Využití vysokoúčinných separačních metod pro analýzy biologicky aktivních látek / Analysis of biologically active compounds using high performance separation methods

Adamusová, Hana

January 2017

In the first part of this doctoral thesis, a new analytical HPLC-MS/MS method for monitoring of concentration changes of 17β-estradiol (βE2) during in vitro mouse sperm capacitation was developed. Capacitation was performed for three initial concentrations of βE2 (200, 20 and 2 μg/L). For all the concentrations a similar trend for the total unbound βE2 was observed. In general, the βE2 concentration decreased to reach its minimum and then increased again. The position of the minimum differed for the individual tested βE2 concentrations. Experimentally obtained results were subjected to the kinetic analysis. The curves fitted through the experimentally determined points displayed an autocatalytic character. For the agreement between the curves obtained by fitting through the experimental points and the theoretical calculated curves, it is necessary to assume that the first step is adsorption of βE2 onto the surface of the sperm controlled by Langmuir isotherm. The kinetic study was also used to study the effects of fluorides and aluminium fluoride complexes on the capacitation of mouse sperm. The experimental points were in very good agreement with the shape of the theoretical curves and this fact verifies the mechanism of the mouse sperm capacitation kinetics. In the second part of this work, two...

Urinary Analysis of 8-Oxoguanine, 8-Oxoguanosine, Fapy-Guanine and 8-Oxo-2′-Deoxyguanosine by High-Performance Liquid Chromatography-Electrospray Tandem Mass Spectrometry as a Measure of Oxidative Stress

Malayappan, Bhaskar, Garrett, Timothy J., Segal, Mark, Leeuwenburgh, Christiaan

05 October 2007

A sensitive and specific assay aimed at measuring the oxidized nucleic acids, 8-oxoguanine (8-oxoGua), fapy-guanine (Fapy-Gua), 8-oxoguanosine (8-oxoGuo), 8-oxo-2′-deoxyguanosine (8-oxodG) has been developed by coupling reversed phase liquid chromatography (HPLC) with electrospray tandem mass spectrometry detection (MS/MS) and isotope dilution. The HPLC-MS/MS approach with multiple reaction monitoring (MRM) allowed for the sensitive determination of 8-oxoGua, Fapy-Gua, 8-oxoGuo, and 8-oxodG in human urine samples. There is no sample preparation needed except for the addition of buffer and 13C- and 15N-labeled internal standards to the urine prior to sample injection into the HPLC-MS/MS system. This method was tested in urine samples from non-smokers, smokers, non-smokers with chronic kidney disease (CKD) and smokers with CKD, to assess the level of oxidative damage to nucleic acids. Markers of both RNA and DNA damage were significantly increased in the smokers with and without CKD compared to their respective control subjects. These findings suggest that a highly specific and sensitive analytical method such as isotope dilution HPLC-MS/MS may represent a valuable tool for the measurement of oxidative stress in human subjects.

8-Oxo-2′-deoxyguanosine (8-oxodG)

8-Oxoguanine (8-oxoGua)

8-Oxoguanosine (8-oxoGuo)

DNA biomarkers

Fapy-guanine (Fapy-Gua)

HPLC-tandem mass spectrometry

nucleic acids

oxidative stress

renal disease

The effect of eicosapentaenoic acid on brain and platelet produced bioactive lipid mediators. The effect of eicosapentaenoic acid, docosapentaenoic acid and other polyunsaturated fatty acids on the eicosanoids and endocannabinoids produced by rat brain and human platelets using electrospray ionisation tandem mass spectrometry-based analysis.

Mir, Adnan A.

January 2009

Eicosapentaenoic acid (EPA) is a polyunsaturated fatty acid (PUFA) with neuroprotective and cardioprotective properties. It is thought that some of the actions of EPA may be attributed to its elongated metabolite, the PUFA docosapentaenoic acid (DPA). Docosahexaenoic acid (DHA) and arachidonic acid (AA) are bioactive PUFA ubiquitously expressed in neural tissues. EPA and AA can be converted by cyclooxygenase (COX) to prostanoids and by lipoxygenase (LOX) to hydroxy fatty acids. PUFA can also be converted to ethanolamides in the brain. These mediators are involved in physiological and pathological processes in many bodily systems. The purpose of this study was to examine the production of eicosanoids, hydroxy fatty acids and fatty acid ethanolamides in young and aged rat brain following EPA or DPA enriched diets. The effects of specific PUFA on human platelet eicosanoid production were also investigated as these mediators play a role in adhesion and aggregation. Liquid chromatography coupled to tandem mass spectrometry (LC/ESI-MS/MS) assays were developed and used to measure lipid mediators in rat brain and human platelets. Ageing in rat brain was accompanied with several changes in the prostanoid and hydroxy fatty acid profiles. Supplementing the diet with EPA or DPA at a daily dose of 200 mg/kg for 8 weeks prevented these changes and decreased levels of PGE2. DPA changed the profile of hydroxy fatty acids synthesised in the brain tissue of young animals. This study has shown that levels of eicosapentaenoylethanolamide (EPA-EA) increase in the brain as a result of ageing and that this is accompanied by an increase in levels of anandamide. Feeding aged animals EPA or DPA further increased the levels of EPA-EA but prevented any change in the level of anandamide. Niacin is used to treat hypercholesterolaemia although it is associated with an unpleasant PGD2 mediated skin flush. This exploratory study has shown that human platelets treated with niacin did not show any changes in their prostanoid and hydroxy fatty acid profiles. Platelets treated with EPA showed increased production of TXB3 and 12-HEPE. Niacin augmented the effects of EPA on human platelet mediator synthesis. Overall, this study has demonstrated that EPA can change brain and platelet lipid mediator synthesis and has provided evidence that could explain some of the neuroprotective and cardioprotective actions of this PUFA.

Eicosapentaenoic acid (EPA)

Docosapentaenoic acid (DPA)

Endocannabinoids

Eicosanoids

Brain

Platelets

Polyunsaturated fatty acid (PUFA)

Docosahexaenoic acid (DHA)

Arachidonic acid (AA)

Eicosapentaenoylethanolamide (EPA-EA)

Anandamide

Neuroprotective action

Cardioprotective action

Studies on Bioactive Lipid Mediators Involved in Brain Function and Neurodegenerative Disorders. The effect of ¿-3PUFA supplementation and lithium treatment on rat brain sphingomyelin species and endocannabinoids formation; changes in oxysterol profiles in blood of ALS patients and animal models of ALS.

Drbal, Abed Alnaser A.A.

January 2013

Lipids are important for structural and physiological functions of neuronal cell membranes. They exhibit a range of biological effects many are bioactive lipid mediators derived from polyunsaturated fatty acids such as sphingolipids, fatty acid ethanolamides (FA-EA) and endocannabinoids (EC). These lipid mediators and oxysterols elicit potent bioactive functions in many physiological and pathological processes of the brain and neuronal tissues. They have been investigated for biomarker discovery of ageing, neuroinflammation and neurodegenerative disorders. The n-3 fatty acids EPA and DPA are thought to exhibit a range of neuroprotective effects many of which are mediated through production of such lipid mediators. The aims of this study were to evaluate the effects of n-3 EPA and n-3 DPA supplementation on RBC membranes and in this way assess dietary compliance and to investigate brain sphingomyelin species of adult and aged rats supplemented with n-3 EPA and n-3 DPA to evaluate the effects and benefits on age-related changes in the brain. Furthermore, to study the effects of lithium on the brain FA-EAs and ECs to further understand the neuroprotective effects of lithium neuroprotective action on neuroinflammation as induced by LPS. Finally to examine if circulating oxysterols are linked to the prevalence of ALS and whether RBC fatty acids are markers of this action in relation to age and disease stages. These analytes were extracted from tissue samples and analysed with GC, LC/ESI-MS/MS and GC-MS. It was found that aged rats exhibited a significant increase in brain AA and decrease in ¿n-3 and ¿n-6 PUFAs when compared to adult animals. The observed increase of brain AA was reversed following n-3 EPA and n-3 DPA supplementation. Sphingomyelin was significantly increased when aged animals were supplemented with n-3 DPA. LPS treatment following lithium supplementation increased LA-EA and ALA-EA, while it decreased DHA-EA. Both oxysterols 24-OH and 27-OH increased in ALS patients and SOD1-mice. Eicosadienoic acid was different in ASL-patients compared to aged SOD1-mice. These studies demonstrated that dietary intake of n-3 EPA and n-3DPA significantly altered RBC fatty acids and sphingolipids in rat brain. They suggest that n-3 DPA can be a potential storage form for EPA, as shown by retro-conversion of n-3 DPA into EPA in erythrocyte membranes, ensuring supply of n-3 EPA. Also, n-3 EPA and n-3 DPA supplementation can contribute to an increase in brain sphingomyelin species with implications for age effects and regulation of brain development. Effects of lithium highlight novel anti-neuroinflammatory treatment pathways. Both 24-hydroxycholesterol and eicosadienoic acid may be used as biomarkers in ALS thereby possibly helping to manage the progressive stages of disease. / Libyan Government

Eicosapentaenoic acid,

Docosapentaenoic acid

Sphingomyelin

Lithium chloride

Lipopolysaccharide

Tandem mass spectrometry

Oxysterols

Amyotrophic Lateral Sclerosis

Gas chromatography

SOD1-mice

Bioactive lipid mediators

Neuronal cell membranes

Amyotrophic lateral sclerosis (ALS)

Motor neurone disease

Neurodegenerative disorders

Brain ageing

Simultaneous lipidomic analysis of three families of bioactive lipid mediators leukotrienes, resolvins, protectins and related hydroxy-fatty acids by liquid chromatography/electrospray tandem mass spectrometry.

Masoodi, Mojgan, Mir, Adnan A., Petasis, N.A., Serhan, S.N., Nicolaou, Anna

January 2008

No / Bioactive lipid mediators derived from polyunsaturated fatty acids (PUFA) and exhibit a range of tissue and cell-specific activities in many physiological and pathological processes. Electrospray tandem mass spectrometry coupled to liquid chromatography (LC/ESI-MS/MS) is a sensitive, versatile analytical methodology for the qualitative and quantitative analysis of lipid mediators. Here we present an LC/ESI-MS/MS assay for the simultaneous analysis of twenty mono- and poly-hydroxy fatty acid derivatives of linoleic, arachidonic, eicosapentaenoic and docosahexaenoic acids. The assay was linear over the concentration range 1-100 pg/¿L, whilst the limits of detection and quantitation were 10-20 and 20-50 pg respectively. The recovery of the extraction methodology varied from 76-122% depending on the metabolite. This system is useful for profiling a range of biochemically-related potent mediators including the newly discovered resolvins and protectins, and their precursor hydroxy-eicosapentaenoic and hydroxy-docosahexaenoic acids, and, consequently, advance our understanding of the role of PUFA in health and disease. / Wellcome Trust, British Heart Foundation

Hydroxy fatty acids

Eicosanoids

Arachidonic Acid

Eicosapentaenoic Acid

Resolvins

Protectin

Docosahexaenoic acid

Polyunsaturated fatty acids (PUFA)

Lipid mediators

Archaeological, radiological, and biological evidence offer insight into Inca child sacrifice

Wilson, Andrew S., Brown, Emma, Villa, C., Lynnerup, N., Healey, Andrew R., Ceruti, M.C., Reinhard, J., Previgliano, C.H., Araoz, F.A., Diez, J.G., Taylor, Timothy F.

January 2013

No / Examination of three frozen bodies, a 13-y-old girl and a girl and boy aged 4 to 5 y, separately entombed near the Andean summit of Volcan Llullaillaco, Argentina, sheds new light on human sacrifice as a central part of the Imperial Inca capacocha rite, described by chroniclers writing after the Spanish conquest. The high-resolution diachronic data presented here, obtained directly from scalp hair, implies escalating coca and alcohol ingestion in the lead-up to death. These data, combined with archaeological and radiological evidence, deepen our understanding of the circumstances and context of final placement on the mountain top. We argue that the individuals were treated differently according to their age, status, and ritual role. Finally, we relate our findings to questions of consent, coercion, and/or compliance, and the controversial issues of ideological justification and strategies of social control and political legitimation pursued by the expansionist Inca state before European contact.

Adolescent

Age factors

Archaeology

Argentina

Burial

Ceremonial behaviour

Child

Chromatography

Coca

Ethanol

Female

Hair

History

Humans

Indians

South America

Male

Mummies

Radiography

Tandem Mass Spectrometry

Tomography

X-Ray

REF 2014

Développement de techniques analytiques pour la détermination des agents anti-infectieux dans les eaux environnementales

Segura, Pedro A.

08 1900

Les agents anti-infectieux sont utilisés pour traiter ou prévenir les infections chez les humains, les animaux, les insectes et les plantes. L’apparition de traces de ces substances dans les eaux usées, les eaux naturelles et même l’eau potable dans plusieurs pays du monde soulève l’inquiétude de la communauté scientifique surtout à cause de leur activité biologique. Le but de ces travaux de recherche a été d’étudier la présence d’anti-infectieux dans les eaux environnementales contaminées (c.-à-d. eaux usées, eaux naturelles et eau potable) ainsi que de développer de nouvelles méthodes analytiques capables de quantifier et confirmer leur présence dans ces matrices. Une méta-analyse sur l’occurrence des anti-infectieux dans les eaux environnementales contaminées a démontré qu’au moins 68 composés et 10 de leurs produits de transformation ont été quantifiés à ce jour. Les concentrations environnementales varient entre 0.1 ng/L et 1 mg/L, selon le composé, la matrice et la source de contamination. D’après cette étude, les effets nuisibles des anti-infectieux sur le biote aquatique sont possibles et ces substances peuvent aussi avoir un effet indirect sur la santé humaine à cause de sa possible contribution à la dissémination de la résistance aux anti-infecteiux chez les bactéries. Les premiers tests préliminaires de développement d’une méthode de détermination des anti-infectieux dans les eaux usées ont montré les difficultés à surmonter lors de l’extraction sur phase solide (SPE) ainsi que l’importance de la sélectivité du détecteur. On a décrit une nouvelle méthode de quantification des anti-infectieux utilisant la SPE en tandem dans le mode manuel et la chromatographie liquide couplée à la spectrométrie de masse en tandem (LC-MS/MS). Les six anti-infectieux ciblés (sulfaméthoxazole, triméthoprime, ciprofloxacin, levofloxacin, clarithromycin et azithromycin) ont été quantifiés à des concentrations entre 39 et 276 ng/L dans les échantillons d’affluent et d’effluent provenant d’une station d’épuration appliquant un traitement primaire et physico- chimique. Les concentrations retrouvées dans les effluents indiquent que la masse moyenne totale de ces substances, déversées hebdomadairement dans le fleuve St. Laurent, était de ~ 2 kg. En vue de réduire le temps total d’analyse et simplifier les manipulations, on a travaillé sur une nouvelle méthode de SPE couplée-LC-MS/MS. Cette méthode a utilisé une technique de permutation de colonnes pour préconcentrer 1.00 mL d’échantillon dans une colonne de SPE couplée. La performance analytique de la méthode a permis la quantification des six anti-infectieux dans les eaux usées municipales et les limites de détection étaient du même ordre de grandeur (13-60 ng/L) que les méthodes basées sur la SPE manuelle. Ensuite, l’application des colonnes de SPE couplée de chromatographie à débit turbulent pour la préconcentration de six anti-infectieux dans les eaux usées a été explorée pour diminuer les effets de matrice. Les résultats obtenus ont indiqué que ces colonnes sont une solution de réchange intéressante aux colonnes de SPE couplée traditionnelles. Finalement, en vue de permettre l’analyse des anti-infectieux dans les eaux de surface et l’eau potable, une méthode SPE couplée-LC-MS/MS utilisant des injections de grand volume (10 mL) a été développée. Le volume de fuite de plusieurs colonnes de SPE couplée a été estimé et la colonne ayant la meilleure rétention a été choisie. Les limites de détection et de confirmation de la méthode ont été entre 1 à 6 ng/L. L’analyse des échantillons réels a démontré que la concentration des trois anti-infectieux ciblés (sulfaméthoxazole, triméthoprime et clarithromycine) était au dessous de la limite de détection de la méthode. La mesure des masses exactes par spectrométrie de masse à temps d’envol et les spectres des ions produits utilisant une pente d’énergie de collision inverse dans un spectromètre de masse à triple quadripôle ont été explorés comme des méthodes de confirmation possibles. / Anti-infectives are used to treat or prevent infections in humans, animals, insects and plants. The occurrence of traces of these substances in wastewaters, natural waters and even drinking water has caused concern among the scientific community especially because of their biological activiy. The goal of this research was to study the occurrence of anti-infectives in contaminated environmental waters (wastewaters, natural waters, and drinking water) and to develop new analytical methods able to quantitate and confirm their presence in these matrices. A meta-analysis on the occurrence of anti-infectives in contaminated environmental waters demonstrated that at least 68 parent compounds and 10 transformation products have been quantified to date. Environmental concentrations vary between 0.1 ng/L and 1 mg/L depending on the compound, the matrix and the source of contamination. According to this study, detrimental effects of anti-infectives on aquatic biota are possible and these substances could also affect indirectly human health because of their possible contribution to the dissemination of antibiotic resistance in bacteria. Preliminary tests on the development of a method of determination of anti-infectives in wastewaters showed the main difficulties to overcome during solid-phase extraction (SPE) as well as the importance of the detector selectivity. A novel method of determination of anti-infectives was described using off-line tandem SPE and liquid chromatography-tandem mass spectrometry (LC-MS/MS). Six target anti-infectives (sulfamethoxazole, trimethoprim, ciprofloxacin, levofloxacin, clarithromycin and azithromycine) were quantitated at concentrations between 39 and 276 ng/L in samples of influent and effluent collected from a primary and physico-chemical wastewater treatement plant. Reported effluent concentrations indicate that the mean mass of these substances discharged daily in the St. Lawrence River was ~ 2 kg. In order to reduce total analysis time and simplify sample preparation, a new on-line SPE-LC-MS/MS was presented. This method used a column-switching technique to preconcentrate 1.00 mL of sample in an on-line SPE column. Method analytical performance allowed the quantitation of six anti-infectives in municipal wastewaters and limits of detection were of the same magnitude (13-60 ng/L) than methods based in offline SPE. Next, the application of turbulent flow chromatography on-line SPE columns for the preconcentration of six anti-infectives in wastewaters was explored. Results showed that these columns are an interesting alternative to traditional on-line SPE columns. Finally, in order to allow analysis of anti-infectives in surface and drinking water, we developed an on-line SPE-LC-MS/MS method using large-volume injections (10 mL). Breakthrough volumes of several on-line SPE columns were estimated and the column having the best retention, Strata-X, was chosen. Method detection and confirmation limits were between 1 and 6 ng/L. Analysis of real samples indicated that the concentration of the three target anti-infectives (sulfamethoxazole, trimethoprim and clarithromycin) was lower that the method detection limits. Accurate mass measurement by time-of-flight mass spectrometry and product ion spectra obtained by a reversed-energy ramp in a triple quadrupole mass spectrometer were explored as alternative confirmation methods.

Anti-infectieux

Pharmaceutiques

Eaux usées

Eau de surface

Eau potable

Extraction sur phase solide

Chromatographie liquide

Spectrométrie de masse en tandem

Antibiotiques

Analyse de traces

Anti-infectives

Pharmaceuticals

Drinking water

Surface water

Solid-phase extraction

Tandem mass spectrometry

Liquid chromatography

Antibiotics

Wastewaters

Trace analysis

Establishment, validation and application of immunological and LC-MS/MS-based detection methods to study the role of human aromatic L-amino acid decarboxylase as an enzyme potentially involved in thyronamine biosynthesis

Höfig, Carolin

18 December 2012

Thyronamine (TAM) sind eine neue Molekülklasse, die endokrinologische und metabolische Prozesse miteinander vereinen. Der biologisch aktive Metabolit 3-Iod-L-Thyronamin (3-T1AM) wird durch eine kombinierte Deiodierung und Decarboxylierung von Schilddrüsenhormonen (TH) gebildet. Existierende Methoden zum Nachweis und zur Quantifizierung von 3-T1AM im menschlichen Serum sind immer noch umstritten. Auch die an der Biosynthese vermutlich beteiligte TH-Decarboxylase konnte noch nicht identifiziert werden. Für die Identifizierung und Quantifizierung von TH und TAM Profilen wurde die Flüssigchromatographie-Tandem-Massenspektrometrie (LC-MS/MS) verwendet. In der bisherigen präanalytischen Aufarbeitung liefern weder Flüssig-Flüssig- noch Festphasenextraktionen reproduzierbare Ergebnisse des 3-T1AM-Gehalts im Serum. Mit der Entwicklung eines spezifischen Extraktionsverfahrens und nachfolgender Detektion mittels LC-MS/MS gelang der gleichzeitige Nachweis der häufigsten TH im humanen Serum. Parallel dazu wurden monoklonale Antikörper gegen 3-T1AM entwickelt, auf deren Basis ein quantitativer 3-T1AM Chemilumineszenz-Immunoassay entstand. Ergebnisse aus klinischen Kollektiven zeigen, dass 3-T1AM im Serum im nM Konzentrationsbereich vorkommt und dass 3-T1AM bei Patienten außerhalb der Schilddrüse produziert wird. Viele Forscher gehen davon aus, dass die aromatische L-Aminosäure Decarboxylase (AADC) die Synthese von TAM über Decarboxylierung von TH katalysiert. Diese Hypothese wurde durch Inkubation von rekombinanter humaner AADC mit TH getestet. In keinem der Experimente konnte AADC die Decarboxylierung von TH katalysieren. Zusammenfassend ist die Bestimmung von 3-T1AM im Serum mittels LC-MS/MS aufgrund der nicht reproduzierbaren präanalytischen Probenaufbereitung problematisch. In dieser Arbeit wird der erste MAb-basierte 3-T1AM assay vorgestellt, der 3-T1AM zuverlässig in humanem Serum quantifiziert. Die AADC ist wahrscheinlich nicht an der Biosynthese von TAM beteiligt. / Thyronamines (TAM) are a new class of molecules linking endocrinology and metabolism. Combined deiodination and decarboxylation of thyroid hormones (TH) generates a biologically active ‘cooling’ metabolite, 3-iodo-L-thyronamine (3-T1AM).. It remains controversial, which methods are able or not to reliably detect 3-T1AM in human serum, and the presumed TH decarboxylase is still elusive. Liquid chromatography-tandem mass spectrometry (LC-MS/MS) was used for the simultane-ous identification and quantification of TH and TAM profiles in biological samples. Several preanalytical methods were tested for complete extraction of 3-T1AM in human serum. Thus far, neither liquid-liquid nor solid-phase extraction methods allowed reproducible extraction of 3-T1AM from human serum samples in the preanalytical sample workup. Nevertheless, a rapid and sensitive extraction procedure was developed for detection of the major TH by LC-MS/MS in a single human serum sample. In parallel, monoclonal antibodies (MAb) targeting 3-T1AM were developed and characterized, and a highly specific quantitative 3-T1AM MAb-based chemiluminescence immunoassay was developed. Studies in clinical cohorts provide evidence that 3-T1AM is present in human serum in the nM concentration range and that 3-T1AM is produced extrathyroidally. Many researchers have reasoned that the aromatic L-amino acid decarboxylase (AADC) mediates TAM synthesis via decarboxylation of TH. This hypothesis was tested by incubating recombinant human AADC with several TH. In all tested conditions, AADC failed to catalyze the decarboxylation of TH. These in vitro observations are supported by the finding that 3-T1AM is also present in plasma samples of patients with AADC deficiency. In summary, 3-T1AM detection in serum using LC-MS/MS encounters preanalytical problems. The first MAb-based 3-T1AM CLIA is presented, which reliably quantifies 3-T1AM in human serum. AADC is likely not involved in TAM biosynthesis.

Schilddrüsenhormonmetabolismus

Thyronamine

3-Iod-L-thyronamin

Thyroxin

Monoclonaler Antikörper

Chemilumineszenz-Immunoassay

Aromatische L- Aminosäure Decarboxylase

monoclonal antibody

thyroid hormone metabolism

Thyronamines

3-iodo-L-thyronamine

thyroxine

chemiluminescent immunoassay

aromatic L-amino acid decarboxylase

570 Biowissenschaften, Biologie

32 Biologie

WD 5802

ddc:570

Desenvolvimento de métodos por cromatografia líquida acoplada à espectrometria de massas em tandem para análises de fármacos (LC-MS/MS no modo column switching com capilar monolítico de sílica híbrida), aminoácidos e neurotransmissores (HILIC-MS/MS) em amostras de plasma de pacientes esquizofrênicos. / Development of methods for liquid chromatography coupled to tandem mass spectrometry for drug analysis (LC-MS/MS in column switching mode with monolithic capillary hybrid silica), amino acids and neurotransmitters (HILIC-MS/MS) in plasma samples of schizophrenic patients.

Domingues, Diego Soares

26 August 2015

A esquizofrenia é um transtorno neuropsiquiátrico crônico que afeta aproximadamente 1% da população mundial. As teorias neurobiológicas descrevem que a esquizofrenia é essencialmente causada por alterações bioquímicas e estruturais do cérebro, devido às disfunções nos sistemas glutamatérgico, dopaminérgico e serotoninérgico. Desta forma, a determinação das concentrações de aminoácidos e neurotransmissores em amostras de plasma de pacientes esquizofrênicos pode auxiliar na avaliação da eficácia da terapia. Além dos antipsicóticos, medicação de primeira linha no tratamento inicial da esquizofrenia, a maioria dos pacientes também faz uso concomitante de outras classes de fármacos, tais como antidepressivos, anticonvulsivantes e ansiolíticos para minimizar os sintomas associados a esta doença. Nesta tese, um método empregando a precipitação de proteínas (PPT) e a cromatografia líquida por interação hidrofílica acoplada à espectrometria de massas em tandem (HILIC-MS/MS) foi adequadamente desenvolvido e validado para a determinação de aminoácidos (aspartato, serina, glicina, alanina, metionina, leucina, tirosina e triptofano) e neurotransmissores (glutamato e ácido -aminobutírico) em amostras de plasma de 35 pacientes esquizofrênicos em tratamento com clozapina (27 pacientes) e olanzapina (8 pacientes) para avaliar a eficácia do tratamento, tendo como controle 38 voluntários sadios. O método HILIC-MS/MS apresentou linearidade do LIQ (9,7 pmol mL-1 - 13,3 nmol mL-1) ao LSQ (19,4 nmol mL-1 - 800 nmol mL-1), tempo de análise de 3,0 min, exatidão com EPR de -18 a 19% e precisão com CV de 0,1 a 16% (LIQ). A análise de variância (ANOVA), seguida por teste post-hoc de Duncan, revelou que os níveis médios plasmáticos (nmol mL-1) de metionina (F2,70 = 3,14, p = 0,049) de pacientes esquizofrênicos em tratamento com olanzapina foram significativamente mais elevados, quando comparados aos valores obtidos com o grupo controle (voluntários saudáveis), já o nível de glutamato em pacientes esquizofrênicos em tratamento com clozapina apresentaram tendência a valores mais altos (F2.70 = 2,50, p = 0,090). Já os métodos, PPT/LC-MS/MS e LC-MS/MS no modo column switching utilizando uma coluna monolítica de sílica híbrida com grupos cianopropil na primeira dimensão, foram desenvolvidos e validados para a determinação dos antipsicóticos (olanzapina, quetiapina, clozapina, haloperidol e clorpromazina), antidepressivos (mirtazapina, paroxetina, citalopram, sertralina, imipramina, clomipramina e fluoxetina), anticonvulsivantes (carbamazepina e lamotrigina), e ansiolíticos (diazepam e clonazepam) em amostras de plasma de pacientes esquizofrênicos para fins de monitorização terapêutica. O método PPT/LC-MS/MS apresentou linearidade do LIQ (0,2 ng mL-1 - 5,0 ng mL-1) ao LSQ (40,5 ng mL-1 - 10,5 g mL-1), exatidão com EPR de -9,7 a 8,0%, e precisão com CV de 0,1 a 12%. Já o método LC-MS/MS no modo column switching apresentou linearidade do LIQ (63,0 pg mL-1 - 1250,0 pg mL-1) ao LSQ (40,5 ng mL-1 - 10,5 g mL-1), exatidão com EPR de -14 a 12% e precisão com CV de 0,6 a 6,5%. A pré-concentração seletiva dos fármacos na coluna monolítica com grupos cianopropil incorporados e a remoção dos componentes endógenos da amostra biológica, antes da separação cromatográfica, favoreceram a seletividade e detectabilidade do método LC-MS/MS no modo column switching. Este método quando comparado ao de referência PPT/LC-MS/MS, através da análise de 10 amostras de pacientes esquizofrênicos, não apresentou diferença significativa (teste t) entre as concentrações plasmáticas, podendo ser aplicado na monitorização terapêutica. Além deste fato, este método automatizado favoreceu a precisão, a exatidão e a freqüência analítica. / Schizophrenia is a chronic neuropsychiatric disorder that affects approximately 1% of the world population. According to neurobiological theories, schizophrenia stems from biochemical and structural alterations in the brain due to dysfunction in the glutamatergic, dopaminergic, and serotonergic systems. Determining the concentrations of amino acids and neurotransmitters in plasma samples from schizophrenic patients may assist evaluation of therapy effectiveness. In addition to antipsychotics (the first-line drug in the initial treatment of schizophrenia), most patients concomitantly use other classes of drugs such as antidepressants, anticonvulsants, and anxiolytics to minimize the symptoms associated with this disease. To evaluate treatment efficacy, in this thesis a method based on protein precipitation (PPT) and hydrophilic interaction liquid chromatography coupled to tandem mass spectrometry (HILIC-MS/MS) has been properly developed and validated to determine amino acids (aspartate, serine, glycine, alanine, methionine, leucine, tyrosine, and tryptophan) and neurotransmitters (glutamate and -aminobutyric acid) in plasma samples obtained from 35 schizophrenia patients treated with clozapine (27 patients) or olanzapine (8 patients); 38 healthy volunteers served as controls. The HILIC-MS/MS method was linear for concentrations ranging from the LLOQ (9.7 pmol mL-1 - 13.3 nmol mL-1) to the ULOQ (19.4 nmol mL-1 - 800 nmol mL-1). The analysis time was 3.0 min. In the case of accuracy, RSE ranged from -18 to 19%. As for precision, CV lay between 0.1 and 16% (LLOQ). Analysis of variance (ANOVA) followed by post-hoc Duncan showed that the average methionine serum levels (nmol mL-1) (F2.70 = 3.14, p = 0.049) in schizophrenic patients treated with olanzapine were significantly higher as compared with the control group (healthy volunteers). The glutamate level in schizophrenic patients treated with clozapine tended to higher values (F2.70 = 2.50, p = 0.090). Concerning the analytical methods, PPT/LC-MS/MS and LC-MS/MS operating in the column-switching mode were developed and validated to determine antipsychotic (olanzapine, quetiapine, clozapine, haloperidol, and chlorpromazine), antidepressants (mirtazapine, paroxetine, citalopram, sertraline, imipramine, clomipramine, and fluoxetine), anticonvulsants (carbamazepine and lamotrigine), and anxiolytics (diazepam and clonazepam) in plasma samples taken from schizophrenic patients for therapeutic drug monitoring. A monolithic hybrid column containing silica with cyanopropyl groups in the first dimension was employed. The PPT/LC-MS/MS method was linear from the LLOQ (0.2 ng mL-1 - 5.0 ng mL-1) to the ULOQ (40.5 ng mL-1 - 10.5 g mL-1). In the case of accuracy, RSE ranged from -9.7 to 8.0%; as for precision, CV lay between 0.1 and 12%. LC-MS/MS in the column-switching mode was linear from the LLOQ (63.0 pg mL-1 - 1250.0 pg mL-1) to the ULOQ (40.5 ng mL-1 - 10.5 g mL-1). RSE ranged from -14 to 12%; CV lay between 0.6 and 6.5%. The drugs were selectively pre-concentrated in the monolithic column containing silica incorporated with cyanopropyl groups. For the LC-MS/MS method operating in the column-switching mode, the endogenous components of the biological sample of the LC-MS/MS method were removed before analysis. Analysis of 10 plasma samples obtained from schizophrenic patients did not reveal any significant differences (t test) between the LC-MS/MS method and the reference PPT/LC-MS/MS method. Therefore, LC-MS/MS can be applied in therapeutic monitoring, with the advantage that this method offers improved precision, accuracy, and analytical frequency.

Amino acids

Aminoácidos

amostras de plasma

antipsicóticos

column switching

column switching

drugs

esquizofrenia

hybrid monolith

hydrophilic interaction

interação hidrofílica

monitorização terapêutica

monolito híbrido

neurotransmissores

neurotransmitters

plasma samples

schizophrenia

therapeutic drug monitoring

Aspects analytiques, cliniques et médico-judiciaires des nouvelles substances psychoactives / Analytical, clinical and forensic aspects of new psychoactive substances

Ameline, Alice

14 June 2019

En raison de la diffusion incontrôlée sur le e-commerce, la sécurité et l’alternative légale aux stupéfiants habituels, les nouvelles substances psychoactives (NPS), d’apparition récente (2008), sont au cœur des phénomènes récents d’addiction et de décès mal expliqués. Au-delà des différents défis dans nos sociétés (prévention, législation), la capacité d’identifier les NPS dans des échantillons biologiques pour caractériser leur utilisation, présente de nombreux challenges analytiques. L’objectif principal de cette thèse a été de collecter des échantillons biologiques (sang, urine, cheveux) provenant de cas d’exposition à des NPS et d’y caractériser les substances présentes à l’aide de méthodes analytiques originales, dans le but d’enrichir les librairies de spectres de masse et d’améliorer, en conséquence, la détection de la consommation de NPS. En particulier, il s’agissait d’augmenter la fenêtre de détection de la prise de NPS en se focalisant sur les métabolites qui sont, le plus souvent, les produits majeurs d’élimination. Le développement analytique, par chromatographie liquide ultra haute performance couplée à la spectrométrie de masse en tandem (UHPLC-MS/MS), a demandé plusieurs mois d’optimisation afin d’obtenir une méthode robuste, exhaustive et sensible. Actuellement, la librairie de spectres MS comporte 114 NPS et est mise à jour régulièrement. A la suite de ce développement, ma thèse a porté sur l’étude de cas d’intoxication vus au service des urgences du CHU de Strasbourg, mais aussi en médecine légale, avec des situations de décès et d’identification de produits inconnus provenant de saisies (poudres et cristaux). Il a également été nécessaire de développer des outils analytiques complémentaires, tels que la caractérisation de métabolite(s) par étude sur microsomes hépatiques humains (HLMs), et l’utilisation de la spectroscopie par résonance magnétique nucléaire (RMN) afin d’identifier avec certitude certains composés et de déterminer leur degré de pureté. Les outils analytiques développés et la stratégie mise en place ont permis la rédaction de 18 publications, ainsi que l’agencement de nombreuses collaborations. / Due to the uncontrolled spread on the Internet and their legal alternative to usual drugs, the new psychoactive substances (NPS), recently appeared (2008), are at the center of recent phenomena of addiction and badly explained deaths. Beyond different challenges in our societies (prevention, legislation), the ability to identify NPS in biological samples, in order to characterize their use, presents many analytical challenges. The main objective of this thesis was to collect biological samples (blood, urine, hair) from cases of exposure to NPS and to characterize the substances present using original analytical methods, in order to enlarge the libraries of mass spectra and improve, as a result, the detection of NPS consumption. In particular, it was intended to increase the detection sensitivity of NPS intake by focusing on the metabolites that are often the major products of elimination. This analytical development, by ultra-high liquid chromatography coupled with tandem mass spectrometry (UHPLC-MS/MS), required several months of optimization in order to obtain a robust, exhaustive and sensitive method. At present, the mass spectra database has 114 NPS and is regularly updated. Thereafter, ma thesis focused on the study of cases of intoxication observed in the emergency department of Strasbourg, but also in legal medicine with situations of deaths and identification of unknown products collected from seizures (powders and crystals). It has also been necessary to implement complementary analytical tools, such as the characterization of metabolites by human liver microsomes (HLMs), and the use of nuclear magnetic resonance (NMR) spectroscopy to accurately identify the compounds and establish their purity degrees. The analytical tools developed, and the strategy adopted, allowed the writing of 18 publications, as well as the setting up of numerous collaborations.

Nouvelles substances psychoactives (NPS)

Métabolites

Microsomes hépatiques humains (HLMs)

Résonance magnétique nucléaire (RMN)

Intoxication

Décès

New psychoactive substances (NPS)

Metabolites

Human liver microsomes (HLMs)

Nuclear magnetic resonance (NMR)

Intoxication

Death

615.9

616.86