Severity of coeliac disease and clinical management study when using a non-metabolised medication: a phase I pharmacokinetic study

Marc L Chretien; David G Bailey; Linda Asher; Jeremy Parfitt; David Driman; Jamie Gregor; George K Dresser

doi:10.1136/bmjopen-2021-057151

Severity of coeliac disease and clinical management study when using a non-metabolised medication: a phase I pharmacokinetic study

BMJ Open. 2023 Feb 24;13(2):e057151. doi: 10.1136/bmjopen-2021-057151.

Authors

Marc L Chretien¹, David G Bailey^{2

3}, Linda Asher², Jeremy Parfitt⁴, David Driman⁴, Jamie Gregor⁵, George K Dresser^{2

3}

Affiliations

¹ Division of Clinical Pharmacology, Department of Medicine, Schulich School of Medicine & Dentistry, Western University, London, Ontario, Canada marc.chretien@lhsc.on.ca.
² Division of Clinical Pharmacology, Department of Medicine, Schulich School of Medicine & Dentistry, Western University, London, Ontario, Canada.
³ Lawson Health Research Institute, London, Ontario, Canada.
⁴ Division of Pathology & Laboratory Medicine, Department of Medicine, Schulich School of Medicine & Dentistry, Western University, London, Ontario, Canada.
⁵ Division of Gastroenterology, Department of Medicine, Schulich School of Medicine & Dentistry, Western University, London, Ontario, Canada.

Abstract

Objective: The non-metabolised antihistamine fexofenadine has oral absorption resulting from transporter activity. Uptake by enterocyte organic anion transporting polypeptides and efflux by an ATP-binding cassette transporter (P-glycoprotein) are primary determinants. Coeliac disease-mediated lesions to the small intestinal mucosa may alter oral absorption of the drug probe, fexofenadine.

Design: A phase I, open-label, single-dose, pharmacokinetic study SETTING: London, Ontario, Canada PARTICIPANTS: Patients with coeliac disease (n=41) with positive serology and healthy individuals (n=48).

Main outcome measures: Patients with coeliac disease-duodenal histology and oral fexofenadine pharmacokinetics within a 3-week period. Healthy individuals-oral fexofenadine pharmacokinetics with water and grapefruit juice.

Results: Patients with coeliac disease were stratified by disease severity: Group A (n=15, normal), B+C (n=14, intraepithelial lymphocytosis with/without mild villous blunting) and D (n=12, moderate to severe villous blunting). Patients with coeliac disease in groups A, B+C and D and healthy individuals receiving water had similar fexofenadine AUC_0-8 (2038±304, 2259±367, 2128±410, 1954±138 ng.h/mL; p>0.05; mean±SEM) and Cmax (440±73, 513±96, 523±104, 453±32 ng/mL; p>0.05), respectively. These four groups all had higher fexofenadine AUC_0-8 (1063±59; p<0.01) and Cmax (253±18; p<0.05) compared with those for healthy individuals receiving grapefruit juice. Coeliac groups had a positive linear trend between disease severity and fexofenadine Tmax (2.0±0.3, 2.7±0.4, 3.1±0.5 hours; p<0.05).

Conclusions: Coeliac disease severity based on duodenal histopathology did not affect oral fexofenadine bioavailability. Increased Tmax suggested absorption distal to the duodenum (jejunum + ileum), where histology seems more normal which may be the key determinant. Patients with coeliac disease may not require consideration for alternative clinical drug management for a number of non-metabolised and transport-mediated medications.

Keywords: adverse events; clinical pharmacology; clinical trials; coeliac disease.

Publication types

Clinical Trial, Phase I
Research Support, Non-U.S. Gov't

MeSH terms

Celiac Disease*
Citrus paradisi*
Humans
Ontario
Terfenadine / pharmacokinetics
Water

Substances

fexofenadine
Terfenadine
Water

Grants and funding

MOP 77569/CIHR/Canada