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131	AVALIAÇÃO DO POTENCIAL PROGNÓSTICO DA ANEMIA E DO RDW NA ESTRATIFICAÇÃO DE RISCO EM PACIENTES COM SÍNDROME CORONARIANA AGUDA / ASSESSMENT OF PROGNOSTIC POTENTIAL OF ANEMIA AND RDW IN RISK STRATIFICATION OF PATIENTS WITH ACUTE CORONARY SYNDROME Sangoi, Manuela Borges 03 April 2013 (has links) Conselho Nacional de Desenvolvimento Científico e Tecnológico / Ischemic heart diseases stands out among the diseases that affect the cardiovascular system due to its high prevalence and its impact on mortality in the general population. Ischemic heart disease is the leading worldwide cause of mortality. Fenomenum that also happens in the Americas and Brazil. The term acute coronary syndrome (ACS) is used to describe a heterogeneous spectrum of clinical conditions associated with acute myocardial ischemia, including unstable angina and acute myocardial infarction (AMI). The plurality in its clinical presentation represents a diagnostic challenge for clinicians. Moreover, appropriate risk stratification is mandadatory in all patients with ACS. Some clinical tools such as physical examination, electrocardiographic observations and risk scores are extremely usefull to identify patients at high risk of unfavorable clinical outcomes. Scores of risk stratification, among those the Global Registry of Acute Coronary Events (GRACE), are widely used in the prognostic evaluation of patients with ACS.Some plasma biomarkers have also been used to improove risk stratification. The GRACE score is a fundamental part of the assessment of patients with ACS and may even prevent or minimize adverse consequences in these individuals. Nevertheless, the search for new potential prognostic parameters that could add information to these establised scores has been the subject of intense research. In this context, stands out the use of routine hematological tests , since the complete blood count is readily available for clinical use and has a good cost-benefit relationship. Recent studies have investigated the potential role of some of red cell indices, especially anemia and red cell distribution width (RDW), in the prognostic evaluation of patients with several cardiovascular conditions. The presence of anemia and elevated RDW in patients with ACS have been independently associated with increased risk of adverse events such as heart failure, recurrent ischemic events, and death. We have hipotezazed that the addition of the hemalological indices to the GRACE score would improve its ability to stratify patients.The main objective of this study was to investigate whether inclusion of anemia or RDW, assessed at admission, in the GRACE score model to predic in-hospital mortality, could improve the discrimination and calibration of these model, as well as risk stratification in patients with ACS. For this, a cohort study, including 109 patients with AMI was carried out. Cox regression models including the variables of the GRACE score and RDW or anemia were constructed. Measures of calibration and discrimination, and reclassification of patients were also calculated for the new models. The new models, either with the inclusion of anemia, or the addition of RDW showed adequate calibration and discrimination. Furthermore, the addition of these parameters to the original model allowed adequate reclassification of patients in different categories of risk. The red cell indices, anemia and RDW showed potential prognostic for use in risk assessment of patients with ACS, allowing the improvement of risk stratification performed through the GRACE score. / A cardiopatia isquêmica destaca-se entre as doenças que acometem o sistema cardiovascular, devido à sua alta prevalência e a seu impacto sobre a mortalidade na população em geral. As doenças isquêmicas do coração são a principal causa de mortalidade mundial, nas Américas e no Brasil. O termo SCA é usado para descrever um espectro heterogêneo de condições clínicas associadas com isquemia aguda do miocárdio, incluindo angina instável e infarto agudo do miocárdio (IAM). A diversidade na apresentação clínica de pacientes com esta patologia representa um desafio para os clínicos em termos de diagnóstico e de estratificação de risco apropriada. Algumas ferramentas clínicas como exame físico, observações eletrocardiográficas e escores de risco, são de extrema relevância na identificação de pacientes com alto risco de desfechos clínicos desfavoráveis. Além disso, alguns biomarcadores plasmáticos também vêm sendo utilizados com este propósito e a busca por novos parâmetros com potencial prognóstico tem sido alvo de intensas pesquisas. Neste contexto, destaca-se a utilização dos testes hematológicos de rotina na estratificação de risco, uma vez que o hemograma é um exame amplamente disponível para uso clínico e possui uma boa relação custo benefício. Estudos recentes tem investigado o potencial papel de alguns dos índices hematimétricos, especialmente anemia e amplitude de distribuição dos eritrócitos (RDW), na avaliação prognóstica de pacientes apresentando diversas condições cardiovasculares. A presença de anemia, bem como valores elevados de RDW em pacientes com SCA tem sido independentemente associados com maior risco de eventos adversos como mortalidade, desenvolvimento de insuficiência cardíaca e ocorrência de eventos isquêmicos recorrentes. Os escores de estratificação de risco, principalmente o Global Registry of Acute Coronary Events (GRACE), são amplamente utilizados na avaliação prognóstica de pacientes com SCA. No entanto, os modelos disponíveis atualmente não incluem os índices hematimétricos na determinação do risco do paciente. Considerando que a estratificação de risco é parte fundamental da avaliação de pacientes com SCA, podendo evitar ou mesmo minimizar consequências adversas nestes indivíduos, o principal objetivo deste estudo foi investigar se a inclusão de anemia ou RDW, avaliados na admissão hospitalar, ao escore GRACE para a predição de mortalidade durante o período de internação hospitalar, podem melhorar a calibração e discriminação do modelo, bem como a estratificação de risco em pacientes com SCA. Para isso, um estudo de coorte, incluindo 109 pacientes com IAM, foi realizado. Modelos de regressão de Cox incluindo as variáveis do escore GRACE e o RDW ou a anemia foram construídos. Medidas de calibração e discriminação também foram calculadas, bem como o percentual de reclassificação dos pacientes para os novos modelos propostos. Os novos modelos, tanto com a inclusão de anemia, quanto com a adição de RDW, apresentaram adequada calibração e discriminação. Além disso, a adição destes parâmetros ao modelo original permitiu uma adequada reclassificação dos pacientes em diferentes categorias de risco. Os índices hematimétricos, anemia e RDW, demonstraram potencial prognóstico para utilização na avaliação de risco de pacientes com SCA, permitindo o aprimoramento da estratificação de risco realizada através do escore GRACE. Prognóstico Anemia Síndrome Coronariana Aguda Prognostic Anemia Red blood cell distribution width Acute Coronary Syndrome CNPQ::CIENCIAS BIOLOGICAS::FARMACOLOGIA
132	Etude des altérations morphologiques et biochimiques des érythrocytes au cours du sepsis / Studies of the alterations of shape and biochemistry of erythrocytes during sepsis. Piagnerelli, Michaël 05 November 2009 (has links) La microcirculation est rapidement altérée dans le sepsis et la persistance de ces altérations est associée à un mauvais pronostic. La microcirculation est composée de vaisseaux invisibles à l’œil (< 100 µm), de l’endothélium, du glycocalyx, des cellules musculaires lisses et des éléments sanguins dont les GR. <p>De nombreuses études animales et humaines ont rapporté des altérations rhéologiques des GR dans le sepsis. Ces modifications comprennent une diminution de la déformabilité, une augmentation de l’agrégation et de l’adhérence globulaire. <p>De plus, l’altération de la déformabilité peut induire des altérations du flux microcirculatoire dans des modèles expérimentaux animaux. Ces mêmes altérations rhéologiques sont rapportées dans le diabète. Dans cette pathologie, les GR présentent une diminution du contenu membranaire en AS, comme dans les processus de sénescence. <p>La déformabilité des GR dépend des caractéristiques cellulaires incluant surtout les propriétés de la membrane, la géométrie cellulaire et dans une moindre mesure la viscosité cellulaire. Malgré la connaissance des altérations de la rhéologie dans le sepsis, peu de travaux, au contraire du diabète, s’interessent aux modifications de la membrane.<p>Nous avons étudié, par analogie aux altérations globulaires rapportées dans le diabète, la membrane des GR de patients admis en soins intensifs pour un sepsis, et comparé à des GR de patients non septiques et de volontaires sains. Le contenu membranaire en AS était significativement diminué chez les patients septiques par rapport aux patients non-septiques et aux volontaires sains. De plus, les GR des patients septiques, analysés par une technique de cytométrie en flux indépendante de la température de l’échantillon, étaient rapidement plus sphériques (dans les 24 heures du sepsis) et incapables de modifier leurs formes en hypoosmolalité. Cette technique de cytométrie a par ailleurs aussi été utilisée pour l’analyse de GR de patients diabétiques et en insuffisance rénale terminale. <p> La diminution du contenu en AS est aussi rapidement observée sur la transferrine, suggérant une augmentation de la concentration et/ou de l’activité de la neuraminidase, enzyme clivant l’AS. Dans un modèle de choc septique induit chez l’ovin, nous avons confirmé la rapidité de ce phénomène. En effet, la concentration en AS libre augmente dès la 15ième heure après induction du sepsis.<p>In-vitro, nous avons pu reproduire les modifications de forme des GR observés chez les patients septiques par incubation de GR de volontaire avec de la neuraminidase, et ce en 10 heures, quelles que soient les concentrations utilisées. Ces modifications de forme et de membrane s’accompagnent d’une augmentation significative du contenu en lactate, suggérant une stimulation de la glycolyse érythrocytaire et en 2,3-DPG, facilitant la libération de l’O2 de l’Hb vers les tissus. <p>Toutes ces modifications touchant la membrane des GR des patients de soins intensifs, surtout septiques, peuvent être responsables des altérations de rhéologie que nous avons observé grâce au LORCA sur une large population admis aux soins intensifs.<p>Une meilleure compréhension des mécanismes conduisant aux altérations rhéologiques des GR dans le sepsis, et ses effets potentiellement déletères sur la microcirculation, sont nécessaires avant d’envisager les GR comme cible thérapeutique.<p><p><p> / Doctorat en Sciences médicales / info:eu-repo/semantics/nonPublished Médecine pathologie humaine Microcirculation disorders Septicemia Flow cytometry Blood -- Rheology Erythrocytes -- Deformability Microcirculation, Troubles de la Septicémie Cytométrie de flux Sang -- Rhéologie Erythrocytes -- Déformabilité globules ruges cytométrie en flux/ inflammation flow cytometry microcirculation red blood cell Inflammation
133	Estresse oxidativo em eritrócitos de bovinos intoxicados por Senecio sp. / Oxidative stress in the erythrocytes of cattle intoxicated with Senecio sp. Bondan, Carlos 10 February 2006 (has links) Coordenação de Aperfeiçoamento de Pessoal de Nível Superior / Intoxication caused by Senecio sp is characterized by irreversible damage to liver cells and may be associated with oxidative stress. The aim of this study was to evaluate the effects of intoxication by Senecio sp on lipoperoxidation, antioxidant defenses, and the osmotic resistance of erythrocytes in cattle. Blood samples from 30 intoxicated animals (group 1) and 30 samples from healthy animals (group 2) were analyzed. The diagnosis of poisoning by Senecio sp was based on histopathologic lesions verified through hepatic biopsy. The following biochemical parameters of oxidative stress in the erythrocytes were determined: thiobarbituric acid-reactive substances (TBARS), copper zinc superoxide dismutase (CuZnSOD) activity, and nonprotein sulfhydryl (NPSH) groups. Erythrocyte osmotic fragility also was evaluated. TBARS concentration and CuZnSOD activity were significantly (P < .001) higher in group 1 when compared with group 2. The concentration of erythrocyte NPSH groups was significantly (P < .03) lower in group 1 when compared with group 2. Osmotic fragility was more pronounced in the erythrocytes of group 1 when compared with group 2 (P < .001). The results of this study indicate that poisoning by Senecio sp causes a increase in lipoperoxidation, oxidation of NPSH groups, and consequently, oxidative stress in bovine erythrocytes that may contribute to hemolysis. These findings may contribute to a better understanding of the mechanisms involved in cell damage in animals intoxicated by Senecio sp. / Intoxicação causada por Senecio sp é caracterizada por danos irreversíveis às células hepáticas e pode estar associada com estresse oxidativo. O objetivo deste estudo foi avaliar os efeitos da intoxicação por Senecio sp sobre a peroxidação lipídica, defesa antioxidante e resistência osmótica dos eritrócitos em bovinos. Amostras sanguíneas de 30 animais intoxicados (grupo 1) e 30 animais sadios (grupo 2) foram analisadas. O diagnóstico de intoxicação por Senecio sp foi baseado nas lesões histopatológicas verificadas através de biópsia hepática. Os seguintes parâmetros bioquímicos de estresse oxidativo nos eritrócitos foram determinados: substâncias reativas ao ácido tiobarbitúrico (TBARS), atividade da cobre-zinco superóxido dismutase (CuZnSOD) e grupamentos sulfidris nãoproteicos (NPSH).Fragilidade osmótica dos eritrócitos também foi avaliada. A concentração de TBARS e atividade da CuZnSOD foi significativamente maior (p<.001) no grupo 1 quando comparado com o grupo 2. A concentração dos grupamentos NPSH nos eritrócitos foi significativamente menor (p<.03) no grupo 1 quando comparado o grupo 2. A fragilidade osmótica foi maior nos eritrócitos do grupo 1 quando comparada com o grupo 2 (p<.001). O resultado deste estudo indica que a intoxicação por Senecio sp causa um aumento na peroxidação lipídica, oxidação dos grupamentos NPSH, e consequentemente, estresse oxidativo nos eritrócitos de bovinos que pode contribuir para a hemólise. Estes achados podem contribuir para o melhor entendimento dos mecanismos envolvidos no dano celular em animais intoxicados por Senecio sp. Bovinos Hemólise Peroxidação lipídica Grupos sulfidris não protéicos Estresse oxidativo Celulas vermelhas do sangue Senecio sp Superoxido dismutase Bovine Hemolysis Lipid peroxidation Nonprotein sulfhydryl Oxidative stress Red blood cell Senecio sp Superoxide dismutase
134	Deciphering causal genetic determinants of red blood cell traits Lessard, Samuel 04 1900 (has links) Les études d’association pan-génomiques ont révélé plusieurs variants génétiques associés à des traits complexes. Les mesures érythrocytaires ont souvent fait l’objet de ce genre d’études, étant mesurées de façon routinière et précise. Comprendre comment les variations génétiques influencent ces phénotypes est primordial étant donné leur importance comme marqueurs cliniques et leur influence sur la sévérité de plusieurs maladies. En particulier, des niveaux élevés d’hémoglobine fœtal chez les patients atteints d’anémie falciforme est associé à une réduction des complications et une augmentation de l’espérance de vie. Néanmoins, la majorité des variants génétiques identifiés par ces études tombent à l’intérieur de régions génétiques non-codantes, augmentant la difficulté d’identifier des gènes causaux. L’objectif premier de ce projet est l’identification et la caractérisation de gènes influençant les traits complexes, et tout particulièrement les traits sanguins. Pour y arriver, j’ai tout d’abord développé une méthode permettant d’identifier et de tester l’effet de gènes knockouts sur les traits anthropométriques. Malgré un échantillon de grande taille, cette approche n’a révélé aucune association. Ensuite, j’ai caractérisé le méthylome et le transcriptome d’érythroblastes différentiés à partir de cellules souches hématopoïétiques et identifié plusieurs gènes potentiellement impliqués dans les programmes érythroïdes fœtaux et adultes. Par ailleurs, j’ai identifié plusieurs micro-ARNs montrant des motifs d’expression spécifiques entre les stages fœtaux et adultes et qui sont enrichis pour des cibles exprimées de façon opposée. Finalement, j’ai identifié plusieurs variants génétiques associés à l’expression de gènes dans les érythroblastes (eQTL). Cette étude a permis d’identifier des variants associés à l’expression du gène ATP2B4, qui encode le principal transporteur de calcium des érythrocytes. Ces variants, qui sont également associés à des traits sanguins et à la susceptibilité à la malaria, tombent dans un élément d’ADN spécifique aux cellules érythroïdes. La délétion de cet élément par le système CRISPR/Cas9 induit une forte diminution de l’expression du gène et une augmentation des niveaux de calcium intracellulaires. En conclusion, des échantillons de génotypages exhaustifs seront nécessaires pour étudier l’effet de gènes knockouts sur les traits complexes. Les érythroblastes montrent de grandes différences au niveau de leur méthylome et transcriptome entre les différents stages développementaux. Ces différences influencent potentiellement la régulation de l’hémoglobine fœtale et impliquent de nombreux micro-ARNs et régions régulatrices non-codantes. Finalement, l’exemple d’ATP2B4 montre qu’intégrer des études épigénomiques, transcriptomiques et des expériences d’édition de génome est une approche puissante pour caractériser des variants génétiques non-codants. Par ailleurs, ces résultats impliquent ATP2B4 dans l’hydratation des érythroblastes, qui est associé à la susceptibilité à la malaria et la sévérité de l’anémie falciforme. Cibler ATP2B4 de façon thérapeutique pourrait avoir un impact majeur sur ces maladies qui affectent des millions d’individus à travers le monde. / Genome-wide association studies (GWAS) have revealed several genetic variants associated with complex phenotypes. This is the case for red blood cell (RBC) traits, which are particularly amenable to GWAS as they are routinely and accurately measured. Understanding RBC trait variation is important given their significance as clinical markers and modifiers of disease severity. Notably, increased fetal hemoglobin (HbF) production in sickle cell disease (SCD) patients is associated with a higher life expectancy and decreased morbidity. Nonetheless, most variants identified through GWAS fall in non-coding regions of the human genome, increasing the difficulty of identifying causal links. The main goal of this project was to identify and characterize genes influencing complex traits, and in particular RBC phenotypes. First, I developed an approach to identify and test potential gene knockouts affecting anthropometric traits in a large sample from the general population, which did not yield significant associations. Then, I characterized the DNA methylome and transcriptome of erythroblasts differentiated ex vivo from hematopoietic progenitor stem cells (HPSC), and identified several genes potentially implicated in fetal and adult-stage erythroid programs. I also identified microRNAs (miRNA) that show specific developmental expression patterns and that are enriched in inversely expressed targets. Finally, I mapped expression quantitative trait loci (eQTL) in erythroblasts, and identify erythroid-specific eQTLs for ATP2B4, the main calcium ATPase of RBCs. These genetic variants are associated with RBC traits and malaria susceptibly, and overlap an erythroid-specific enhancer of ATP2B4. Deletion of this regulatory element using CRISPR/Cas9 experiments in human erythroid cells minimized ATP2B4 expression and increased intracellular calcium levels. In conclusion, large and comprehensive genotyping datasets will be necessary to test the role of rare gene knockouts on complex phenotypes. The transcriptomes and DNA methylomes of erythroblasts show substantial differences correlating with their developmental stages and that may be implicated in HbF production. These results also suggest a strong implication of erythroid enhancers and miRNAs in developmental stage specificity. Finally, characterizing the erythroid-specific enhancer of ATP2B4 suggest that integrating epigenomic, transcriptomic and gene editing experiments can be a powerful approach to characterize non-coding genetic variants. These results implicate ATP2B4 in erythroid cell hydration, which is associated with malaria susceptibility and SCD severity, suggesting that therapies targeting this gene could impact diseases affecting millions of individuals worldwide. Sickle cell disease Anémie falciforme Malaria Mesures érythrocytaires Red blood cell traits Études d'associtation pan-génomiques Édition du génome Genome editing Malaria susceptibility Genome-wide association studies
135	Complications associated with preoperative anemia, perioperative bleeding and blood transfusions after isolated coronary artery bypass grafting Tauriainen, T. (Tuomas) 16 May 2017 (has links) Abstract Cardiovascular diseases are the leading cause of death worldwide, and coronary artery disease accounts for the majority of them. The treatment of choice for complex coronary artery disease is coronary artery bypass grafting. However, as surgery in general, cardiac surgery is associated with an increased risk of perioperative bleeding and utilization of blood products. The present study aimed to investigate the impact of preoperative anemia, perioperative bleeding and retained blood syndrome as well as blood transfusion on the outcomes after isolated coronary surgery. The severity of perioperative bleeding was assessed mainly using the E-CABG and UDPB stratification criteria. Our analyses showed that severe bleeding is associated with a significantly increased risk of stroke. Furthermore, severe bleeding increased the risk of several adverse events even in low-risk patients. Retained blood syndrome was observed to be a common complication after coronary surgery and was associated with an increased risk of postoperative complications. Preoperative anemia seems to have no significant impact on patient early and late survival. Instead, the frequent exposure to blood products may be the determinant of poorer survival observed among anemic patients. Perioperative blood loss and exposure to allogeneic blood has been shown to increase adverse events. Therefore, prevention of bleeding and measures to optimize patient blood management could improve patient outcomes after cardiac surgery. / Tiivistelmä Sydän ja verisuonitaudit ovat maailmanlaajuisesti yleisin kuoleman aiheuttaja, joista sepelvaltimotaudilla on suurin vaikutus. Sepelvaltimoiden ohitusleikkaus on käypä hoito vakavassa sepelvaltimotaudissa. Kuten kirurgiassa yleisestikin, erityisesti sydänkirurgia on yhdistetty suurentuneeseen verenevuodon ja verituotteiden saannin riskiin. Tutkimukseni tavoitteena oli selvittää preoperatiivisen anemian, perioperatiivisen verenvuodon, verituotteiden annon, sekä leikkausalueelle jääneen veren itsenäisiä vaikutuksia potilaiden lopputulemiin sepelvaltimoiden ohitusleikkauksen jälkeen. Verituotteiden ja perioperatiivisen verenvuodon määrää arvioitiin pääsääntöisesti käyttäen E-CABG ja UDPB verenvuotoluokituksia. Tuloksenamme oli, että vakava verenvuoto lisää merkitsevästi aivoinfarktin riskiä. Lisäksi vakava perioperatiivinen verenvuoto on yhteydessä useisiin komplikaatioihin myös matalan leikkausriskin potilailla. Leikkausalueelle jääneen veren huomattiin olevan yleinen ongelma sepelvaltimoiden ohitusleikkauksen jälkeen, minkä lisäksi se lisäsi riskiä useille haitta-tapahtumille. Preoperatiivisella anemialla ei ollut tilastollisesti merkitsevää vaikutusta potilaiden lyhyen ja pitkän aikavälin ennusteisiin. Sen sijaan, aneemisille potilaille annetut verensiirrot saattaisivat aiheuttaa näillä potilailla huomatun alentuneen elinajan ennusteen. Perioperatiivisen verenvuodon ja altistumisen verituotteille on osoitettu lisäävän haittatapahtumia. Siispä verenvuodon vähentäminen ja verituotteiden säästäminen voisi parantaa potilaiden ennustetta sydänkirurgiassa. bleeding bleeding severity blood loss blood transfusion cardiac surgery coronary artery bypass grafting low-risk outcome preoperative anemia red blood cell retained blood stroke aivoinfarkti leikkausalueelle jäänyt veri matala leikkausriski preoperatiivinen anemia punasolu sepelvaltimoiden ohitusleikkaus sydänkirurgia verensiirrot verenvuodon vakavuus verenvuoto
136	Utilisation des caroténoïdes naturels de Momordica cochinchinensis (gac) comme composés santé : extraction et bioactivité en fonction de l'origine et du procédé / Utilisation of natural carotenoids from Momordica cochinchinensis (gac) as health compounds : extraction and bioactvity depending on the origin and on the process Phan, Thi Hanh 30 October 2014 (has links) L’arille de Momordica cochinchinensis (gac), un fruit de la famille des Cucurbitacées, est la source végétale la plus riche en lycopène et β-carotène. Ces deux composés ont, respectivement, un rôle de puissant antioxydant et de provitamine A, intéressant les compléments santé. Tout d'abord, un procédé d’extraction fractionnée douce a été développé pour extraire ces caroténoïdes naturels en gardant leur qualité originale. Puis, le lycopène et le β-carotène extraits ont été caractérisés et analysés. Au moins 95 % des extraits sont composés de l’isomère all-trans. Ils ne sont pas dégradés pendant le traitement thermique représentant les procédés de formulation. Leur stéréo-mutation thermique a été évaluée. Le lycopène est plus antioxydant et donc plus rapidement isomérisé que le β-carotène à haute température. L’isomérisation augmente leur activité antioxydante, qui a été évalué par test chimique TEAC et sur l’hémolyse des cellules sanguines (KRL) in vitro. Les deux caroténoïdes de l’arille de gac sont beaucoup plus antioxydants que le Trolox contre l’hémolyse. En comparant avec d’autres sources de β-carotène, les caroténoïdes extraits de gac dans ces conditions douces restent antioxydants même à des concentrations plus élevées contrairement à ceux extraits dans des conditions classiques qui deviennent prooxydants. Ces résultats permettent de discuter la bioactivité des caroténoïdes d'après leur qualité et de leur origine, c’est à dire leur source et leur procédé d’extraction. D’un point de vue applicatif, outre le procédé de fractionnement qui est industrialisable, le traitement thermique appliqué permet de contrôler la fonctionnalité des produits riches en caroténoïdes. / The aril of Momordica cochinchinensis (gac), plant from the Cucurbitaceae family, is the richest source of lycopene and β-carotene, which are a strong antioxidant and a pro-vitamin A, respectively, interesting for health-complements. First, a process of soft extraction-fractionation was developed for extracting effectively the natural carotenoids from gac without loss of their original quality. Then, the lycopene and β-carotene extracted from gac were analyzed and characterized. At least 95% of the extracts were composed of the all-trans isomer. They were not degraded during the heat-treatment mimicking formulation processing. Their thermal stereo-mutation was evaluated. Lycopene is more antioxidant, it is thus isomerized more rapidly than β-carotene at high temperature. The isomerization of carotenoids increases their antioxidant activity that was evaluated by the chemical test TEAC and through the hemolysis of red blood cells (KRL) in vitro. The lycopene and β-carotene from gac are notably more antioxidant than Trolox. By comparing with other sources of β-carotene, carotenoids extracted from gac in these soft conditions keep their antioxidant properties, even at high concentration, contrasting with extracts obtained in classical conditions that become prooxidant. From these results, the bioactivity of carotenoids is discussed from their quality and their origin that is their source and extraction process. For application, in addition to the fractionation process which is easily transferable to the industry scale, the heat-treatment used in this study is interesting for controlling products rich in functional carotenoids Momordica cochinchinensis (gac) Caroténoïdes naturels Extraction fractionné Traitement thermique Antioxydant Bioactivité Isomérisation Cellule sanguine Compléments santé Momordica cochinchinensis (gac) Natural carotenoids Extraction-fractionation Heat-treatment Antioxidant Bioactivity Isomerization Red blood cell Health-complements 572 664.07
137	Verifiering av en förstärkningslösning vid manuella serologiska metoder / Verification of an enhancement solution for manual serological tests Carlsson, Malin January 2021 (has links) IntroduktionDe humana blodgrupperna består av A, B, AB samt O. Antigen kan detekteras av alloantikroppar, att en reaktion sinsemellan kan ske är ett krav för att en molekyl ska kunna kallas antigen. Antigen och antikroppar är vitala för analys inom transfusionsmedicin och möjliggör transfusioner av blod samtidigt som man förhindrar allvarliga transfusionsreaktioner. För att effektivisera manuella serologiska analyser används saltlösning med låg jonstyrka. Syftet med arbetet var att verifiera lösningen MLB 2 (Bio-Rad Medical Diagnostics GmbH, Dreieich, Tyskland). Denna lösning ska förstärka reaktioner i antikroppsidentifiering, blodgruppskontroll med antikropps-screening samt förenlighetsprövning, men även för fenotypning av erytrocyter gällande antigenen s, Fya, Fyb, Kpa, Kpb samt Lua. MetodTotalt fenotypades 61 prover varav 31 var positiva och 30 var negativa för sökt fenotyp. Av de 31 positiva var 17 fenotyper av känt heterozygot anlag. Vid varje analystillfälle utfördes kontroller som bestod av heterozygot positiva samt negativa celler från Örebropanelen för vardera fenotyp. För antikroppsidentifiering ämnade två antikroppar, anti-E samt anti-Lea, att analyseras från två prover där de tidigare identifierats. Beträffande blodgruppskontroll med antikroppsscreening samt förenlighetsprövning analyserades tre prover från patienter som varit i behov av transfusioner och som tidigare påvisat antikroppar. Resultat och slutsatsSamtliga provers resultat överensstämde fullständigt vid fenotypning. För antikroppsidentifiering bekräftas tidigare påvisad anti-E för ett av proven, men för det andra provet erhölls inte resultat fullständigt överensstämmande med patientens anti- Lea. För blodgruppskontroller med antikropps-screen samt förenlighetsprövning överensstämde samtliga resultat. Effekten av förstärkningslösningen MLB 2 bedöms som god. Tydligt blir dock att gelteknik, som idag används som golden standard, är överlägsen de äldre rörteknikerna. / BackgroundHuman blood groups are defined as A, B, AB and O. Antigens are detectable by alloantibodies and a reaction between them is necessary in order to denominate as such. Antigens and antibodies respectively are essential within immunohematology to enable transfusion therapy while evading severe transfusion reactions. To improve the efficiency of manual serological test, low ionic strength saline is used. The purpose of this study was to verify MLB 2 (Bio-Rad Medical Diagnostics GmbH, Dreieich, Germany) for use as low ionic saline solution (LISS) in indirect agglutination technique (IAT) tube-tests for antibody identification, blood group verification with antibody-screen and compatibility test, also for phenotyping antigens s, Fya, Fyb, Kpa, Kpb and Lua. MethodsA total of 61 samples, of which 31 were previously known positive and 31 negative were tested. Of the 31 positive, 17 were heterozygous. At every assay, positive heterozygous and negative cells for each of the phenotype was applied as control, from the Örebro panel. For antibody identification, two previously positive samples were used. For blood group verification with antibody-screen and compatibility test, three samples with previous need for transfusion therapy and positive antibody screen were used. Results and conclusionAll samples phenotyped present fully consistent results compared to the previous ones. For antibody identification the results for one of the samples are completely confirmed. The second sample showed inconsistencies to the previous result. For blood group verification with antibody-screen and compatibility test all samples had equivalent results. The effect from MLB 2 in IAT-LISS tube tests are adequate. A distinct observation can be made; gel column technology is superior to the tube tests. phenotyping red blood cell antigen antibody detection antibody identification immunohematology traditional tube test compatibility test fenotypning erytrocytantigen antikroppsidentifiering rörteknik immunhematologi förenlighetsprövning rörteknik Biomedical Laboratory Science/Technology
138	Large Scale Synthesis of Polymerized Human Hemoglobin for Use as a Perfusate in <i>Ex Vivo</i> Normothermic Machine Perfusion Cuddington, Clayton 09 September 2022 (has links) No description available. Chemical Engineering Red Blood Cell Substitute Artificial Oxygen Carrier Oxygen Therapeutic Hemoglobin-based Oxygen Carrier HBOC Polymerized Human Hemoglobin PolyhHb Normothermic Machine Perfusion NMP Ex Vivo Lung Perfusion EVLP
139	TYROSINE PHOSPHORYLATION MEDIATED REMODELING OF THE ERYTHROCYTE MEMBRANE IN SICKLE CELL DISEASE John M Hausman (14043162) 04 November 2022 (has links) <p>The pathological hallmarks of sickle cell disease originate from a single mutation of the beta hemoglobin gene resulting in a valine at position 6 instead of the canonical glutamic acid. This small change perpetuates many factors, manifesting into chronic embolic processes in the microvasculature, causing painful vaso-occlusive episodes and eventual organ failure. There have been numerous therapies developed to reduce the mortality of sickle cell ranging from agents to induce production of fetal hemoglobin to chronic blood transfusions. Although each of these options are effective at improving the quality of life for sickle cell patients, they only treat one aspect of the disease and, for some, become ineffective over time. In the hope of producing a better therapy, a better understanding of the pathogenesis of vaso-occlusive episodes is needed. While many models have been offered to account for these vaso-occlusive events, one recently proposed mechanism stems from the elevated tyrosine phosphorylation of the cytoplasmic domain of the major erythrocyte membrane protein, Band 3. Band 3 serves as a hub for many critical proteins in the red cell. It binds ankyrin, which associates the spectrin cortical cytoskeleton to the red cell membrane, deoxygenated hemoglobin, the kinases Wnk1 and OSR1, which regulate cation transport, and a glycolytic enzyme metabolon that regulates the production of ATP and glutathione. When Band 3 is tyrosine phosphorylated, each of these proteins dissociate, causing significant changes to red cell homeostasis. These changes include an accumulation of reactive oxygen species, vesiculation and release of prothrombotic microvesicles, leakage of cell free hemoglobin, and a decrease in cell volume. Normally, Band 3 exists in a predominantly unphosphorylated state, however, in sickle cell disease, Band 3 is abundantly tyrosine phosphorylated. Reduction in the tyrosine phosphorylation of Band 3 has been documented to prevent the release of microvesicles and hemoglobin from sickle cell red blood cells. Because these microvesicles and cell free hemoglobin contribute to the vaso-occlusive episodes in sickle cell patients, inhibiting the mechanism for their release offers a potential therapeutic option. But to accomplish this, the molecular cause for the elevated tyrosine phosphorylation in sickle cell disease must be identified. Since tyrosine phosphorylation is performed by a tyrosine kinase and removed by a tyrosine phosphatase, the elevation in phosphorylation must be due to changes in both of these processes. Unfortunately, the identity and nature of these kinases and phosphatases are poorly understood. In this dissertation, I identified the tyrosine kinases Syk, Lyn, and Src attributed to Band 3</p> <p>15</p> <p>phosphorylation that facilitates the release of microvesicles and hemoglobin in sickle cell red blood cells. Inhibition of Syk or one of the two Src family kinases is sufficient to prevent the destabilization of the red blood cell membrane. These kinases function in a hierarchy, where one of the three Src family kinase, Lyn phosphorylates Syk, activating it, and promoting the phosphorylation of Band 3 at tyrosines 8 and 21. Prevention of either phosphorylation event prevents the release of microvesicles and cell free hemoglobin. I also report the identification of PTP1B as the tyrosine phosphatase responsible for maintaining Band 3 in an unphosphorylated state. Interestingly, in sickle cell disease, this tyrosine phosphatase is proteolytically cleaved, resulting in a reduction in dephosphorylating potential. It has been reported previously that PTP1B is a substrate of the calcium dependent protease, calpain and that calpain inhibitors improve the cell morphology of sickle erythrocytes. Inhibition of this proteolytic process may offer an additional therapeutic option for the treatment of sickle cell disease.</p> Biologically active molecules Molecular medicine Proteins and peptides Red Blood Cell membrane protein band 3 Tyrosine Kinase Inhibitors Targeting Tyrosine Phosphatases
140	Age-Related Differences in In-vitro Sensitivity to Inhibition of Human Red Blood Cell Acetylcholinesterase and Plasma Butyrylcholinesterase by the Cholinesterase Inhibitors Physostigmine (PHYS), Pyridostigmine (PYR), Donepezil (DON) and Galantamine (GAL) Lee, David 31 July 2009 (has links) Alzheimer’s disease (AD) is a chronic, progressive neurodegenerative disorder, characterized clinically by a progressive loss of memory, cognitive function, ability to care for oneself and psychiatric symptoms. First-line agents for the treatment of AD are ChE inhibitors (DON, GAL), whose modest clinical efficacy and the high incidence of dose-limiting toxicities limit their clinical utility. In addition to AD, ChE inhibitors (PYR) are used for other medical conditions, such as myasthenia gravis (MG). Furthermore, ChE inhibitors (PYR) are used by military personnel prophylactically if impending exposure to chemical warfare agents, e.g., soman, is suspected. The purpose of this research project was to understand the effect of age on the in-vitro sensitivity of ChE inhibitors in human RBCs and plasma. Understanding possible covariates, such as age and gender, may assist in optimizing dosing regimens of ChE inhibitors and/or developing newer ChE inhibitors with better adverse effect profiles. Plasma PHYS concentrations were measured by a validated HPLC-FD method. RBC AChE activity and plasma BuChE activity were measured by a modified Ellman’s colorimetric method using the model substrates, acetylthiocholine and butyrylthiocholine, respectively. The kinetics of RBC and plasma ChE activity followed Michaelis-Menten kinetics. Acetylthiocholine was found to be a nonselective substrate (RBC AChE Km = 73 μM; plasma BuChE Km = 117 μM); while butyrylthiocholine was a selective substrate for plasma BuChE (RBC AChE Km = 130,000 μM; plasma BuChE Km = 72 μM). For the following studies, RBC AChE activity was measured using acetylthiocholine as the substrate and plasma BuChE activity was measured using butyrylthiocholine as the substrate. This research project was performed in two parts: First, mechanistic studies of PHYS, PYR, DON and GAL, explored and determined the mechanism of in-vitro inhibition of RBC AChE and plasma BuChE inhibition, as well as the in-vitro degradation of PHYS in human whole blood, plasma and RBC. PHYS was rapidly degraded in human whole blood, RBC and plasma and followed Michaelis-Menten kinetics but its degradation clearance - scaled to whole blood clearance - was only predicted to account for 4-6% (i.e., 195-261 ml/min) of the reported total body clearance for PHYS (4500 ml/min). RBCs were responsible for 60% of the whole blood clearance while plasma accounted for 40% of the whole blood clearance. Inhibition results indicated that both PHYS and PYR were nonselective and rapid suicide ChE inactivators. PYR inactivated RBC AChE more rapidly at low concentrations and inactivated plasma BuChE more rapidly at high concentrations, but inactivated both more rapidly than PHYS. PHYS was a more potent inactivator than PYR with a Ki for RBC AChE of 0.011 μM and 0.063 μM, respectively, and 0.023 μM and 0.036 μM, respectively for plasma BuChE. DON was found to be a noncompetitive inhibitor for RBC AChE (Ki,noncomp = 114 μM), but a competitive inhibitor for plasma BuChE (Ki,comp = 213 μM). GAL was found to be a competitive inhibitor for both RBC AChE (Ki,comp = 66 μM) and plasma BuChE (Ki,comp = 358 μM). The second part involved a clinical study with ten young and nine elderly healthy subjects, balanced for gender, who donated blood for an in-vitro study in order to assess any age- and gender-related differences in in-vitro sensitivity to RBC AChE and plasma BuChE inhibition to all four ChE inhibitors. Elderly adults were found to be 2-3-fold less sensitive compared to the young adults for PHYS (BuChE Ki,pss; 0.010 and 0.015 μM, young and elderly, respectively) and PYR (AChE Ki,pss; 0.12 and 0.25 μM, young and elderly, respectively) only, while neither DON nor GAL showed any age-related differences in sensitivity. The observed differences for PHYS and PYR may be due to kinetic differences in ChE inactivation between young and aged adults, rather then a difference in binding affinities/potencies. These carbamate ChE inhibitors, presumably, have a slower decarbamoylation rate in younger adults than elderly adults, which leads to the observed difference in in-vitro sensitivity. The above in-vitro results were consistent with results of a meta-analysis: In a study by Knapp et al. (1991), young males (n=6), receiving 18 mg, 24 mg and 30 mg PHYS tablets, showed similar ex-vivo plasma BuChE sensitivity to (28 %/(ng/ml)) as the in-vitro sensitivity for young males in the current study (33 %/(ng/ml)). On the other hand, in the study by Men (2004), elderly males (n=8) and females (n=8), receiving 6.7 μg/kg PHYS as 30-minute infusion, showed similar ex-vivo RBC AChE sensitivity (12 %/(ng/ml)) as the in-vitro sensitivity for elderly subjects in the current study (9.7 %/(ng/ml)). This suggests that in-vitro measurement of ChE sensitivity is predictive of ex-vivo sensitivity in clinical studies. The study results suggest that elderly adults may require a 2-3-fold higher blood concentration than young adults to achieve the same ChE inhibition. This may explain why for epistigmine, an investigational carbamate ChE inhibitor for the treatment of AD, the maximum tolerated dose observed in young adults (40 mg single dose) was lower than for older adults (90 mg/day). Higher sensitivity in young adults prevented further dose escalation, while all elderly subjects tolerated higher doses. This research may have implications for other diseases and conditions, most notably MG and as a prophylaxis of nerve gases poisoning. As patients with MG age, they may become less sensitive to PYR, the most common symptomatic treatment for MG, and an increase in dose may be required. Further, older military personnel assigned to receive PYR, may require increased doses to achieve the targeted 10% RBC AChE inhibition, necessary to protect against nerve gas poisoning. acetylcholinesterase butyrylcholinesterase cholinesterase inhibitors aging in-vitro sensitivity physostigmine galantamine donepezil pyridostigmine red blood cell plasma age-related suicide inactivator competitive inhibitors noncompetitive inhibitors mechanism-based inhibitor inhibitor models enzyme kinetics inhibitor kinetics Alzheimer’s disease myathenia gravis Medicine and Health Sciences Pharmacy and Pharmaceutical Sciences

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