Literature DB >> 26964996

Gut Wall Metabolism. Application of Pre-Clinical Models for the Prediction of Human Drug Absorption and First-Pass Elimination.

Christopher R Jones1,2, Oliver J D Hatley3, Anna-Lena Ungell4,5, Constanze Hilgendorf6, Sheila Annie Peters7, Amin Rostami-Hodjegan8.   

Abstract

Quantifying the multiple processes which control and modulate the extent of oral bioavailability for drug candidates is critical to accurate projection of human pharmacokinetics (PK). Understanding how gut wall metabolism and hepatic elimination factor into first-pass clearance of drugs has improved enormously. Typically, the cytochrome P450s, uridine 5'-diphosphate-glucuronosyltransferases and sulfotransferases, are the main enzyme classes responsible for drug metabolism. Knowledge of the isoforms functionally expressed within organs of first-pass clearance, their anatomical topology (e.g. zonal distribution), protein homology and relative abundances and how these differ across species is important for building models of human metabolic extraction. The focus of this manuscript is to explore the parameters influencing bioavailability and to consider how well these are predicted in human from animal models or from in vitro to in vivo extrapolation. A unique retrospective analysis of three AstraZeneca molecules progressed to first in human PK studies is used to highlight the impact that species differences in gut wall metabolism can have on predicted human PK. Compared to the liver, pharmaceutical research has further to go in terms of adopting a common approach for characterisation and quantitative prediction of intestinal metabolism. A broad strategy is needed to integrate assessment of intestinal metabolism in the context of typical DMPK activities ongoing within drug discovery programmes up until candidate drug nomination.

Entities:  

Keywords:  animal models; drug-metabolising enzymes; first-pass oral clearance; gut wall metabolism; oral bioavailability

Mesh:

Substances:

Year:  2016        PMID: 26964996      PMCID: PMC5256607          DOI: 10.1208/s12248-016-9889-y

Source DB:  PubMed          Journal:  AAPS J        ISSN: 1550-7416            Impact factor:   4.009


  95 in total

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2.  Evaluation of the human prediction of clearance from hepatocyte and microsome intrinsic clearance for 52 drug compounds.

Authors:  A-K Sohlenius-Sternbeck; L Afzelius; P Prusis; J Neelissen; J Hoogstraate; J Johansson; E Floby; A Bengtsson; O Gissberg; J Sternbeck; C Petersson
Journal:  Xenobiotica       Date:  2010-09       Impact factor: 1.908

3.  Quantitation of extrahepatic metabolism. Pulmonary and intestinal conjugation of naphthol.

Authors:  M Mistry; J B Houston
Journal:  Drug Metab Dispos       Date:  1985 Nov-Dec       Impact factor: 3.922

4.  A unified model for predicting human hepatic, metabolic clearance from in vitro intrinsic clearance data in hepatocytes and microsomes.

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Journal:  Drug Metab Dispos       Date:  2005-06-02       Impact factor: 3.922

5.  Tacrolimus oral bioavailability doubles with coadministration of ketoconazole.

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Journal:  Clin Pharmacol Ther       Date:  1997-07       Impact factor: 6.875

6.  Comparison of oral absorption and bioavailablity of drugs between monkey and human.

Authors:  Win L Chiou; Paul W Buehler
Journal:  Pharm Res       Date:  2002-06       Impact factor: 4.200

7.  Glucuronidation of carcinogenic arylamines and their N-hydroxy derivatives by rat and human phenol UDP-glucuronosyltransferase of the UGT1 gene complex.

Authors:  A Orzechowski; D Schrenk; B S Bock-Hennig; K W Bock
Journal:  Carcinogenesis       Date:  1994-08       Impact factor: 4.944

8.  Lead optimization of ethyl 6-aminonicotinate acyl sulfonamides as antagonists of the P2Y12 receptor. separation of the antithrombotic effect and bleeding for candidate drug AZD1283.

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5.  Optimization of intestinal microsomal preparation in the rat: A systematic approach to assess the influence of various methodologies on metabolic activity and scaling factors.

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  10 in total

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