Composés radiopharmaceutiques marqués au fluor-18 utilisés en routine clinique: nouvelles méthodes de production et validation animale / Florine-18 labelled radiopharmaceuticals in clinical routine use: new methods of production and animal validation

Aerts, Joël

18 December 2008

RESUME: Le travail de recherche rapporté dans cette thèse concerne lamélioration de traceurs marqués au fluor-18 utilisés en routine clinique : la 2-[18F]fluoro-L-tyrosine et le 2-désoxy-2-[18F]fluoro-D-glucose. Les résultats relatifs à lacide aminé, de valeur confirmative pour les connaissances publiées antérieurement dans la littérature, consistent en une validation chez le rat qui entérine le potentiel de ce traceur pour létude de la vitesse de synthèse des protéines cérébrales in vivo. Les perspectives futures pour ce traceur sont dès lors lextension de son utilité dans le domaine de loncologie et son utilisation pour létude de phénomènes physiologiques neurologiques. Durant ce travail, des techniques décrites dans la littérature, mais non pratiquées au CRC ont fait lobjet dune implémentation et sont maintenant accessibles (modèle du rat vigile, méthodes de synthèse de polymères à empreinte moléculaire). La partie principale du travail concerne la récupération du [18F]fluorure et son utilisation pour le marquage nucléophile sans étape dévaporation. La synthèse du 2-désoxy-2-[18F]fluoro-D-glucose a servi de réaction témoin pour tester lapplicabilité des méthodes développées dans ce cadre. Deux stratégies différentes, lune utilisant des supports ioniques et des solvants protiques, lautre utilisant des supports non ioniques et des solvants non protiques, ont permis datteindre les buts fixés avec des rendements dincorporation du [18F]fluorure de même ordre de grandeur que ceux obtenus en radiochimie usuelle du fluor-18. La méthode utilisant les supports non ioniques a par ailleurs démontré sa grande généralité vis-à-vis de précurseurs divers, aliphatiques et aromatiques, dans des conditions de marquage diverses, notamment à température modérée. Les perspectives de ces méthodes nouvelles pour la fabrication des traceurs TEP tirent parti de la possibilité de les implanter dans un automate miniaturisé (milli- ou micro-réacteur), à visée synthétique ou analytique. Lefficacité et la simplicité des méthodes de récupération sans évaporation mises au point dans ce travail les destinent à être utilisées aussi bien en développement des traceurs quen synthèse de routine. Elles sont applicables aussi bien à léchelle des automates courants quà celle des futures applications microfluidiques. Par ailleurs, nous sommes persuadés de lintérêt des polymères à empreinte moléculaire dans le créneau des méthodes analytiques. Egalement applicables à des systèmes miniaturisés, ils devraient aider à la réalisation danalyses automatisées des produits finis et à une libération accélérée. Le gain de temps et les moindres pertes de principe actif conduiront alors à une meilleure disponibilité des traceurs TEP et à leur participation accrue aux objectifs de la médecine personnalisée. Nous pensons dès lors avoir ouvert quelques pistes de recherche prometteuses pour la mise en application de ses nouvelles technologies au domaine de la tomographie à émission de positon. / SUMMARY: The results reported in this work concern the improvement of 18-fluorine labelled radiopharmaceuticals used in routine clinical applications: 2-[18F]fluoro-L-tyrosine and 2-deoxy-2-[18F]fluoro-D-glucose. The study of the metabolism of non carrier added 2-[18F]fluoro-L-tyrosine in rats confirms that this tracer is rapidly and extensively incorporated into cerebral proteins and is therefore well suited to the assessment of Protein Synthesis Rate (PSR) in vivo by PET. A correction for the appearance of metabolites is advised for quantitative interpretation of the data. An improvement in the radiosynthesis is necessary to make 2-[18F]fluoro-L-tyrosine widely available for its application in oncology and to envisage the extended use of this tracer for the study of the protein synthesis in other physiological or pathological processes. The second chapter deals with use of molecular imprints in the PET radiochemistry. The molecularly imprinted polymers were synthetized, characterized and tested for the production of specific PET tracers and the plasma analysis of the parent metabolites. The third part of the work consisted in a development of new methods for the [18F]fluoride recovery in order to permit the labelling of different precursors through nucleophilic substitution without the evaporation step classically performed in 18-fluorine radiochemistry. The synthesis of 2-deoxy-2-[18F]fluoro-D-glucose has been used as a tool for the evaluation of the developed methods. Two strategies were considered to concentrate and recover the [18F]fluoride. The first one used ionic solid supports and protic solvents. The second one relied on the use of non ionic solid supports and non protic solvents. Both strategies led us to reach [18F]fluoride incorporation yields as high as in classical radiosyntheses with evaporation. Ionic liquids and tertiary alcohols were also evaluated in order to improve the tolerance of the [18F]fluoride nucleophilic substitution to water. The molecularly imprinted polymers and the new methods for the recovery of [18F]fluoride will now be tested for the implementation of PET tracers radiosynthesis and quality control into microchip devices.

PSR

protein synthesis/synthese des proteines

18F

2-fluoro-L-tyrosine

fluorine-18/fluor-18

PET/TEP

ionic liquid/liquide ionique

ILs

18F evaporation/18F evaporation

MIP

FTYR

FDG

fluoride-18/fluorure-18

Molecular probes for the evaluation of three isomerase enzyme mechanisms in secondary metabolism

Nasomjai, Pitak

January 2010

This thesis is focused on an investigation of the mechanisms of three enzymatically mediated carbon skeleton isomerisation reactions. Chapter 1 provides an overview of some representative examples of the carbon skeleton rearrangement reactions in enzymology. Chapter 2 describes the preparation and use of fluorolittorines to explore the mechanism of the rearrangement of the tropane alkaloid littorine to hyoscyamine which is a reaction mediated by the cytochrome P450 enzyme. Chapter 3 describes the synthesis of D-ribose-1-phosphonates and the cyclic phosphonates (phostone) that are candidate inhibitors of the enzymatic isomerisation of 5-fluoro-5-deoxy-ribose-1-phosphate (5-FDRP) to 5-fluoro-5-deoxy-ribulose-1-phosphate (5-FDRulP), an important step in fluorometabolite biosynthesis pathway in Streptomyces cattleya. Chapter 4 describes the synthesis of 5-hydroxy-3,4-dioxohexylphosphonate and [5-13C]-5-hydroxy-3,4-dioxohexylphosphonate. These compounds are proposed as candidates for the transition state of the retro-aldol/aldol mechanism of the enzymatic isomerisation of 1-deoxy-D-xylulose-5-phosphate (DXP) to 2-C-methylerythitol-phophate-2-phosphate (MEP) in the biosynthesis of isopentenyl pyrophosphate (IPP) and dimethylallyl pyrophosphate (DMAPP). The influence of pH on tautomerisation of [5-13C]-5-hydroxy-3,4-dioxohexylphosphonate is also described. Chapter 5 describes the general chemical and biochemical methodologies utilised in this research project.

572.7

Avaliação da perfusão e do metabolismo glicolítico miocárdicos na miocardiopatia não-compactada isolada / Evaluation of myocardial perfusion and glycolytic metabolism in isolated non-compacted cardiomyopathy

Melo, Marcelo Dantas Tavares de

29 September 2017

Introdução: O miocárdio não-compactado é uma doença genética rara de fisiopatologia desconhecida e controversa. Vários fatores têm sido implicados na fisiopatologia, como a disfunção da microcirculação, a perda da torção ventricular, distúrbios mitocondriais e mutações. A alteração do metabolismo cardíaco ocorre precocemente a disfunção diastólica e sistólica, reforçando a relevância desse estudo na análise combinada de tomografia de emissão de pósitron (PET) com 18F-Fluor-2-desoxiglicose e cintilografia de perfusão miocárdica com 99mTc-sestamibi pela tomografia por emissão de fóton simples (SPECT) e suas implicações clínicas. Métodos: Trinta pacientes com miocárdio não-compactado (41 ± 12 anos, 53% do sexo masculino), diagnosticados pelos critérios da ressonância magnética cardíaca, e 8 indivíduos saudáveis (42 ± 12 anos, 50% do sexo masculino) foram recrutados prospectivamente para serem submetidos a análise de perfusão miocárdica pelo SPECT e da captação miocárdica de glicose marcada pela PET. Resultados: Os pacientes apresentaram valores de captação de glicose miocárdica (CMG) menor que os controles (36.9 +- 8.8 vs. 44.6 +- 5.4 umol/min/100g, respectivamente, P = 0.02). Analisando a captação nos 17 segmentos de ambos os grupos, a CGM foi significativamente reduzida em 8 segmentos dos pacientes (P < 0,05). A diferença da média da captação miocárdica de glicose de todos os segmentos do grupo controle em relação a média dos segmentos compactados dos pacientes foi de 8,3 ?mol/min/100g (p < 0,001). Déficit de perfusão foi demonstrado em 15 (50%) dos pacientes, correspondendo a 45 segmentos do ventrículo esquerdo, destes 64,4% com padrão match e 35,6% com padrão mismatch pela análise de perfusão e metabolismo cardíaco. Nas análises univariada e multivariada foram observadas que o betabloqueador aumenta a CMG (coeficiente beta = 10.1, P = 0.008), como também ocorre um aumento gradual da CMG naqueles com doses mais elevadas (P para tendência linear = 0.01). Conclusão: A redução da captação miocárdica de glicose suporta a hipótese de que um mecanismo metabólico celular possa ter um papel na fisiopatologia do miocárdio não compactado. O betabloqueador demonstrou um efeito incremental dosedependente na captação miocárdica de glicose nos pacientes com miocárdio não-compactado, essa modulação do substrato cardíaco necessita de mais estudos para comprovação do benefício clínico nessa população / Background: Noncompaction cardiomyopathy (NCC) is a rare genetic disease with unknown and controversial pathophysiology. Several factors have been implicated such as microvascular dysfunction, loss of ventricular torsion, mitochondrial disorders, and genetic mutations. The change in cardiac metabolism occurs before the diastolic and systolic dysfunction, reinforcing the relevance of this study by the combined analysis of positron emission tomography with 18F-Fluor-2-deoxyglucose (PET) and myocardial perfusion scintigraphy with 99mTc-sestamibi by single-photon emission computed tomography (SPECT) and their clinical implications. Methods: Thirty patients (41 ± 12 years, 53% male) with NCC, diagnosed by cardiovascular magnetic resonance criteria, and 8 age-matched healthy controls (42 ± 12 years, 50% male) were prospectively recruited to undergo FDG-PET with measurement of the myocardial glucose uptake rate (MGU) and SPECT in order to investigate perfusion-metabolism patterns. Result: Patients with LVNC had lower global MGU compared with that in controls (36.9 +- 8.8 vs. 44.6 +- 5.4 +-mol/min/100g, respectively, P = 0.02). Of 17 LV segments, MGU levels were significantly reduced in 8, and also a reduction was observed when compacted segments from LVNC were compared with the segments from control subjects (P < 0,05). The difference in mean myocardial glucose uptake of all segments of the control group compared to the mean of the compact segments of the patients was 8.3 ?mol/min/100g (p < 0,001). Perfusion defects were also found in 15 (50%) patients (45 LV segments: 64.4% match, and 35.6% mismatch perfusionmetabolism pattern). Univariate and multivariate analyses showed that betablocker therapy was associated with increased MGU (beta coefficient=10.1, P = 0.008). Moreover, a gradual increase occurred in MGU across the beta-blocker dose groups (P for trend = 0.01). Conclusions: The reduction of MGU documented by FDG-PET in LVNC supports the hypothesis that a cellular metabolic pathway may play a role in the pathophysiology of LVNC. Betablocker demonstrated an incremental dose-dependent effect on myocardial glucose uptake in patients with NCC. The beneficial effect of beta-blocker mediating myocardial metabolism in the clinical course of LVNC requires further investigation

18F-fluoro-2-deoxyglucose

Cardiac magnetic resonance imaging

Cardiomiopatias

Cardiomyopathy

Glicose Fluordesoxiglucose F18

Imagem por perfusão do miocárdio

Imagem por ressonância magnética

Metabolism

Metabolismo

Myocardial perfusion imaging

Extraction des actinides et des lanthanides du combustible du réacteur rapide à sels fondus

Jaskierowicz, Sebastien

29 November 2012

Le procédé de traitement du combustible du réacteur à sels fondus (réacteur de génération IV) est un procédé multi-étape dans lequell'extraction des actinides et des lanthanides utilise la technique d'extraction réductrice. Le développement d'un modèle analytique a montré que la mise en contact du sel combustible LiF-ThF4 avec une phase métallique constituée d'un mélange Bi-Li permet l'extraction sélective et quantitative des actinides dans un premier temps, puis l'extraction quantitative des lanthanides dans un second temps. La maitrise de ce procédé nécessite la connaissance des caractéristiques des phases salines impliquées dans le procédé. Les études des propriétés physico-chimiques des sels fluorures fondus ont permis de développer une technique de mesure de la fluoroacidité dans ces milieux via une mesure potentiométrique. Cette technique a permis d'établir un classement de différents mélanges de fluorures fondus en fonction de leur acidité relative. Par ailleurs, une méthode de détermination de la solvatation de solutés dans ces milieux a également été développée par électrochimie afin d'approfondir la connaissance du sel combustible (en particulier solvatation de ThF4 par les ions F-).L'extraction réductrice met également en jeu une phase métallique liquide. Une technique de préparation de cette phase a été développée par électro-réduction de lithium sur une électrode liquide de bismuth en milieu LiCl-LiF. Cette technique permet un bon contrôle de la fraction molaire de lithium introduite dans le bismuth, paramètre essentiel à l'efficacité de l'extraction.Enfin, afin d'optimiser le procédé général de traitement multi-étapes, des méthodes électrochimiques ont été proposées afin de régénérer les différentes phases liquides (salines et métalliques) mise en jeu lors de l'extraction.

[CHIM:OTHE] Chemical Sciences/Other

Sels fondus

Réacteur à sels fondus

Traitement du combustible

Extraction

Fluoro-acidité

Bismuth liquide

LiF-ThF4

LiCl-LiF

Pyrochimie

Regional Lung Kinetics of Ventilator-Induced Lung Injury and Protective-Ventilation Strategies Studied by Dynamic Positron Emission Tomography

Borges, João Batista

January 2014

Mechanical ventilation in itself can harm the lung and cause ventilator-induced lung injury (VILI), which can induce or aggravate acute respiratory distress syndrome (ARDS). Much debate remains over pivotal concepts regarding the pathophysiology of VILI, especially about the precise contribution, kinetics, and primary role of potential VILI mechanisms. Consequently, it remains largely unknown how best to design a well-timed and full-bodied mechanical ventilation strategy. Little is known also about small airways dysfunction in ARDS. Dynamic positron emission tomography (PET) with [18F]fluoro-2-deoxy-D-glucose (18F-FDG) can be used to image cellular metabolism, which during lung inflammation mainly reflects neutrophil activity, allowing the study of regional lung inflammation in vivo. We studied the regional evolution of inflammation using dynamic PET/CT imaging of 18F-FDG in VILI and during different lung-protective mechanical ventilation strategies. By dynamic CT we investigated also the location and magnitude of peripheral airway closure and alveolar collapse under high and low distending pressures and high and low inspiratory oxygen fraction. Piglets were submitted to an experimental model of early ARDS combining repeated lung lavages and injurious mechanical ventilation. The animals were subsequently studied during sustained VILI, or submitted to distinct approaches of lung-protective mechanical ventilation: the one recommended by the ARDS Network (ARDSNet), or to one defined as open lung approach (OLA). The normally and poorly aerated regions - corresponding to intermediate gravitational zones - were the primary targets of the inflammatory process accompanying early VILI, which may be attributed to the small volume of the aerated lung that receives most of ventilation. The ARDSNet strategy did not attenuate global pulmonary inflammation during 27h and led to a concentration of inflammatory activity in the upper and poorly aerated lung regions. The OLA, in comparison with the ARDSNet approach, resulted in sustained and better gas exchange and lung mechanics. Moreover, the OLA strategy resulted in less global and regional inflammation. Dynamic CT data suggested that a significant amount of airway closure and related reabsorption atelectasis occurs in acute lung injury. Whether potential distal bronchioles injury (“bronchiolotrauma”) is a critical and decisive element in ventilator-associated lung injury is a matter for future studies.

Medical and Health Sciences

Medicin och hälsovetenskap

Avaliação da perfusão e do metabolismo glicolítico miocárdicos na miocardiopatia não-compactada isolada / Evaluation of myocardial perfusion and glycolytic metabolism in isolated non-compacted cardiomyopathy

Marcelo Dantas Tavares de Melo

29 September 2017

Introdução: O miocárdio não-compactado é uma doença genética rara de fisiopatologia desconhecida e controversa. Vários fatores têm sido implicados na fisiopatologia, como a disfunção da microcirculação, a perda da torção ventricular, distúrbios mitocondriais e mutações. A alteração do metabolismo cardíaco ocorre precocemente a disfunção diastólica e sistólica, reforçando a relevância desse estudo na análise combinada de tomografia de emissão de pósitron (PET) com 18F-Fluor-2-desoxiglicose e cintilografia de perfusão miocárdica com 99mTc-sestamibi pela tomografia por emissão de fóton simples (SPECT) e suas implicações clínicas. Métodos: Trinta pacientes com miocárdio não-compactado (41 ± 12 anos, 53% do sexo masculino), diagnosticados pelos critérios da ressonância magnética cardíaca, e 8 indivíduos saudáveis (42 ± 12 anos, 50% do sexo masculino) foram recrutados prospectivamente para serem submetidos a análise de perfusão miocárdica pelo SPECT e da captação miocárdica de glicose marcada pela PET. Resultados: Os pacientes apresentaram valores de captação de glicose miocárdica (CMG) menor que os controles (36.9 +- 8.8 vs. 44.6 +- 5.4 umol/min/100g, respectivamente, P = 0.02). Analisando a captação nos 17 segmentos de ambos os grupos, a CGM foi significativamente reduzida em 8 segmentos dos pacientes (P < 0,05). A diferença da média da captação miocárdica de glicose de todos os segmentos do grupo controle em relação a média dos segmentos compactados dos pacientes foi de 8,3 ?mol/min/100g (p < 0,001). Déficit de perfusão foi demonstrado em 15 (50%) dos pacientes, correspondendo a 45 segmentos do ventrículo esquerdo, destes 64,4% com padrão match e 35,6% com padrão mismatch pela análise de perfusão e metabolismo cardíaco. Nas análises univariada e multivariada foram observadas que o betabloqueador aumenta a CMG (coeficiente beta = 10.1, P = 0.008), como também ocorre um aumento gradual da CMG naqueles com doses mais elevadas (P para tendência linear = 0.01). Conclusão: A redução da captação miocárdica de glicose suporta a hipótese de que um mecanismo metabólico celular possa ter um papel na fisiopatologia do miocárdio não compactado. O betabloqueador demonstrou um efeito incremental dosedependente na captação miocárdica de glicose nos pacientes com miocárdio não-compactado, essa modulação do substrato cardíaco necessita de mais estudos para comprovação do benefício clínico nessa população / Background: Noncompaction cardiomyopathy (NCC) is a rare genetic disease with unknown and controversial pathophysiology. Several factors have been implicated such as microvascular dysfunction, loss of ventricular torsion, mitochondrial disorders, and genetic mutations. The change in cardiac metabolism occurs before the diastolic and systolic dysfunction, reinforcing the relevance of this study by the combined analysis of positron emission tomography with 18F-Fluor-2-deoxyglucose (PET) and myocardial perfusion scintigraphy with 99mTc-sestamibi by single-photon emission computed tomography (SPECT) and their clinical implications. Methods: Thirty patients (41 ± 12 years, 53% male) with NCC, diagnosed by cardiovascular magnetic resonance criteria, and 8 age-matched healthy controls (42 ± 12 years, 50% male) were prospectively recruited to undergo FDG-PET with measurement of the myocardial glucose uptake rate (MGU) and SPECT in order to investigate perfusion-metabolism patterns. Result: Patients with LVNC had lower global MGU compared with that in controls (36.9 +- 8.8 vs. 44.6 +- 5.4 +-mol/min/100g, respectively, P = 0.02). Of 17 LV segments, MGU levels were significantly reduced in 8, and also a reduction was observed when compacted segments from LVNC were compared with the segments from control subjects (P < 0,05). The difference in mean myocardial glucose uptake of all segments of the control group compared to the mean of the compact segments of the patients was 8.3 ?mol/min/100g (p < 0,001). Perfusion defects were also found in 15 (50%) patients (45 LV segments: 64.4% match, and 35.6% mismatch perfusionmetabolism pattern). Univariate and multivariate analyses showed that betablocker therapy was associated with increased MGU (beta coefficient=10.1, P = 0.008). Moreover, a gradual increase occurred in MGU across the beta-blocker dose groups (P for trend = 0.01). Conclusions: The reduction of MGU documented by FDG-PET in LVNC supports the hypothesis that a cellular metabolic pathway may play a role in the pathophysiology of LVNC. Betablocker demonstrated an incremental dose-dependent effect on myocardial glucose uptake in patients with NCC. The beneficial effect of beta-blocker mediating myocardial metabolism in the clinical course of LVNC requires further investigation

Cardiomiopatias

Glicose Fluordesoxiglucose F18

Imagem por perfusão do miocárdio

Imagem por ressonância magnética

Metabolismo

18F-fluoro-2-deoxyglucose

Cardiac magnetic resonance imaging

Cardiomyopathy

Metabolism

Myocardial perfusion imaging

Vectorisation cérébrale de deux radiotraceurs d’intérêts pour l’imagerie, la m-iodobenzylguanidine (MIBG) et la 3’-désoxy-3’- fluoro-L-thymidine (FLT) / Targeting two radiotracers into the brain for brain imaging, m-iodobenzylguanidine (MIBG) and 3’-désoxy-3’-fluoro-L-thymidine (FLT)

Henry, Axelle

25 November 2016

Ce travail de recherche s'intéresse à la vectorisation au système nerveux central de la MIBG d'une part et de la FLT d'autre part. Pour cela, nous utiliserons des systèmes disposant d'une structure 1,4- dihydoquinoléine comme vecteurs. La synthèse des systèmes de vectorisation a tout d'abord été réalisée en chimie non radioactive. Concernant la MIBG, les résultats obtenus lors de précédents travaux nous ont conduit à envisager l'élaboration d'un système de vectorisation comportant un groupement espaceur entre le vecteur et la MIBG. Dans le cas de la FLT, nous nous sommes consacrés au développement d'un système dans lequel la FLT serait directement liée au vecteur par une liaison ester. Afin de pouvoir moduler les propriétés rédox de nos systèmes de vectorisation, nous avons synthétisé des 1,4-dihydroquinoléines présentant en position 6 et/ou 7 des groupements électroattracteurs ou électrodonneurs. Une étude en milieu acétonitrile/tampon PBS, pour évaluer l'influence de ces groupements sur la libération de la FLT, a été réalisée par un suivi CLHP. La radiosynthèse de ces systèmes a ensuite été menée afin d'évaluer la capacité des vecteurs 1,4- dihydroquinoléines à transporter la MIBG ou la FLT à travers la barrière hématoencéphalique (BHE). Ainsi, nous avons radiomarqué au carbone-11 les systèmes de vectorisation pour valider le passage de la BHE. Des études ex vivo chez le petit animal ont permis de suivre la pénétration cérébrale ainsi que la cinétique d'oxydation au niveau cérébral et en périphérie. / This research work focuses on targeting MIBG or FLT to the central nervous system. The synthesis of 1,4-dihydroquinoline carriers was first carried out in a non-radioactive manner. Previous results led us to consider the use of a linker to connect MIBG to the carrier. Regarding FLT, we focused our interest in the development of a carrier system connected directly to FLT via an ester function. For modulating the redox properties of our delivery systems, we synthesized 1,4-dihydroquinolines having electron-donating or electron-withdrawing groups at position 6 and/or 7. A study in acetonitrile/PBS buffer to determine the influence of these groups on the release of FLT was performed by HPLC. The radiosynthesis of these targeting systems was then conducted to evaluate the ability of 1,4- dihydroquinolines to deliver MIBG or FLT across the blood brain barrier (BBB). Thus, using carbon-11, we radiolabeled the delivery systems to validate the BBB crossing. Small animais were used for ex vivo studies to monitor the brain penetration and the kinetics of oxidation in the brain and periphery.

Vectorisation

Imagerie cérébrale

M-iodobenzylguanidine

MIBG

3’-désoxy-3’- fluoro-L-thymidine

FLT

Dihydroquinoline

Cerebrum--Imaging

Central nervous system

Delivery systems

Identification of the Effects of Diabetes Mellitus on the Brain

Mikhail, Tryphina A

01 January 2016

As more studies accumulate on the impact of diabetes mellitus on the central nervous system, they resound with the same conclusion - diabetes has a detrimental effect on cognition regardless of the presence of comorbidities. Less consistent however, are the specific mental processes wherein these declines are noticeable, and the structural changes that accompany these reductions in mental capacity. From global atrophy to changes in the volume of gray and white matter, to conflicting results regarding the effects of hypo- and hyperglycemic states on the development of the hippocampus, the studies display a variety of results. The goal of this research is to link the structural and compositional changes occurring in the diabetic brain with the clinical and behavioral findings highlighted in the literature, as well as to explore the potential mechanisms behind the pathologic brain state of diabetic encephalopathy. Using diabetic (OVE26) and non-diabetic wild type (FVB) mice as models, differences in the number of hippocampal neurons in the dentate gyrus, and cornu ammonis areas 1,2, and 3 were investigated through Nissl staining. Neurodegeneration was confirmed in those cells determined to be hyperchromatic in the diabetic model through staining with Fluoro-Jade C. Finally, the presence of progenitor cells in the hippocampus was compared in the diabetic and non-diabetic models using Musashi-1 antibodies, to determine whether neurogenesis in these areas is affected by diabetes. These experiments were performed to better understand the effect of DM on learning and memory, and could potentially explain the linkage between diabetes mellitus and the increased prevalence of Alzheimer’s disease, vascular dementia, and depression in this subset of the population.

diabetes mellitus

cognition

neurogenesis

neurodegeneration

hippocampus

Musashi-1

Fluoro-Jade C

Endocrine System Diseases

Nervous System Diseases

Preparation of Heteroatom-Substituted 1,3-Thiazoles as Building Blocks for Liquid Crystal Synthesis

Grubb, Alan M.

28 November 2011

No description available.

Organic Chemistry

synthetic organic chemistry

1,3-thiazole

4-fluoro-1,3-thiazole

alkoxy-1,3-thiazole

carboxy-1,3-thiazole

dibromo-1,3-thiazole

liquid crystals

Calibration and quality assessment of DESCARTES : grabsampler for stratospheric tracers

Arvelius, Johan

January 2005

<p>DESCARTES is a light-weight, balloon-borne grab sampler for stratospheric long-lived tracers developed at the University of Cambridge. 33 flights have been performed with two versions of the instrument at northern latitudes by the DESCARTES team at the Swedish Institute of Space Physics (IRF) in Kiruna during the years 1997-2000.</p><p>The general interest in long-lived stratospheric tracers is to study the general global circulation of air in the stratosphere and the exchange between the stratosphere and troposphere. In the study of chemical ozone depletion in the stratosphere, long-lived tracers serve as an important reference to distinguish between the variations in ozone of dynamical and chemical origin.</p><p>This thesis focuses on calibrations and quality assessment of the measurements made with the third version of the DESCARTES instrument based at IRF. Two different general approaches to make calibrations are discussed. Uncertainty estimations for both of these methods are made and the results are tested by laboratory methods and by comparisons to other instruments, including comparisons between two versions of DESCARTES. Analyzed and calibrated flight data for all successful flights are presented.</p><p>The basic principle of the instrument is to chemically adsorb a number of tracers (in practice only CFC-11 is measured) in an adsorption bed of Carboxen in a micro trap through which the sampled air is driven by a pump. After recovery the adsorbed species in the trap is desorbed by electrical heating of the trap and analysed by gas chromatography.</p><p>The resulting estimated mixing ratios from the instrument are directly dependent on the adsorption of the sampled species being quantitative in the traps. Laboratory experiments are described using two traps in series, where the performance of the first is tested by sampling the breakthrough by the second. A model is developed to recreate these tests in order to be able to compensate for breakthrough during flights. The model showed that the adsorption in the traps is not explained by simple chromatographic theory and the results allow us only to give an estimation of the uncertainty due to breakthrough.</p> / <p>DESCARTES är ett lätt ballongburet provtagningsinstrument för stratosfäriska spårgaser. Det är utvecklat vid universitetet i Cambridge. DESCARTES-teamet vid Institutet för rymdfysik (IRF) i Kiruna har under åren 1997-2000 genomfört 33 flygningar med två olika versioner av instrumentet från nordliga latituder.</p><p>Det generella intresset av långlivade stratosfäriska spårgaser är att studera den globala cirkulationen i stratosfären och utbytet av luft mellan stratosfären och troposfären. För studier av den kemiska ozonnedbrytningen i stratosfären spelar långlivade spårgaser en avgörande roll som referens för att skilja mellan variation i ozonkoncentrationen av kemiskt och dynamiskt ursprung.</p><p>Denna avhandling fokuserar på kalibrering och kvalitetssäkring av mätningar gjorda med den tredje versionen av DESCARTES-instrumentet hemmahörande vid IRF. Två i grunden olika kalibreringsförfaranden för instrumentet behandlas. Osäkerhetsuppskattningar är gjorda för båda dessa metoder och resultaten är prövade i laboratorietester. Dessutom jämförs resultaten från två versioner av DESCARTES och andra instrument. Analyserade data från samtliga lyckade flygningar presenteras.</p><p>Den grundläggande principen för instrumentet är att pumpa luftprover genom en fälla som innehåller en bädd av det kemiska adsorptionsmaterialet Carboxen, som adsorberar ett antal spårgaser. När instrumentet hämtats tillbaka efter en flygning gasas de adsorberade ämnena i fällan ut genom att fällan upphettas på elektrisk väg. De utgasade ämnena analyseras med gaskromatografi. I praktiken kan endast CFC-11 analyseras.</p><p>Den slutgiltiga bestämningen av blandningsförhållandet från instrumentet är direkt beroende av att adsorptionen i fällorna för de ämnen man vill undersöka är fullständig. En serie laboratorieexperiment har genomförts där två likadana fällor kopplats efter varandra. På så sätt har tillförlitligheten av den första fällan kunnat studeras genom att uppmäta hur mycket som bryter igenom till den andra fällan. En modell har utvecklats för att förstå resultatet av dessa tester och kunna kompensera för eventuella genombrott vid provtagning under flygningar. Modellen visade att adsorptionen i fällorna inte kan förklaras med enkel kromatografisk teori. Resultaten ger endast möjlighet att bedöma osäkerheten i mätningarna till följd av risken för genombrott.</p>

Adsorption

Balloon

Carboxen

CFC

Chloro-Fluoro Carbon

Grab sampling

Halocarbon

Molecular sieve

Stratospheric tracer

Tracer

Adsorption

Ballong

Carboxen

CFC

Halogeniserade kolväten

Klor-Flourkarbon

Spårgas

Stratosfärisk spårgas

Space physics

Rymdfysik