
title_fullStr Effect of Crohn’s Disease on Villous Length and CYP3A4 Expression in the Pediatric Small Intestine
title_full_unstemmed Effect of Crohn’s Disease on Villous Length and CYP3A4 Expression in the Pediatric Small Intestine
title_sort effect of crohn’s disease on villous length and cyp3a4 expression in the pediatric small intestine
publisher Wiley
series Clinical and Translational Science
issn 1752-8054
1752-8062
publishDate 2021-03-01
description Changes in absorptive capacity and first‐pass metabolism in the small intestine affect oral drug bioavailability. Characterization of such changes as a consequence of inflammation is important for developing physiologically‐based pharmacokinetic (PBPK) models for inflammatory bowel disease. We sought to elucidate the impact of small intestinal Crohn’s disease (CD) on villous length and CYP3A4 expression in children. Freshly frozen duodenal and terminal ileum (TI) biopsies from 107 children (1–19 years) with and without CD were evaluated for active inflammation. Villous length and CYP3A4 mRNA/protein expression were compared among regions of active and inactive inflammation in CD and controls. A twofold reduction in villous length was observed in inflamed duodena and ilia of children with CD, but in the absence of regional inflammation, villi in CD were comparable in length to controls. Expression of CYP3A4 mRNA correlated significantly with villous length in the TI (P = 0.0003), with a trend observed in the duodenum that did not reach statistical significance. In the presence of active inflammation, a significant decrease in CYP3A protein expression was confirmed in the duodenum, where protein expression also correlated significantly with villous length across diagnoses (P < 0.0001). Our findings suggest that previous observations of decreased CYP3A4 expression and function in inflamed intestine may not be due solely to downregulation by inflammatory cytokines, but also to villous blunting and subsequent loss of surface area for protein expression. This information is relevant for PBPK model development and could aid with dose adjustment decisions for oral CYP3A4 substrates administered during CD flare (e.g., budesonide).
url https://doi.org/10.1111/cts.12938
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