Intestinal Absorption of FITC-Dextrans and Macromolecular Model Drugs in the Rat Intestinal Instillation Model

[Image: see text] In this work, we studied the intestinal absorption of a peptide with a molecular weight of 4353 Da (MEDI7219) and a protein having a molecular weight of 11 740 Da (PEP12210) in the rat intestinal instillation model and compared their absorption to fluorescein isothiocyanate (FITC)-...

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Autores principales: Berg, Staffan, Suljovic, Denny, Kärrberg, Lillevi, Englund, Maria, Bönisch, Heiko, Karlberg, Ida, Van Zuydam, Natalie, Abrahamsson, Bertil, Hugerth, Andreas Martin, Davies, Nigel, Bergström, Christel A. S.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Chemical Society 2022
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9257752/
https://www.ncbi.nlm.nih.gov/pubmed/35642793
http://dx.doi.org/10.1021/acs.molpharmaceut.2c00261
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author Berg, Staffan
Suljovic, Denny
Kärrberg, Lillevi
Englund, Maria
Bönisch, Heiko
Karlberg, Ida
Van Zuydam, Natalie
Abrahamsson, Bertil
Hugerth, Andreas Martin
Davies, Nigel
Bergström, Christel A. S.
author_facet Berg, Staffan
Suljovic, Denny
Kärrberg, Lillevi
Englund, Maria
Bönisch, Heiko
Karlberg, Ida
Van Zuydam, Natalie
Abrahamsson, Bertil
Hugerth, Andreas Martin
Davies, Nigel
Bergström, Christel A. S.
author_sort Berg, Staffan
collection PubMed
description [Image: see text] In this work, we studied the intestinal absorption of a peptide with a molecular weight of 4353 Da (MEDI7219) and a protein having a molecular weight of 11 740 Da (PEP12210) in the rat intestinal instillation model and compared their absorption to fluorescein isothiocyanate (FITC)-labeled dextrans of similar molecular weights (4 and 10 kDa). To increase the absorption of the compounds, the permeation enhancer sodium caprate (C10) was included in the liquid formulations at concentrations of 50 and 300 mM. All studied compounds displayed an increased absorption rate and extent when delivered together with 50 mM C10 as compared to control formulations not containing C10. The time period during which the macromolecules maintained an increased permeability through the intestinal epithelium was approximately 20 min for all studied compounds at 50 mM C10. For the formulations containing 300 mM C10, it was noted that the dextrans displayed an increased absorption rate (compared to 50 mM C10), and their absorption continued for at least 60 min. The absorption rate of MEDI7219, on the other hand, was similar at both studied C10 concentrations, but the duration of absorption was extended at the higher enhancer concentration, leading to an increase in the overall extent of absorption. The absorption of PEP12210 was similar in terms of the rate and duration at both studied C10 concentrations. This is likely caused by the instability of this molecule in the intestinal lumen. The degradation decreases the luminal concentrations over time, which in turn limits absorption at time points beyond 20 min. The results from this study show that permeation enhancement effects cannot be extrapolated between different types of macromolecules. Furthermore, to maximize the absorption of a macromolecule delivered together with C10, prolonging the duration of absorption appears to be important. In addition, the macromolecule needs to be stable enough in the intestinal lumen to take advantage of the prolonged absorption time window enabled by the permeation enhancer.
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spelling pubmed-92577522022-07-07 Intestinal Absorption of FITC-Dextrans and Macromolecular Model Drugs in the Rat Intestinal Instillation Model Berg, Staffan Suljovic, Denny Kärrberg, Lillevi Englund, Maria Bönisch, Heiko Karlberg, Ida Van Zuydam, Natalie Abrahamsson, Bertil Hugerth, Andreas Martin Davies, Nigel Bergström, Christel A. S. Mol Pharm [Image: see text] In this work, we studied the intestinal absorption of a peptide with a molecular weight of 4353 Da (MEDI7219) and a protein having a molecular weight of 11 740 Da (PEP12210) in the rat intestinal instillation model and compared their absorption to fluorescein isothiocyanate (FITC)-labeled dextrans of similar molecular weights (4 and 10 kDa). To increase the absorption of the compounds, the permeation enhancer sodium caprate (C10) was included in the liquid formulations at concentrations of 50 and 300 mM. All studied compounds displayed an increased absorption rate and extent when delivered together with 50 mM C10 as compared to control formulations not containing C10. The time period during which the macromolecules maintained an increased permeability through the intestinal epithelium was approximately 20 min for all studied compounds at 50 mM C10. For the formulations containing 300 mM C10, it was noted that the dextrans displayed an increased absorption rate (compared to 50 mM C10), and their absorption continued for at least 60 min. The absorption rate of MEDI7219, on the other hand, was similar at both studied C10 concentrations, but the duration of absorption was extended at the higher enhancer concentration, leading to an increase in the overall extent of absorption. The absorption of PEP12210 was similar in terms of the rate and duration at both studied C10 concentrations. This is likely caused by the instability of this molecule in the intestinal lumen. The degradation decreases the luminal concentrations over time, which in turn limits absorption at time points beyond 20 min. The results from this study show that permeation enhancement effects cannot be extrapolated between different types of macromolecules. Furthermore, to maximize the absorption of a macromolecule delivered together with C10, prolonging the duration of absorption appears to be important. In addition, the macromolecule needs to be stable enough in the intestinal lumen to take advantage of the prolonged absorption time window enabled by the permeation enhancer. American Chemical Society 2022-06-01 2022-07-04 /pmc/articles/PMC9257752/ /pubmed/35642793 http://dx.doi.org/10.1021/acs.molpharmaceut.2c00261 Text en © 2022 The Authors. Published by American Chemical Society https://creativecommons.org/licenses/by/4.0/Permits the broadest form of re-use including for commercial purposes, provided that author attribution and integrity are maintained (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Berg, Staffan
Suljovic, Denny
Kärrberg, Lillevi
Englund, Maria
Bönisch, Heiko
Karlberg, Ida
Van Zuydam, Natalie
Abrahamsson, Bertil
Hugerth, Andreas Martin
Davies, Nigel
Bergström, Christel A. S.
Intestinal Absorption of FITC-Dextrans and Macromolecular Model Drugs in the Rat Intestinal Instillation Model
title Intestinal Absorption of FITC-Dextrans and Macromolecular Model Drugs in the Rat Intestinal Instillation Model
title_full Intestinal Absorption of FITC-Dextrans and Macromolecular Model Drugs in the Rat Intestinal Instillation Model
title_fullStr Intestinal Absorption of FITC-Dextrans and Macromolecular Model Drugs in the Rat Intestinal Instillation Model
title_full_unstemmed Intestinal Absorption of FITC-Dextrans and Macromolecular Model Drugs in the Rat Intestinal Instillation Model
title_short Intestinal Absorption of FITC-Dextrans and Macromolecular Model Drugs in the Rat Intestinal Instillation Model
title_sort intestinal absorption of fitc-dextrans and macromolecular model drugs in the rat intestinal instillation model
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9257752/
https://www.ncbi.nlm.nih.gov/pubmed/35642793
http://dx.doi.org/10.1021/acs.molpharmaceut.2c00261
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