From achiral to chiral analysis of citalopram

Carlsson, Björn

January 2003

Within the field of depression the “monoamine hypothesis” has been the leading theory to explain the biological basis of depression. This theory proposes that the biological basis of depression is due to a deficiency in one or more of three key neurotransmitter systems, namely noradrenaline, dopamine and serotonin which are thought to mediate the therapeutic actions of virtually every known antidepressant agent. Citalopram is a selective serotonin-reuptake inhibitor (SSRI) used for the treatment of depression and anxiety disorders. Citalopram is a racemic compound, in other words composed of a 50:50 mixture of two enantiomers (S-(+)-citalopram and R-(-)-citalopram) and with one of the enantiomers (S-(+)-citalopram) accounting for the inhibitory effect. At the time of introduction of citalopram the physician needed a therapeutic drug monitoring service to identify patients with interactions, compliance problems and for handling questions concerning polymorphic enzymes and drug metabolism. An achiral analytical separation method based on solid-phase extraction followed by high-performance liquid chromatography (HPLC) was developed for routine therapeutic drug monitoring (TDM) of citalopram and its two main demethylated metabolites. As the data available on citalopram were from achiral concentration determinations and to be able to further investigate citalopram enantiomers effects and distribution, a chiral method for separation of the enantiomers of citalopram and its demethylated metabolites was established. The advances within chiral separation techniques have made measurement of the concentrations of the individual enantiomers in biological fluids possible. The process behind enantioselective separation is however not fully understood and the mechanism behind the separation can be further scrutinized by the use of multivariate methods. A study of the optimization and characterization of the separation of the enantiomers of citalopram, desmethylcitalopram and didesmethylcitalopram on an acetylated ß-cyclodextrin column, by use of two different chemometric programs - response surface modelling and sequential optimization was performed. Sequential optimization can be a quicker mean of optimizing a chromatographic separation; response surface modelling, in addition to enabling optimization of the chromatographic process, also serves as a tool for learning more about the separation mechanism. Studies of the antidepressant effect and pharmacokinetics of citalopram have been performed in adults, but the effects on children and adolescents have only been studied to a minor extent, despite the increasing use of citalopram in these age groups. A study was initiated to investigate adolescents treated for depression, with respect to the steady-state plasma concentrations of the enantiomers of citalopram and its demethylated metabolites. The ratios between the S- and R-enantiomers of citalopram and didesmethylcitalopram were in agreement with studies involving older patients. The concentrations of the S-(+)- and R-(-) enantiomers of citalopram and desmethylcitalopram were also in agreement with values from earlier studies. The results indicate that the use of oral contraceptives may have some influence on the metabolism of citalopram. This might be because of an interaction of the contraceptive hormones with the polymorphic CYP2C19 enzyme. Even though the SSRIs are considered less toxic compared with older monoamine-active drugs like the tricyclic/tetracyclic antidepressants, the risk of developing serious side effects such as ECG abnormalities and convulsions has been seen for citalopram, when larger doses have been ingested. Furthermore, fatal overdoses have been reported where citalopram alone was the cause of death. Data on the toxicity of each of the enantiomers in humans have not been reported and no data on blood levels of the enantiomers in cases of intoxication have been presented. An investigation was initiated on forensic autopsy cases where citalopram had been found at the routine screening and these cases were further analysed with enantioselective analysis to determine the blood concentrations of the enantiomers of citalopram and metabolites. Furthermore the genotyping regarding the polymorphic enzymes CYP2D6 and CYP2C19 were performed. In 53 autopsy cases, we found increasing S/R ratios with increasing concentrations of citalopram. We found also that high citalopram S/R ratio were associated with high parent drug to metabolite ratio and may be an indicator of recent intake. Only 3.8 % were found to be poor metabolizers regarding CYP2D6 and for CYP2C19 no poor metabolizer was found. Enantioselective analysis of citalopram and its metabolites can provide valuable information about the time that has elapsed between intake and death. Genotyping can be of help in specific cases but the possibility of pharmacokinetic interactions is apparently a far greater problem than genetic enzyme deficiency. / On the day of the public defence the status of article IV was: Submitted.

depression

noradrenaline

dopamine

serotonin

citalopram

therapeutic drug monitoring (TDM)

enantioselective separation

MEDICINE

MEDICIN

Enantioselektivní separace vybraných analytů v systémech superkritické fluidní chromatografie a vysokoúčinné kapalinové chromatografie / Enantioselective separation of certain analytes using supercritical fluid chromatography and high performance liquid chromatography

Martínková, Monika

January 2017

(EN) Cellulose tris-(3,5-dimethylphenylcarbamate) chiral stationary phase was used for separation of selected 24 analytes. Enantioseparations were realized using two systems, high performance liquid chromatography and supercritical fluid chromatography. Effect of mobile phase composition was studied. Five different aditives (isopropylamine, diethylamine, triethylamine, trifluoroacetic acid, isopropylamine combined with trifluoroacetic acid) and their influence on enantioseparation were tested. Influence of two different modifiers (methanol, propan-2-ol) combined with all aditives was also tested in supercritical fluid chromatography system. The aim of this work was to find optimized composition of mobile phase which was suitable for separation of the analytes studied and to compare separation potential among all mobile phases and also between used separations systems. The supercritical fluid chromatography was shown to yield better results, i.e. better resolution in shorter analysis time. However examples of analytes better resolved under optimized conditions in high performance liquid chromatography system have also been found. Keywords (EN) Chirality, enantiomers, enantioselective separation, chiral stationary phase, high performance liquid chromatography, supercritical fluid chromatography.

Conception et étude des propriétés physico-chimiques de réseaux de coordination / Conception and study of the physico-chemical properties of coordination networks

Corso, Romain

28 September 2018

L’essor de la chimie supramoléculaire et plus particulièrement de la tectonique moléculaire a rendu la formation de matériaux poreux hautement organisés possible. La fonctionnalisation de tels composés favorise leur utilisation pour de nombreuses applications. Les travaux présentés dans cette thèse ont été consacrés aux réseaux moléculaires poreux homochiraux ainsi que leur utilisation pour le stockage de gaz, la reconnaissance et la séparation d’énantiomères.Le premier chapitre décrit la synthèse de divers ligands organiques optiquement purs et leur assemblage avec des sels de cuivre pour l’obtention de monocristaux. Les isothermes d’adsorption de chacun de ces composés cristallins ont été mesurés via des analyses BET et le stockage de N2,CO2 et CH4 ont été évalué.Le second chapitre s’intéresse à l’utilisation de ces mêmes composés chiraux pour la reconnaissance des énantiomères (L)- et (D)-tryptophane. Des tests de séparation énantiosélective de molécules aminées ou dérivées d’amides sont également exposés.Le dernier chapitre décrit la formation de réseaux moléculaire mono- et tridimensionnels par l’association de ligands organiques avec des sels métalliques variés. Leurs structures cristallines ont pu être déterminées par diffraction des rayons X sur monocristal. / The development in supramolecular chemistry and more particularly in molecular tectonics has madepossible the formation of porous and highly organized materials. The functionalization of suchcompounds favored their use for various applications. This PhD work is about the application ofporous homochiral coordination networks for storage, enantioselective recognition or separation.The first chapter deals with the synthesis of chiral ligands and their combinations with copper salts toenable the formation of single crystals. Their adsorption isotherms were evaluated by BETmeasurements. Storage of N2, CO2 and CH4 by these crystalline architectures was also evaluated.The second part describes the use of these chiral compounds for enantioselective recognition of (L)-and (D)-tryptophan. Tests of enantioselective separation of amines or amides were also carried out.The last part of this work deals with the formation of mono- or tridimensional coordination polymersby combinations of organic ligands and a variety of metallic salts. Their structures were determinedby X-ray diffraction on single crystal.

Chimie Supramoléculaire

Réseaux de coordination

MOF

Chiralité

BET

Stockage de Gaz

Reconnaissance Enantiosélective

Séparation énantiosélective

Supramolecular Chemistry

Molecular tectonics

Coordination polymers

MOF

Chirality

BET

Gas Storage

Enantioselective recognition

Enantioselective separation

547.1