The Metabolic Inhibition Model Which Predicts the Intestinal Absorbability and Metabolizability of Drug: Theory and Experiment

The Metabolic Inhibition Model Which Predicts the Intestinal Absorbability and Metabolizability of Drug: Theory and Experiment

<p>The intestinal absorption of analgesic peptides (leucine enkephalin and kyotorphin) and modified peptides in rat were studied. Although these peptides were not absorbed, the absorbability (absorption clearance) of these peptides were increased in the presence of peptidase inhibitors. In ord...

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Main Authors: Mizuma Takashi, Awazu Shoji
Format: Article
Language:English
Published: BMC 1998-01-01
Series:Biological Procedures Online
Subjects:
intestinal absorption
pharmacokinetics
Online Access:http://www.biologicalprocedures.com/bpo/arts/1/8/m8.htm
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spelling doaj-180cf8f64a3244a685710376e77cf56a2020-11-25T01:10:55ZengBMCBiological Procedures Online1480-92221998-01-0111323910.1251/bpo8The Metabolic Inhibition Model Which Predicts the Intestinal Absorbability and Metabolizability of Drug: Theory and Experiment Mizuma TakashiAwazu Shoji<p>The intestinal absorption of analgesic peptides (leucine enkephalin and kyotorphin) and modified peptides in rat were studied. Although these peptides were not absorbed, the absorbability (absorption clearance) of these peptides were increased in the presence of peptidase inhibitors. In order to kinetically analyze these phenomena, we proposed the metabolic inhibition model, which incorporated the metabolic clearance (metabolizability) with the absorption clearance. Metabolic activity was determined with intestinal homogenates. The higher the metabolic clearance was, the lower was the absorption clearance. The relationships between the absorption clearance and the metabolic clearance of the experimental data as well as of the theoretical values were hyperbolic. This model predicted the maximum absorption clearances of cellobiose-coupled leucine enkephalin (0.654 &mgr;l/min/cm) and kyotorphin (0.247 &mgr;l/min/cm). Details of the experimental methods are described. http://www.biologicalprocedures.com/bpo/arts/1/8/m8.htmintestinal absorptionpharmacokinetics
collection DOAJ
language English
format Article
sources DOAJ
author Mizuma Takashi
Awazu Shoji
spellingShingle Mizuma Takashi
Awazu Shoji
The Metabolic Inhibition Model Which Predicts the Intestinal Absorbability and Metabolizability of Drug: Theory and Experiment
Biological Procedures Online
intestinal absorption
pharmacokinetics
author_facet Mizuma Takashi
Awazu Shoji
author_sort Mizuma Takashi
title The Metabolic Inhibition Model Which Predicts the Intestinal Absorbability and Metabolizability of Drug: Theory and Experiment
title_short The Metabolic Inhibition Model Which Predicts the Intestinal Absorbability and Metabolizability of Drug: Theory and Experiment
title_full The Metabolic Inhibition Model Which Predicts the Intestinal Absorbability and Metabolizability of Drug: Theory and Experiment
title_fullStr The Metabolic Inhibition Model Which Predicts the Intestinal Absorbability and Metabolizability of Drug: Theory and Experiment
title_full_unstemmed The Metabolic Inhibition Model Which Predicts the Intestinal Absorbability and Metabolizability of Drug: Theory and Experiment
title_sort metabolic inhibition model which predicts the intestinal absorbability and metabolizability of drug: theory and experiment
publisher BMC
series Biological Procedures Online
issn 1480-9222
publishDate 1998-01-01
description <p>The intestinal absorption of analgesic peptides (leucine enkephalin and kyotorphin) and modified peptides in rat were studied. Although these peptides were not absorbed, the absorbability (absorption clearance) of these peptides were increased in the presence of peptidase inhibitors. In order to kinetically analyze these phenomena, we proposed the metabolic inhibition model, which incorporated the metabolic clearance (metabolizability) with the absorption clearance. Metabolic activity was determined with intestinal homogenates. The higher the metabolic clearance was, the lower was the absorption clearance. The relationships between the absorption clearance and the metabolic clearance of the experimental data as well as of the theoretical values were hyperbolic. This model predicted the maximum absorption clearances of cellobiose-coupled leucine enkephalin (0.654 &mgr;l/min/cm) and kyotorphin (0.247 &mgr;l/min/cm). Details of the experimental methods are described.
topic intestinal absorption
pharmacokinetics
url http://www.biologicalprocedures.com/bpo/arts/1/8/m8.htm
work_keys_str_mv AT mizumatakashi themetabolicinhibitionmodelwhichpredictstheintestinalabsorbabilityandmetabolizabilityofdrugtheoryandexperiment
AT awazushoji themetabolicinhibitionmodelwhichpredictstheintestinalabsorbabilityandmetabolizabilityofdrugtheoryandexperiment
AT mizumatakashi metabolicinhibitionmodelwhichpredictstheintestinalabsorbabilityandmetabolizabilityofdrugtheoryandexperiment
AT awazushoji metabolicinhibitionmodelwhichpredictstheintestinalabsorbabilityandmetabolizabilityofdrugtheoryandexperiment
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