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  • About
  • The Global ETD Search service is a free service for researchers to find electronic theses and dissertations. This service is provided by the Networked Digital Library of Theses and Dissertations.
    Our metadata is collected from universities around the world. If you manage a university/consortium/country archive and want to be added, details can be found on the NDLTD website.
171

Influence of matrix effect of selected organochlorine pesticide residues in water from the Jukskei River catchment

Rimayi, Chengetayi Cornelius 11 1900 (has links)
M. Tech. (Biotechnology) Vaal University of Technology / One of the major problems encountered in qualitative and quantitative determination of residual pesticides by gas chromatography is the matrix effects. Matrix components have a considerable effect on the way analysis is conducted and the quality of results obtained, introducing problems such as inaccurate quantification, low analyte delectability and reporting of false positive or even false negative results. It was aimed to develop and validate a suitable method for counteracting the matrix effects so as to improve the detection and quantification of selected organochlorine pesticide residues from real water samples. The real water samples used were sampled from three points along the Jukskei River catchment area in Gauteng, South Africa for a period of 7 months from January to July 201 0 so as to create a representative sample. An automated solid phase extraction (SPE) method coupled to Gas ChromatographyMass Spectrometry (GC-MS) method for the analysis of 20 selected organochlorine pesticides was developed and validated for the purposes of studying the matrix effects. The analytical method showed a significant degree of validity when tested against parameters such as linearity, repeatability and sensitivity. Endosulphan beta, 4,4' Dichlorodiphenyldichloroethane, and Heptachlor-epoxide had the broadest linear calibration ranges of 1 ppm- 0.0156 ppm. Benzene hexachloride (BHC) delta and Lindane had the lowest statistical limits of detection of 0.018 ppm. Statistical hypothesis testing indicated that there was significant linearity in all selected organochlorine calibration curves. Four different reversed sorbent phases, including LC18, SC18- E and Strata-X (styrene divinyl benzene) were tested for organochlorine retention efficiency. The LC-18 200 mg cartridge proved to be the most robust and effective sorbent phase as it produced better recoveries varying from 90-130% for most analytes. A breakthrough volume of 100 ml for the LC-18 200 mg cartridge was determined using an optimum matrix load curve. It was then concluded that the method developed was suitable for further research towards the influence of the matrix on selective determination of the selected organochlorine pesticides. Four different calibration methods, namely matrix-free external standard, matrixmatched external standard, matrix-free internal standard and matrix-matched internal standard were applied to test the efficiency of computing recoveries. All calibration curves for the 20 organochlorine pesticides showed significant linearity > 0.99 when plotted on both Chemstation and Excel. The calibration methods were tested on three different matrices composed of a high sample matrix (synthetic matrix), a low sample matrix (real sample matrix) and a no sample matrix (ultrapure water). Statistical hypothesis testing led to the decision that there are significant differences between the mean recoveries of the three water sample matrices and also that the differences in the mean recoveries of the three sample matrices are independent of the both the two calibration techniques (internal standard and external standard) and calibration types (matrix-matched and matrix-free) applied. This led to the overall conclusion that the matrix effects have an overwhelming influence on the selective determination of the selected organochlorine pesticides.
172

Biomarqueurs d'exposition aux composés organochlorés et risque de cancer du sein : analyse de l'étude cas-témoins en population générale CECILE basée sur l'utilisation de modèles pharmacocinétiques / Biomarkers of exposure to organochlorine compounds and breast cancer risk : analysis of the CECILE study, a population-based case-control study in France, based on pharmacokinetic models to assess exposure during critical exposure windows

Bachelet, Delphine 23 January 2012 (has links)
Le cancer du sein est le plus fréquent des cancers de la femme. Son incidence n’est expliquée que partiellement par les facteurs de risque bien établis comme les facteurs reproductifs, hormonaux ou génétiques. Plusieurs éléments suggèrent l’existence de facteurs de risque environnementaux, tels que les polluants organochlorés persistants connus comme perturbateurs endocriniens. Les objectifs de ce travail sont : d’étudier les niveaux d’exposition, et leurs déterminants, au DDE (principal métabolite de l’insecticide DDT) et aux polychlorobiphényles (PCB) ; d’estimer par une modélisation pharmacocinétique à base physiologique (PBPK) les niveaux d’exposition au PCB-153 à la période péri-pubertaire qui constitue une fenêtre de susceptibilité accrue de la glande mammaire aux agents environnementaux ; d’étudier le rôle du DDE et du PCB-153 dans le risque de cancer du sein, à la fois à partir de prélèvements sanguins actuels et, pour le PCB-153, à partir de niveaux estimés à la période péri-pubertaire.Ce travail a été effectué à partir de l’étude CECILE, étude cas-témoins en population générale incluant 1055 témoins et 1080 cas de cancer du sein diagnostiqués de février 2005 à mars 2008 dans les départements d’Ille-et-Vilaine et de Côte d’Or chez lesquels un prélèvement sanguin a permis d’effectuer des dosages de p,p’-DDE et de PCB-153. La modélisation PBPK mise en place en coopération avec une équipe de toxicologues canadiens a permis de simuler des profils toxicocinétiques vie entière de PCB-153 et d’estimer les niveaux d’exposition au cours de la puberté. Cette modélisation est basée sur les niveaux mesurés au moment de l’enquête, les facteurs individuels de variation (poids, taille, grossesses, allaitement) connus d’après le questionnaire et la courbe de contamination environnementale au cours du temps.Les niveaux de contamination biologique observés sont plus faibles que ceux rapportés précédemment dans les populations occidentales. Nous montrons également que les principaux facteurs prédictifs des niveaux sériques de p,p’-DDE et de PCB-153 chez les femmes incluent l’âge, les habitudes alimentaires, le poids et ses variations au cours du temps, les grossesses et l’allaitement, et le lieu de résidence. Nous n’observons pas d’association entre les niveaux de p,p’-DDE et le risque de cancer du sein, mais une association inverse apparaît pour les cancers du sein de type négatifs pour les récepteurs hormonaux. Nous observons également une association inverse avec les niveaux de PCB-153 chez les femmes de 50 ans et plus. L’association inverse est renforcée lorsque les niveaux sont estimés pour la période péri-pubertaire à l’aide des modèles PBPK chez les femmes de la génération 1951-1960, correspondant à la cohorte de naissance des femmes de plus de 50 ans ayant connu les expositions aux PCB les plus élevées durant leur puberté.Plusieurs mécanismes biologiques pourraient expliquer l’association inverse observée entre le cancer du sein et l’exposition aux PCB. Ces résultats doivent être confirmés par des études tenant compte des fenêtres de susceptibilité de la glande mammaire et constituent une piste intéressante à approfondir. / Breast cancer is the most frequent cancer in women. Its incidence is only partially explained by well-established risk factors as reproductive, hormonal or genetic factors. It has been suggested that endocrine disrupting chemicals such as persistent organochlorine pollutants also play a role in breast cancer. The objectives of this study were: to assess exposure levels to DDE (main metabolite of DDT) and to polychlorobiphenyls (PCBs), and to explore their determinants; to estimate PCB-153 levels during the puberty using physiologically-based pharmacokinetic (PBPK) models, as this period of life constitutes a critical exposure window with increased susceptibility to carcinogens; to study the associations between breast cancer risk and separately DDE, PCB-153 measured at the time of diagnosis, and PCB-153 levels estimated during puberty.The analyses were based on data from the CECILE study, a population-based case-control study including 1055 controls and 1080 breast cancer cases who gave a blood specimen. The cases were diagnosed from February 2005 to March 2008 in two French administrative areas (Ille-et-Vilaine and Côte d’Or). p,p’-DDE and PCB-153 serum levels were measured. PBPK modeling allowed simulating PCB-153 lifetime toxicokinetic profiles and estimating exposure levels during puberty. These PBPK models were based on blood measurements at the time of recruitment in the study, on individual characteristics elicited from the questionnaire (weight, height, pregnancies, breastfeeding) and on the curve of environmental contamination by PCBs estimated since the 1930’s. The levels of biological contamination were lower than those previouly reported in Western populations in earlier periods. The main predictive factors of p,p’-DDE and PCB-153 serum levels included age; dietary habits; weight and its variations; pregnancies and breastfeeding; and residence area. We did not observed any association between p,p’-DDE levels and the risk of breast cancer, but an inverse association was observed for estrogen receptor-negative breast cancers. We also observed an inverse association of breast cancer with PCB-153 among women above 50 years. This inverse association was reinforced when considering PCB-153 levels estimated during peripubertal period from PBPK models, particularly among women born in 1951-1960, a birth cohort with peak exposure to PCB-153 during puberty. Biological mechanisms explaining the observed inverse association between breast cancer and PCB exposure are considered. These findings should be confirmed by further studies.
173

An investigation of the association between toxin producing staphylococcus, biochemical changes and jaw muscle pain.

McGregor, Neil Roland January 2000 (has links)
Objectives: To assess the expression of the symptoms of jaw muscle pain and its association with alterations in biochemistry, other symptoms and the carriage of staphylococci. Methods: Three different study populations were assessed. The first was selected and examined by the author and consisted of 43 pain and 41 age and sex matched controls. The second was a study of CFS patients who were blinded to the author and the author subsequently examined the associations between jaw muscle symptom reporting and the standardised biochemistry measures. The third study was also blinded to the author but included an investigation of staphylococci and certain cytokine and biochemistry measures. Results: The three studies clearly establish an association between the carriage of toxicogenic coagulase negative staphylococci and the expression of jaw muscle pain in both males and females. These associations were homogeneous and were found whether the patients were selected on the basis of having jaw muscle pain or selected from within a population of patients selected on the basis of having Chronic Fatigue Syndrome. The studies associated the changes with variations in biochemistry and these were in turn associated with symptom expression within the jaw muscle pain patients. These biochemical alterations included the dysregulation of immune cell counts, cytokines, electrolyte and protein metabolism. These symptoms and biochemical changes were associated with pain severity and illness duration and staphylococcal toxin production. From the data a model was developed which shows the mechanisms involved in the development of chronic pain in the jaw muscles. Conclusions: The carriage of toxicogenic coagulase-negative staphylococci were found to be associated with the expression of jaw muscle pain and the alterations in biochemistry associated with these symptoms.
174

An investigation of the association between toxin producing staphylococcus, biochemical changes and jaw muscle pain.

McGregor, Neil Roland January 2000 (has links)
Objectives: To assess the expression of the symptoms of jaw muscle pain and its association with alterations in biochemistry, other symptoms and the carriage of staphylococci. Methods: Three different study populations were assessed. The first was selected and examined by the author and consisted of 43 pain and 41 age and sex matched controls. The second was a study of CFS patients who were blinded to the author and the author subsequently examined the associations between jaw muscle symptom reporting and the standardised biochemistry measures. The third study was also blinded to the author but included an investigation of staphylococci and certain cytokine and biochemistry measures. Results: The three studies clearly establish an association between the carriage of toxicogenic coagulase negative staphylococci and the expression of jaw muscle pain in both males and females. These associations were homogeneous and were found whether the patients were selected on the basis of having jaw muscle pain or selected from within a population of patients selected on the basis of having Chronic Fatigue Syndrome. The studies associated the changes with variations in biochemistry and these were in turn associated with symptom expression within the jaw muscle pain patients. These biochemical alterations included the dysregulation of immune cell counts, cytokines, electrolyte and protein metabolism. These symptoms and biochemical changes were associated with pain severity and illness duration and staphylococcal toxin production. From the data a model was developed which shows the mechanisms involved in the development of chronic pain in the jaw muscles. Conclusions: The carriage of toxicogenic coagulase-negative staphylococci were found to be associated with the expression of jaw muscle pain and the alterations in biochemistry associated with these symptoms.

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