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5 - Predictability of metabolic antiepileptic drug interactions

from Part II - Pharmacokinetic interactions

Published online by Cambridge University Press:  07 September 2009

Edoardo Spina
Affiliation:
Section of Pharmacology, Department of Clinical and Experimental Medicine and Pharmacology, University of Messina, Messina, Italy
Emilio Perucca
Affiliation:
Clinical Pharmacology Unit, University of Pavia, Pavia, Italy
Rene Levy
Affiliation:
Department of Pharmaceutics, University of Washington, Seattle, WA, USA
Jerzy Majkowski
Affiliation:
Foundation of Epileptology, Warsaw
Blaise F. D. Bourgeois
Affiliation:
Harvard University, Massachusetts
Philip N. Patsalos
Affiliation:
Institute of Neurology, London
Richard H. Mattson
Affiliation:
Yale University, Connecticut
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Summary

Principles of drug metabolism

Many drugs are lipid soluble, weak organic acids or bases that are not readily eliminated from the body, being reabsorbed into the blood from the glomerular filtrate. Metabolic processes are necessary to convert a drug into one or more metabolites which are chemically different from the parent compound, but generally more polar and water soluble, facilitating their excretion in urine or bile. Although metabolism usually results in inactivation or detoxification, many drug metabolites have pharmacological activity. Metabolites may occasionally be much more active than the parent compound (which then may be designated as a prodrug), they may exert effects similar to or different from those of the parent molecule, or they may be responsible for toxic effects (Perucca and Richens, 1995). When metabolites are active, termination of their action occurs by further biotransformation or by direct excretion of the metabolite in urine or bile.

The chemical reactions involved in the biotransformation of drugs are catalyzed by various enzyme systems and are conventionally divided into phase I (functionalization) and phase II (conjugation) biotransformation reactions, which may occur in series. Phase I reactions involve the addition of a polar functional group (e.g. a hydroxyl group) or the deletion of a non-polar alkyl group (e.g. N-demethylation) by oxidation, reduction, or hydrolysis.

Type
Chapter
Information
Antiepileptic Drugs
Combination Therapy and Interactions
, pp. 57 - 92
Publisher: Cambridge University Press
Print publication year: 2005

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