| Literature DB >> 18370465 |
L P Delbressine1, M E Moonen, F M Kaspersen, G N Wagenaars, P L Jacobs, C J Timmer, J E Paanakker, H J van Hal, G Voortman.
Abstract
This paper investigated the pharmacokinetics and biotransformation of mirtazapine in healthy human volunteers. The results showed that the area under the plasma drug concentration-time curve (AUC) of mirtazapine in human plasma appeared to be three times higher than the AUC of demethylmirtazapine. As mirtazapine is marketed as a racemic mixture and both enantiomers possess pharmacological properties essential for the overall activity of the racemate, the pharmacokinetics of mirtazapine were examined and appeared to be enantioselective. The R(-)-enantiomer showed the longest elimination half-life from plasma. This was ascribed to the preferred formation of a quaternary ammonium glucuronide of the R(-)-enantiomer. This glucuronide may be deconjugated, leading to a further circulation of the parent compound, thus causing a prolongation in the elimination half-life. The S(+)-enantiomer was preferentially metabolised into an 8-hydroxy glucuronide. Other metabolic transformation pathways found for mirtazapine were demethylation and N-oxidation. Mirtazapine was extensively metabolised and almost completely excreted in the urine (over 80%) and faeces within a few days after oral administration.Entities:
Year: 1998 PMID: 18370465 DOI: 10.2165/00044011-199815010-00006
Source DB: PubMed Journal: Clin Drug Investig ISSN: 1173-2563 Impact factor: 2.859