Evaluation in pig of an intestinal administration device for oral peptide delivery

Staffan Berg; Teresia Uggla; Malin Antonsson; Sandro Filipe Nunes; Maria Englund; Louise Rosengren; Masoud Fahraj; Xiaoqiu Wu; Rydvikha Govender; Magnus Söderberg; David Janzén; Natalie Van Zuydam; Andreas Hugerth; Anette Larsson; Susanna Abrahmsén-Alami; Bertil Abrahamsson; Nigel Davies; Christel A S Bergström

doi:10.1016/j.jconrel.2022.12.011

Evaluation in pig of an intestinal administration device for oral peptide delivery

J Control Release. 2023 Jan:353:792-801. doi: 10.1016/j.jconrel.2022.12.011. Epub 2022 Dec 16.

Authors

Staffan Berg¹, Teresia Uggla², Malin Antonsson², Sandro Filipe Nunes², Maria Englund³, Louise Rosengren³, Masoud Fahraj⁴, Xiaoqiu Wu⁴, Rydvikha Govender⁵, Magnus Söderberg⁶, David Janzén³, Natalie Van Zuydam⁷, Andreas Hugerth⁸, Anette Larsson⁹, Susanna Abrahmsén-Alami¹⁰, Bertil Abrahamsson⁵, Nigel Davies⁴, Christel A S Bergström¹¹

Affiliations

¹ The Swedish Drug Delivery Center, Department of Pharmacy, Uppsala University, BMC P.O. Box 580, SE-751 23 Uppsala, Sweden; Advanced Drug Delivery, Pharmaceutical Sciences, R&D, AstraZeneca, Gothenburg, Sweden.
² Animal Sciences and Technologies, Clinical Pharmacology and Safety Sciences, BioPharmaceuticals R&D, AstraZeneca, Gothenburg, Sweden.
³ Drug Metabolism and Pharmacokinetics, Research and Early Development, Cardiovascular, Renal and Metabolism, BioPharmaceuticals R&D, AstraZeneca, Gothenburg, Sweden.
⁴ Advanced Drug Delivery, Pharmaceutical Sciences, R&D, AstraZeneca, Gothenburg, Sweden.
⁵ Oral Product Development, Pharmaceutical Technology & Development, Operations, AstraZeneca Gothenburg, Sweden.
⁶ Cardiovascular, Renal and Metabolism Safety, Clinical Pharmacology & Safety Sciences, BioPharmaceuticals R&D, AstraZeneca, Gothenburg, Sweden.
⁷ Data Science and Quantitative Biology, Discovery Sciences, BioPharmaceuticals R&D, AstraZeneca, Gothenburg, Sweden.
⁸ Ferring Pharmaceuticals A/S, Product Development and Drug Delivery, Global Pharmaceutical R&D, Amager Strandvej 405, 2770 Kastrup, Denmark.
⁹ Applied Chemistry, Department of Chemistry and Chemical Engineering, Chalmers University of Technology, SE-412 96 Gothenburg, Sweden.
¹⁰ Innovation Strategies & External Liasons, Pharmaceutical Technology & Development, Operations, AstraZeneca Gothenburg, Sweden.
¹¹ The Swedish Drug Delivery Center, Department of Pharmacy, Uppsala University, BMC P.O. Box 580, SE-751 23 Uppsala, Sweden. Electronic address: christel.bergstrom@farmaci.uu.se.

PMID: 36493948
DOI: 10.1016/j.jconrel.2022.12.011

Abstract

The bioavailability of peptides co-delivered with permeation enhancers following oral administration remains low and highly variable. Two factors that may contribute to this are the dilution of the permeation enhancer in the intestinal fluid, as well as spreading of the released permeation enhancer and peptide in the lumen by intestinal motility. In this work we evaluated an Intestinal Administration Device (IAD) designed to reduce the luminal dilution of drug and permeation enhancer, and to minimize movement of the dosage form in the intestinal lumen. To achieve this, the IAD utilizes an expanding design that holds immediate release mini tablets and places these in contact with the intestinal epithelium, where unidirectional drug release can occur. The expanding conformation limits movement of the IAD in the intestinal tract, thereby enabling drug release at a single focal point in the intestine. A pig model was selected to study the ability of the IAD to promote intestinal absorption of the peptide MEDI7219 formulated together with the permeation enhancer sodium caprate. We compared the IAD to intestinally administered enteric coated capsules and an intestinally administered solution. The IAD restricted movement of the immediate release tablets in the small intestine and histological evaluation of the mucosa indicated that high concentrations of sodium caprate were achieved. Despite significant effect of the permeation enhancer on the integrity of the intestinal epithelium, the bioavailability of MEDI7219 was of the same order of magnitude as that achieved with the solution and enteric coated capsule formulations (2.5-3.8%). The variability in plasma concentrations of MEDI7219 were however lower when delivered using the IAD as compared to the solution and enteric coated capsule formulations. This suggests that dosage forms that can limit intestinal dilution and control the position of drug release can be a way to reduce the absorptive variability of peptides delivered with permeation enhancers but do not offer significant benefits in terms of increasing bioavailability.

Keywords: Intestinal administration; MEDI7219; Oral peptide delivery; Permeation enhancer; Sodium caprate.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Administration, Oral
Animals
Biological Availability
Intestinal Absorption
Intestinal Mucosa* / metabolism
Intestines*
Peptides / chemistry
Swine
Tablets

Substances

MEDI7219
Peptides
Tablets