A aplicabilidade de combinações seletivas de linhagens S. typhimurium na caracterização da mutagenicidade de amostras de ar / The applicability of selective combinations of strains S. typhimurium in the characterization of mutagenicity of airborne samples

Débora Kristina Magalhães Alves

03 October 2011

O material particulado atmosferico é reconhecido como mutagênico. Embora vários compostos já tenham sido identificados nessa matriz, os mesmos não explicam o efeito observado na maioria dos bioensaios realizados. O ensaio de mutagenicidade Salmonella/microssoma tem sido amplamente utilizado para a avaliação de amostras atmosféricas o qual é muito sensível na detecção de vários tipos de mutágenos, pois é realizado com diferentes linhagens de Salmonella typhimurium na presença e ausência de ativação metabólica exógena. O principal objetivo deste trabalho foi verificar a aplicabilidade da utilização de combinações seletivas de linhagens S. typhimurium na caracterização da mutagenicidade de amostras de material particulado total de ar coletado em Limeira, uma cidade do interior do estado de São Paulo sob influência de intenso tráfego, emissões industriais e da agricultura, incluindo o plantio de cana de açúcar. Foram avaliados seis extratos orgânicos obtidos com diclorometano por ultrasonicação, utilizando o método Salmonella/microssoma em microssuspensão na presença e ausência de ativação metabólica (mistura S9) em experimentos de dose-resposta, com quantidade máxima de 50 µg de material orgânico extraído (MOE) por placa. Os pares de linhagens utilizados foram: YG1041/TA98, para verificar a presença de nitrocompostos, como 1- nitropireno e/ou aminas aromáticas; YG5161/TA1538, altamente sensivel aos hidrocarbonetos policíclicos aromáticos (HPA) não substituídos como o benzo[a]pireno (BaP); e YG7108/TA1535, para a indicação de agentes alquilantes. Os resultados indicaram que os compostos que podem melhor explicar os efeitos observados são os nitro e/ou aminas aromáticas e não os HPA não substituídos como o BaP. O par YG7108/TA1535 forneceu respostas negativas para todas as amostras. As combinações seletivas de linhagens S. typhimurium (YG1041/TA98 e YG5161/TA1538) mostraram-se eficientes na caracterização da mutagenicidade de amostras de ar coletadas na cidade de Limeira, podendo ser utilizadas como uma importante ferramenta de auxílio do ensaio Salmonella/microssoma em microssuspensão em estudos de análises quimicas direcionadas pelo efeito biológico (ADEB). As potências mutagênicas observadas com a linhagem TA98 para a cidade de Limeira foram similares aquelas verificadas na Região Metropolitana de São Paulo. A comparação das respostas de mutagenicidade observadas para as amostras analisadas com o perfil de compostos puros, encontrados na literatura, não forneceu candidatos que podem representar a mistura. Mais estudos de mutagenicidade com compostos puros utilizando os pares de linhagens propostos (TA98/YG1041 e TA1538/YG5161) e análises quimicas de extratos fracionados são necessários para verificar se esta abordagem pode ser útil em estudos de ADEB, e consequentemente na descoberta de novos poluentes atmosféricos. / The atmospheric particulate matter is recognized as mutagenic. Although several compounds have been identified in this matrix, they do not explain the observed effect in most bioassays that have been performed. The Salmonella/microsome assay has been widely used for the evaluation of atmospheric samples, The assay is very sensitive in the detection of various types of mutagens, because it is performed with different strains of Salmonella typhimurium in the presence and absence of exogenous metabolic activation. The main objective of this work was to verify the applicability of selective combination of strains in the characterization of mutagenicity of total airborne particulate matter collected in Limeira, a São Paulo State city in a site influenced by heavy traffic, industrial and agricultural emissions, including sugar cane plantations. We tested six extracts obtained with methylene chloride by ultrasonication using the Salmonella/microsome microsuspension protocol in the presence and absence of rat liver S9 in dose response experiments, using 50 µg of extractable organic matter (EOM) as a maximum dose per plate. The following pairs of strains were used: YG1041/TA98, to verify the presence of nitro-compounds, as 1-nitropyrene and/or aromatic amines; YG5161/TA1538, highly sensitive to non-substituted polycyclic aromatic hydrocarbons (PAHs) as benzo[a]pyrene (BaP); and YG7108/TA1535, for the indication of alkylating agents. The results indicated that the compounds that can better explain the observed effect are the nitro and/or aromatic amines and not nonsubstituted PAHs such as BaP. The pair YG7108/TA1535 provided negative responses for all the samples. Selective combinations of S. typhimurium strains (YG1041/TA98 and YG5161/TA1538) proved efficient in the characterization of mutagenicity of airborne samples collected in the city of Limeira and can be used as an important tool for the Salmonella/microsome microsuspension assay in effect directed chemical analysis (EDA) studies. The mutagenic potencies observed with TA98 strain for the city of Limeira were similar to those verified in the Metropolitan Region of São Paulo. The comparison of the observed mutagenicity responses for the samples analyzed with the profiles of pure compounds found in the literature did not provide any candidates that could alone represent the mixture. More mutagenicity studies with pure compounds using the proposed pair of strains (TA98/YG1041 and TA1538/YG5161) along with chemical analysis of fractioned extracts are needed to verify if this approach can be useful in EDA studies, and consequently in the discovery of new air priority pollutants.

Agentes alquilantes

Benzo[a]pireno

HPA

Mutagenicidade do ar

Nitrocompostos

Poluição atmosférica

YG1041

YG5161

YG7108

Airborne particulate matter mutagenicity

Alkylating agents

Atmospheric pollution

Benzo[a]pyrene

Nitro-compounds

PAHs

YG1041

YG5161

YG7108

Dietary exposure to contaminants during pregnancy and fetal growth

Duarte Salles, Talita, 1985-

31 July 2012

Introduction: Prenatal exposure to polycyclic aromatic hydrocarbons (PAH) and to acrylamide has been suggested to reduce fetal growth. The role of diet, the main source of exposure to these compounds in the general population, remains uncertain. This thesis aimed to characterize women’s exposure during pregnancy to dietary acrylamide and the genotoxic PAH benzo(a)pyrene [B(a)P], and to assess the effects of prenatal exposure to these compounds on fetal growth indicators. Methods: This thesis was done within two large European population-based cohort studies conducted in Spain and Norway: the INfancia y Medio Ambiente (INMA; n=657) and The Norwegian Mother and Child Cohort (MoBa; n=50651). Dietary B(a)P and acrylamide intakes were estimated based on information from food frequency questionnaires and the concentrations of these compounds in foods. Results: (i) Smokers had higher dietary intakes of B(a)P and acrylamide compared to non-smokers; (ii) the main predictors of B(a)P intake were shellfish and processed/cured meats while the main predictors of acrylamide intake were snacks, fried potatoes, and crisp bread; (iii) higher prenatal exposure to dietary B(a)P and acrylamide may reduce birth weight and increase the risk of small for gestational age, independently of smoking-related exposure and (iv) stronger effects of dietary B(a)P on fetal growth were observed among women with low vitamin C intake. Conclusions: Dietary B(a)P and acrylamide intakes during pregnancy may impair fetal growth. Therefore, reducing the intake of these compounds from the diet should be recommended in dietary guidelines for pregnant women. Likewise, increasing intakes of fruits and vegetables rich in vitamin C should be recommended given its potential to prevent adverse effects from exposure to such contaminants. / Introducción: La exposición prenatal a los hidrocarburos aromáticos policíclicos (HAP) y a la acrilamida ha sido asociada con la reducción del crecimiento fetal. El papel de la dieta, la principal fuente de exposición a estos compuestos en la población general, sigue siendo incierto. Los objetivos de esta tesis son caracterizar la exposición a través de la dieta a la acrilamida y a los HAP, específicamente el compuesto genotóxico benzo(a)pireno [B(a)P], durante el embarazo, y evaluar los efectos de la exposición prenatal a estos compuestos sobre indicadores del crecimiento fetal. Métodos: Esta tesis se realizó dentro del marco de dos grandes estudios europeos de cohortes de base poblacional realizados en España y Noruega: INfancia y Medio Ambiente (INMA; n=657) y The Norwegian Mother and Child Cohort (MoBa; n=50651). La ingesta de B(a)P y acrilamida fue estimada a partir de información de cuestionarios de frecuencia alimentaria y las concentraciones de estos compuestos en los alimentos. Resultados: (i) Las fumadoras tuvieron mayor ingesta de B(a)P y acrilamida a través de la dieta en comparación con las no fumadoras; (ii) los principales predictores de la ingesta de B(a)P fueron los mariscos y los embutidos, mientras que los principales predictores de la ingesta de acrilamida fueron los aperitivos, las patatas fritas y el pan crujiente; (iii) la exposición prenatal al B(a)P y la acrilamida pueden reducir el peso al nacer y aumentar el riesgo de pequeño para la edad gestacional, independientemente de la exposición relacionada con el tabaco y (iv) los efectos de la ingesta de B(a)P a través de la dieta sobre el crecimiento fetal fueron más fuertes entre las mujeres con baja ingesta de vitamina C. Conclusiones: La ingesta de B(a)P y acrilamida a través de la dieta durante el embarazo, puede perjudicar el crecimiento fetal. Consecuentemente, recomendaciones para la reducción de la ingesta de estos compuestos a través de la dieta deberían ser incluidas en las guías dietéticas para mujeres embarazadas. Asimismo, debería recomendarse un aumento en la ingesta de frutas y verduras con alto contenido en vitamina C por su potencial para prevenir efectos relacionados con la exposición a estos contaminantes.

Diet

Pregnancy

Food contaminants

Benzo(a)pyrene

Acrylamide

Birth weight

Small for gestational age

Epidemiology

Dieta

Embarazo

Contaminantes alimentarios

Benzo(a)pireno

Acrilamida

Peso al nacer

Pequeño por edad gestacional

Epidemiologia

618

Recherche de biomarqueurs d'exposition et d'effet à des cancérigènes de l'environnement par spectrométrie de masse

Ibrahim, Marianne

05 December 2013

Le Benzo(a)pyrène (BaP), appartenant à la famille des hydrocarbures aromatiques polycycliques (HAP) est cancérigène pour l'homme. Nous avons développé une approche protéomique quantitative nanoLC-MS/MS label-free pour identifier des biomarqueurs liés à l'exposition au BaP dans le sécrétome des cellules hépatiques humaines exposées au BaP vs. des cellules non exposées et exposées au Benzo(e)pyrène (BeP). Le BeP, agent non classifié comme cancérigène pour l'homme, est choisi comme contrôle négatif afin de distinguer les protéines spécifiques du BaP de celles des HAP. 847 protéines ont été identifiées et quantifiées, et 55 ont été fortement surexprimées avec un ratio supérieur à 5 : la plupart de ces protéinessurexprimées sont précoces et liées au cancer. Une validation ultérieure de l'expression de ces protéines dans le plasma de la population exposée au BaP aidera dans le développement de biomarqueurs qui permettront d'améliorer la détection précoce, le pronostic et prévention.

Benzo(a)pyrène

Benzo(e)pyrène

Biomarqueurs

Cancer

Sécrétome

Protéomique

Quantification label-free

Spectrométrie de masse

Étude du continuum exposition-effet cancérogène du benzo[a]pyrène

Moreau, Marjory

12 1900

Le benzo[a]pyrène (BaP) est un contaminant environnemental de la famille des hydrocarbures aromatiques polycycliques ayant été classé cancérogène chez l’humain. Cependant, la relation entre l’exposition et les effets est toujours mal documentée. L’objectif de cette thèse était de mieux documenter la relation quantitative entre l’exposition au BaP, l’évolution temporelle des biomarqueurs d’exposition et l’apparition d’altérations biologiques précoces, à partir d’études expérimentales chez le rat. Dans un premier temps, nous avons déterminé l’effet de 4 doses de BaP (0.4, 4, 10 et 40 µmol/kg) sur plusieurs biomarqueurs d’exposition (3- et 7-OHBaP, 4,5- et 7,8-diolBaP, BaPtétrol et 1,6-, 3,6- et 7,8-diones-BaP), les adduits à l’ADN et l’expression de gènes impliqués dans le métabolisme du BaP, la réparation de l’ADN et le stress oxydatif. Le BaP et ses métabolites ont été mesurés dans le sang, les tissus et les excrétas, 8 h et 24 h après l’administration intraveineuse de BaP par chromatographie liquide à ultra haute performance (UHPLC) couplée à la fluorescence. Les adduits à l’ADN ont été quantifiés dans les poumons par immuno-essai en chémoluminescence. L’expression des gènes dans les poumons a été réalisée par PCR quantitative en temps réel (qRT-PCR). Les résultats ont révélé une bonne relation dose-excrétion pour le 3-OHBaP, le 4,5-diolBaP et le 7,8-diolBaP et ils ont également renforcé l’utilité du 4,5-diolBaP comme potentiel biomarqueur du BaP en plus du 3-OHBaP. De plus, l’augmentation dose-dépendante de la formation des adduits et de l’expression de certains gènes impliqués dans le métabolisme et le stress oxydatif a suggéré l’intérêt de ces derniers comme biomarqueurs d’effet précoce. Dans un second temps, nous avons évaluer le profil cinétique des biomarqueurs en lien avec la modulation temporelle de la formation des adduits à l’ADN et de l’expression génique, en utilisant la dose de 40 µmol/kg de BaP telle qu’établie dans l’étude précédente, avec une série de mesures sur une durée de 72 h après l’injection intraveineuse de BaP. Il est apparu que le 3- et le 7-OHBaP ainsi que le 4,5- et le 7,8-diolBaP semblaient être de bons biomarqueurs d'exposition; les hydroxyBaP et diolBaP présentaient des cinétiques différentes, mais tous ces métabolites étaient corrélés de façon significative aux adduits BaPDE dans les poumons. L’expression de certains gènes et l’étude de leur profil cinétique a également permis de faire des liens avec la formation des adduits et de mieux comprendre le métabolisme du BaP. Après ces résultats, il semblait alors logique de s’intéresser à l’effet de la voie d’exposition dans un context d’exposition multiple de la population. Les données mesurées dans le sang et les excréta, après administration de 40 µmol/kg de BaP par voie intraveineuse, intratrachéale, orale, et cutanée, ont encore une fois montré l'intérêt de mesurer plusieurs métabolites pour l’évaluation de l’exposition en raison des différences en fonction de la voie d’administration du composé et des différences dans la cinétique de plusieurs biomarqueurs, notamment entre les hydroxy (3- et 7-OHBaP) et les diols-BaP (4,5- et 7,8-diolBaP). Les résultats suggèrent aussi que la mesure de ratios de concentrations de différents métabolites pourrait aider à indiquer le moment et la principale voie d’exposition. Ces données ont permis une meilleure compréhension du continuum entre l’exposition et les effets. / Benzo(a)pyrene (BaP) is a polycyclic aromatic hydrocarbon that has been classified as carcinogenic to humans. However, the relationship between exposure and effect is still poorly documented. The aim of this thesis was to document the quantitative relationship between exposure to BaP, the temporal evolution of biomarkers of exposure and the appearance of early biological alterations, by conducting experimental studies in rats. First, we determined the effect of four doses of BaP (0.4, 4, 10 and 40 µmol / kg) on several biomarkers of exposure (3- and 7-OHBaP, 4,5- and 7,8 -diolBaP, BaPtetrol and 1,6 -, 3,6 - and 7,8-dione-BaP), on DNA adducts and the expression of genes involved in the metabolism of BaP, DNA repair and oxidative stress. BaP and its metabolites were measured in blood, tissues and excreta, 8 h and 24 h after intravenous administration of BaP by ultra high performance liquid chromatography (UHPLC) coupled to fluorescence. The DNA adducts were quantified in lungs by chemiluminescence immunoassay. Gene expression in lungs was achieved by quantitative real time PCR (qRT-PCR). The results showed a good dose-excretion relationship for 3- OHBaP , 4,5- and 7,8- diolBaP and they also showed the usefulness of 4,5- diolBaP as a potential biomarker of BaP in addition to 3- OHBaP. Furthermore, the dose-dependent increase in the formation of adducts and the expression of certain genes involved in metabolism and oxidative stress highlighted the latter as potentially interesting biomarkers of effect. The following study was designed to evaluate the toxicokinetic profile of biomarkers of exposure related to the temporal modulation of the formation of DNA adducts and gene expression, using a dose of 40 µmol/kg BaP as set out in the previous study, but with regular measurements during the 72-h period following intravenous injection of BaP. It appeared that the 3 - and 7- OHBaP and 4,5 - and 7,8- diolBaP seemed to be good biomarkers of exposure; hydroxyBaPs and diolBaPs exhibited different kinetics but all the metabolites were significantly correlated with BaPDE adducts in the lungs. The expression of genes and the study of their kinetic profile also allowed to assess the relationship with the formation of adducts and better understand the metabolism of BaP. Based on these results, it seemed logical to focus on the effect of the route of exposure. The data measured in the blood and excreta after intravenous, intratracheal, oral, and cutaneous administration of 40 mmol/kg BaP have once again demonstrated the importance of measuring several metabolites due to kinetic differences depending on the route of administration of the compound and among biomarkers, in particular between OHBaPs (3 - and 7 - OHBaP) and diolBaPs (4,5 - and 7,8- diolBaP). Results also suggest that measurements of concentration ratios of different metabolites could help indicate the time and the main route of exposure. Overall, these data allowed a better understanding of the continuum between BaP exposure and early effects.

Benzo[a]pyrène

Métabolisme

Biomarqueurs

Toxicocinétique

Relation dose-effet

Voie d'exposition

Adduits à l'ADN

Expression génique

Benzo[a]pyrene

Metabolism

Biomarkers

Toxicokinetics

Dose-effect relationship

Route of exposure

DNA adducts

Gene expression

Využití buněčné linie BEAS-2B pro analýzu mikrojader v genetické toxikologii / The use of BEAS-2B cell line for micronucleus assay in genetic toxicology

Červená, Tereza

January 2016

This thesis deals with the application of BEAS-2B cell line for micronucleus assay in genetic toxicology. It is divided into two main parts: a) theoretical introduction to the analysis and search for suitable models for testing the impact of air pollution and manufactured nanoparticles, b) practical part that describes the results of micronuclei induction by polycyclic aromatic hydrocarbons (PAHs), extractable organic matter (EOM) from diesel exhaust particles obtained from emissions of three types of fuel and engineered nanoparticles. BEAS-2B cell line is a nonmalignant human model of lung epithelium which seems to be suitable for micronucleus assay. This assay is commonly used for determining the genotoxicity of various substances to wide variety of cell cultures and also in human studies. In this thesis, the following substances were tested: benzo[a]pyrene, 3-nitrobenzanthrone and 1-nitropyrene as carcinogenic PAHs commonly found in polluted air; EOMs from exhaust particles of 100 % diesel fuel, a blend of diesel fuel and 30 % of biodiesel, 100 % biodiesel and two types of engineered nanoparticles (TiO2 and Ag). The cells were treated with the compounds for 28, 48 and 72 hours. The results confirm the suitability of BEAS-2B cell line as a model for testing the genotoxicity of substances under...

Impact de la co-exposition au benzo[a]pyrène et à l'éthanol sur la progression pathologique de la stéatose hépatique / Effect of the co-exposure of benzo[a]pyrene with ethanol on the progression of fatty liver disease

Tête, Arnaud

03 July 2018

La stéatose est la pathologie hépatique la plus répandue dans le monde, touchant environ 25 % de la population générale et jusqu’à 80 % des personnes en surpoids ou obèses. Cette maladie se traduisant par l’enrichissement des hépatocytes en triglycérides, est considérée comme bénigne. Cependant, environ 20 % des personnes atteintes de stéatose développent une stéatohépatite, pathologie caractérisée par une mort cellulaire et une inflammation et représentant un stade favorable au développement du carcinome hépatocellulaire. Les causes et mécanismes impliqués dans la progression de la stéatose vers la stéatohépatite sont encore à préciser. L’obésité, l’exposition aux contaminants environnementaux et la consommation d’alcool sont trois facteurs participant au développement des pathologies hépatiques. Pourtant, l’effet de l’interaction entre ces différents facteurs sur les pathologies hépatiques n’est pas connu. Dans ce contexte, cette thèse a eu pour objectif d’étudier l’impact d’une co-exposition au benzo[a]pyrène (B[a]P), un contaminant carcinogène environnemental, et à l’éthanol, utilisé à de faibles doses, sur les cellules hépatiques WIF-B9, présentant une stéatose préalable. Les résultats obtenus ont permis de démontrer qu’une telle exposition induit une progression de la stéatose hépatique vers un stade apparenté à une stéatohépatite, marquée par une augmentation de la mort cellulaire et de l’inflammation. Nous avons mis en évidence que la mort cellulaire résulterait de l’activation de p53 et d’une peroxydation lipidique. Une activation du récepteur aux hydrocarbures aromatiques et une production de monoxyde d’azote sont à l’origine de ces évènements via une modification du métabolisme de l’éthanol et du B[a]P conduisant à des dommages à l’ADN dépendants de la formation d’anion peroxynitrite. / Steatosis is the most common form of liver disease in the world, affecting around 25 % of the general population and up to 80 % of obese people. The disease is defined by the accumulation of triglycerides in hepatocytes and is generally considered as a benign condition. However, around 20 % of people with steatosis develop steatohepatitis, a disease characterized by cell death and inflammation, a condition that favors the development of hepatocellular carcinoma. The causes and mechanisms involved in the progression from steatosis to steatohepatitis are yet not fully understood. Obesity, exposure to environmental contaminants and alcohol consumption are three major factors contributing to the development of liver diseases. However, is still not yet clear what is the effect of the interaction between these different factors on liver diseases. In this context, the aim of this study was to evaluate the impact of a co-exposure to benzo[a]pyrene (B[a]P), an environmental carcinogenic contaminant, and ethanol, used at low doses, in WIF-B9 hepatic cell line, with a prior steatosis . The results demonstrate that this type of co-exposition induces a progression of hepatic steatosis to a steatohepatitis-like stage, marked by an increased cell death and an inflammation. We have shown that in this condition, cell death results from the activation of p53 and lipid peroxidation. Activation of the aromatic hydrocarbon receptor and production of nitric oxide are the origin of these events by a modification of both ethanol and B[a]P metabolism leading to peroxynitrite-dependent DNA damage.

Maladies non alcooliques du foie

Benzo[a]pyrène

Éthanol

Métabolisme des xénobiotiques

Monoxyde d’azote

P53

Récepteur aux hydrocarbures aromatiques

Non-Alcoholic liver diseases

Benzo[a]pyrene

Ethanol

Xenobiotic metabolism

Nitric oxide

P53

Aromatic hydrocarbon receptor

Development of Chiral/Achiral Analysis Methods using Capillary Electrochromatography and Capillary Electrochromatography Coupled to Mass Spectrometry

Zheng, Jie

29 August 2006

The research presented in this dissertation involves the development of chiral and achiral analysis using capillary electrochromatography (CEC) and CEC coupled to mass spectrometry (CEC-MS). Chapter 1 briefly reviews CEC fundamentals and latest development on chiral CEC and CEC-MS. The CEC-UV enantioseparations for several acidic compounds are described in Chapter 2. The optimum resolutions for these acidic enantiomers are achieved in ion-suppression mode, i.e. with an acidic mobile phase. One of major drawback in coupling CEC with MS is the bubble formation at the column outlet end, resulting in irreproducible retention time and erratic baseline, or even current breakdown. By introducing internal tapered columns, the aforementioned limitations of CEC-MS are successfully overcome in Chapter 3. The CEC-MS enantioseparation of warfarin and coumachlor is carefully investigated and applied to quantify R- and S-warfarin in human plasma. For individual enantiomers, a concentration of 25 ng/mL is detectable. To further improve the robustness of CEC-MS column, a new procedure of fabricating internal tapered columns is reported in Chapter 4. These internal tapered columns demonstrate excellent ruggedness, low background noise, and good compatibility in reversed-phase and polar organic modes of CEC-MS. In chapter 5, the feasibility of using internal tapered columns packed with vancomycin chiral stationary phase (CSP) is explored for simultaneous enantioseparation of eight â-blockers using CEC-MS. After a careful optimization of the mobile phase composition, sheath liquid and spray chamber parameter, 15 out of 16 enantiomers could be simultaneously resolved with excellent efficiency and detection sensitivity. The synthesis and characterization of sulfated and sulfonated cellulose phenylcarbamate CSPs is described in Chapter 6. The use of these CSPs, especially the sulfonated one, significantly enhances the EOF profile and sample throughput but maintain high enantiomeric resolving power under various modes of CEC and CEC-MS. By combining CEC and atmospheric pressure photo-ionization (APPI) MS, Chapter 7 demonstrates the separation and detection of mono-methylated benzo[a]pyrene (MBAP) isomers with ~100 times enhancement on detection sensitivity than CEC-UV. In Appedix 2, monolithic columns are synthesized through photopolymerized sol-gel approach and utilized for CEC and CEC-APPI-MS of polyaromatic hydrocarbons, and alkyl phenyl ketones.

Atmospheric Pressure Photoionization

Monomethylated Benzo[a]pyrene

Mass Spectrometry

Chiral Stationary Phase

Chiral Separations

Capillary Electrochromatography (CEC)

Chemistry

Diagnosis and Inhibition Tools in Medicinal Chemistry

Akay, Senol

29 May 2009

Cell surface saccharides are involved in a variety of essential biological events. Fluorescent sensors for saccharides can be used for detection, diagnosis, analysis and monitoring of pathological processes. The boronic acid functional group is known to bind strongly and reversibly to compounds with diol groups, which are commonly found on saccharides. Sensors that have been developed for the purpose of saccharide recognition have shown great potential. However, they are very hydrophobic and this lack of essential water-solubility makes them useful in biological applications. The first section of this dissertation details the process of developing water-soluble saccharide sensors that change fluorescent properties upon binding to saccharides. The second section of the dissertation focuses on the development of DNA-minor groove binders as antiparasitical agents. Parasitical diseases comprise some of the world’s largest health problems and yet current medication and treatments for these parasitical diseases are often difficult to administer, costly to the patients, and have disruptive side effects. Worse yet, these parasites are developing drug resistance, thus creating an urgent need for new treatments. Dicationic molecules constitute a class of antimicrobial drug candidates that possess high activity against various parasites. The second section details the development of a series of di-cationic agents that were then screened in in vitro activities against parasitical species.

Carbohydrate sensing

Boronolectins

Benzo[b]thiophene boronic acid

Physiological pH

DNA-minor groove

HAT

DNA-binders

Malaria

Leishmaniasis

Chemistry

(Benzo[d]azolil)guanidinas: reações de ciclocondensação com trifluoracetil enol éteres na síntese de N-(pirimidinil)-1H-(benzo[d]azolil)aminas e N-derivados / (Benzo[d]azolyl)guanidines: cyclocondensation reactions with trifluoroacetyl enol ethers in the synthesis of N-(pyrimidinyl)-1H-(benzo[d]azolyl)amines and N-derivatives

Calheiro, Tainara Paulus

05 August 2014

Conselho Nacional de Desenvolvimento Científico e Tecnológico / The present research describes a simple and efficient procedure to synthesize a novel series of twenty N-(pyrimidinyl)-1H-(benzo[d]azolyl)amines, from the cyclocondensation reaction of (benzo[d]azolyl)guanidines with 4-alkoxy-4-alkyl(aryl/heteroaryl)-1,1,1-trifluoroalk-3-en-2-ones and 2,2,2-trifluor-1-(2-methoxycyclohexen-1-en-1-yl)ethanone. The (benzo[d]azolyl)guanidines precursors were further obtained from reactions of cyanoguanidine with o-phenylenediamine or 2-aminothiophenol and the trifluoromethylated vinyl ketones from trifluoroacetylation of enolethers or acetals. The reactions were optimized for water as solvent and when were carried out in under reflux for 1 24 h allowed to isolate the respective N-(pyrimidinyl)-1H-(benzo[d]azolyl)amines in 60 to 90 % yields. / O presente trabalho descreve um procedimento simples e eficiente para sintetizar uma nova série de 20 N-(pirimidinil)-1H-(benzo[d]azolil)aminas a partir de reações de ciclocondensação de (benzo[d]azolil)guanidinas com 4-alcóxi-4-alquil(aril/heteroaril)-1,1,1-trifluor-3-alquen-2-onas ou 2,2,2-triflúor-1-(2-metoxiciclohexen-1-en-1-il) etanona. As (benzo[d]azolil)guanidinas precursoras foram obtidas previamente a partir de reações de cianoguanidina com o-fenilenodiamina ou 2-aminotiofenol e as vinil cetonas trifluormetiladas a partir de reações de trifluoracetilação de enoléteres ou acetais. As reações de ciclocondensação foram otimizadas para o meio aquoso, sob refluxo e em tempos reacionais de 1 a 24 horas, levaram ao isolamento das respectivas N-(pirimidinil)-1H-(benzo[d]azolil)aminas em rendimentos de 60 90 %. Uma vez que as N-(pirimidinil)-1H-(benzo[d]azolil)aminas apresentaram uma baixa solubilidade na maioria dos solventes orgânicos, foram realizadas reações de N-alquilação com a finalidade estudar a reatividade e as mudanças nas suas propriedades físicas e espectroscópicas. Utilizou-se como agentes alquilantes iodometano, brometo de alila e brometo de benzila, os quais levaram a formação de novas heteroaril aminas terciárias N-alquiladas com rendimentos de 52 82 %. Finalmente, as estruturas dos compostos foram determinadas com o auxílio e aplicação simultânea de experimentos de RMN de 1H, 13C{1H}, em estados líquido e sólido, Espectrometria de Massas, Espectroscopia no Infravermelho, e a sua pureza comprovada por Análise Elementar ou por Espectrometria de Massas de Alta Resolução (HRMS).

Química

Ciclocondensação

Cetonas trifluormetiladas

Trifluoracetilação

La fura (Mustela putorius furo) com a model experimental per a l'estudi dels efectes del b-carotè en obesitat i càncer

Fuster Roca, Maria Antonia

25 May 2009

Existeix certa controvèrsia sobre els efectes del b-carotè com a promotor o protector del càncer de pulmó. A més, el b-carotè, com a precursor de l'àcid retinoic, podria estimular la termogènesi i regular l'adipositat corporal. La fura representa un bon model per estudiar els efectes de la ingesta de b-carotè ja que l'absorbeix de manera pràcticament intacta (semblant als humans). Hem demostrat que el b-carotè ingerit amb altres antioxidants no sembla tenir efectes inductors del càncer ja que no augmenta la proliferació cel·lular al pulmó i a més prevé els efectes del carcinogen benzo[a]pirè. D'altra banda, dosis farmacològiques de b-carotè fan a la fura efectes contraris als de l'àcid retinoic, ja que augmenten l'adipositat i resulten en una menor capacitat termogènica, principalment al teixit adipós retroperitoneal que, a la fura, presenta certes característiques de teixit adipós marró, ja que té un percentatge considerable d'adipòcits multiloculars i expressa quantitats significatives d'UCP1. / Existe controversia sobre los efectos del b-caroteno como promotor o protector del cáncer de pulmón. Además, el b-caroteno, como precursor del ácido retinoico, podría estimular la termogénesis y regular la adiposidad corporal. El hurón representa un buen modelo para estudiar los efectos de la ingesta de b-caroteno pues lo absorbe de manera prácticamente intacta (similar a los humanos). Hemos demostrado que el b-caroteno ingerido con otros antioxidantes no parece tener efectos inductores del cáncer puesto que no aumenta la proliferación celular del pulmón y además previene los efectos del carcinógeno benzo[a]pireno. Por otra parte, dosis farmacológicas de b-caroteno producen en el hurón efectos contrarios a los del ácido retinoico, ya que aumentan la adiposidad y reducen la capacidad termogénica, principalmente del tejido adiposo retroperitoneal que, en el hurón, presenta ciertas características de tejido adiposo marrón, al contener un porcentaje considerable de adipocitos multiloculares y expresar cantidades significativas de UCP1. / The effects of b-carotene promoting or protecting against lung cancer are unclear. Furthermore, b-carotene, as retinoic acid precursor, could induce thermogenesis and regulate body adiposity. The ferret represents a good model to study the effects of oral administration of b-carotene because it absorbs it almost intact (similarly to humans). We have shown that the intake of b-carotene together with other antioxidants does not seem to inducecancer as it does not increase cellular proliferation in lung and prevents the effects of the carcinogen benzo[a]pyrene. In addition, pharmacological b-carotene doses in ferrets have different effects from retinoic acid, increasing adiposity and decreasing thermogenic capacity, especially in the retroperitoneal adipose tissue which, in ferrets, resembles brown adipose tissue, since it has an important percentage of multilocular adipocytes and expresses significant amount of UCP1.

ferret

obesity

body weight

adiposity

thermogenesis

adipose tissue

lung cancer

cell cycle

benzo[a]pyrene

carotenoids

retinoic acid

Beta-carotene

hurón

obesidad

peso corporal

adiposidad

termogénesis

tejido adiposo

cáncer de pulmón

ciclo celular

benzo[a]pireno

carotenoides

ácido retinoico

Beta-caroteno

fura

obesitat

pes corporal

adipositat

termogènesi

teixit adipós

càncer de pulmó

cicle cel·lular

benzo[a]pirè

carotenoides

àcid retinoic

Beta-carotè

Bioquímica i Biologia Molecular

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