PT  - JOURNAL ARTICLE
AU  - Lisa L. von Moltke
AU  - David J. Greenblatt
AU  - Gina M. Giancarlo
AU  - Brian W. Granda
AU  - Jerold S. Harmatz
AU  - Richard I. Shader
TI  - Escitalopram (&lt;em&gt;S&lt;/em&gt;-Citalopram) and Its Metabolites in Vitro: Cytochromes Mediating Biotransformation, Inhibitory Effects, and Comparison to  &lt;em&gt;R&lt;/em&gt;-Citalopram
DP  - 2001 Aug 01
TA  - Drug Metabolism and Disposition
PG  - 1102--1109
VI  - 29
IP  - 8
4099  - http://dmd.aspetjournals.org/content/29/8/1102.short
4100  - http://dmd.aspetjournals.org/content/29/8/1102.full
SO  - Drug Metab Dispos2001 Aug 01; 29
AB  - Transformation of escitalopram (S-CT), the pharmacologically active S-enantiometer of citalopram, to S-desmethyl-CT (S-DCT), and ofS-DCT to S-didesmethyl-CT (S-DDCT), was studied in human liver microsomes and in expressed cytochromes (CYPs). Biotransformation of theR-enantiomer (R-CT) was studied in parallel. S-CT was transformed to S-DCT by CYP2C19 (Km = 69 μM), CYP2D6 (Km = 29 μM), and CYP3A4 (Km = 588 μM). After normalization for hepatic abundance, relative contributions to net intrinsic clearance were 37% for CYP2C19, 28% for CYP2D6, and 35% for CYP3A4. At 10 μM S-CT in liver microsomes,S-DCT formation was reduced to 60% of control by 1 μM ketoconazole, and to 80 to 85% of control by 5 μM quinidine or 25 μM omeprazole. S-DDCT was formed fromS-DCT only by CYP2D6; incomplete inhibition by quinidine in liver microsomes indicated participation of a non-CYP pathway. Based on established index reactions, S-CT andS-DCT were negligible inhibitors (IC50&amp;gt; 100 μM) of CYP1A2, -2C9, -2C19, -2E1, and -3A, and weakly inhibited CYP2D6 (IC50 = 70–80 μM).R-CT and its metabolites, studied using the same procedures, had properties very similar to those of the correspondingS-enantiomers. Thus S-CT, biotransformed by three CYP isoforms in parallel, is unlikely to be affected by drug interactions or genetic polymorphisms. S-CT andS-DCT are also unlikely to cause clinically important drug interactions via CYP inhibition. The American Society for Pharmacology and Experimental Therapeutics