Tesi sul tema "Blood disorder"
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Neuger, Jolanta. "Platelet serotonin function and personality traits in affective disorder /". Stockholm, 2002. http://diss.kib.ki.se/2002/91-7349-181-0.
Testo completoNewsome, Dominique. "My story, my identity and my relationship with work : sickle cell disorder". Thesis, Canterbury Christ Church University, 2016. http://create.canterbury.ac.uk/14924/.
Testo completoVranish, Jennifer R. "Obstructive Sleep Apnea: Daytime Assessment And Treatment Of A Nighttime Disorder". Diss., The University of Arizona, 2015. http://hdl.handle.net/10150/566239.
Testo completoEwing, Jane Elizabeth. "Support services for adolescents and young adults with cancer or a blood disorder : measurement properties and validation of quality of life instruments for adolescents and young adults with cancer or a blood disorder". University of Technology, Sydney. Faculty of Science, 2006. http://hdl.handle.net/2100/423.
Testo completoFrans, Örjan. "Posttraumatic Stress Disorder (PTSD) in the General Population". Doctoral thesis, Uppsala University, Department of Psychology, 2003. http://urn.kb.se/resolve?urn=urn:nbn:se:uu:diva-3528.
Testo completoThis thesis explored the epidemiology of Posttraumatic Stress Disorder (PTSD) and different aspects of the disorder. Firstly, we investigated the lifetime prevalence of traumatic experiences and PTSD in the general adult population in Sweden and evaluated the impact of different trauma types, trauma frequency, and perceived distress. The results show that traumatic experiences are common and PTSD is not rare; roughly one out of ten traumatic events results in PTSD, with a 5.6% lifetime prevalence. The female/male ratio is 2:1. The risk for PTSD increases considerably with a high trauma-associated emotional impact. The distressing impact of a given trauma appears to be higher in women than in men, indicating an increased vulnerability in women. Secondly, we hypothesized that traffic road accidents (TRA’s) are one of the most prevalent types of traumatic events in Swedish society; therefore, we examined the impact of event and response characteristics associated with TRA’s on PTSD development. The data demonstrate that of those who had experienced a TRA (n=1074, 58.9%), 6.1% reported lifetime PTSD. TRA’s associated with fatal accidents and injury to oneself and related to high distress more than double the risk for PTSD. Thirdly, we compared the relative merits of the DSM-IV’s three-factor solution for PTSD symptoms to alternative models. We found that the symptomatology is equally well accounted for using all factor analytic models as yet presented in the literature; the DSM-IV, we found, provides as good a fit to data as other models. Fourthly, we examined the neurofunctional correlates of PTSD symptoms and whether a treatment-induced (serotonin reuptake inhibitor - SSRI) reduction of PTSD symptoms is associated with altered rCBF during symptom provocation. Our results indicate that PTSD symptoms correlates with areas involved in memory, emotion, attention, and motor control and that SSRI treatment normalizes provocation-induced rCBF in these areas.
Lee, Sherman. "The effect of acute cigarette smoke exposure on regional pulmonary blood flow, volume, red cell transit and polymorphonuclear leukocyte retention in the rabbit lung". Thesis, University of British Columbia, 1985. http://hdl.handle.net/2429/24840.
Testo completoPathology and Laboratory Medicine, Department of
Graduate
Rothman, David J. "The Effect of Pre-Deployment Physiology as a Predictor of Post-Traumatic Stress Disorder Among a Sample of United States Army National Guard and Reserve Soldiers". VCU Scholars Compass, 2016. http://scholarscompass.vcu.edu/etd/4123.
Testo completoNegrao, Bianca Lee. "Autonomic correlates at rest and during evoked attention in children with attention-deficit/hyperactivity disorder and effects of sympathomimetic medication". Diss., Pretoria : [s.n.], 2009. http://upetd.up.ac.za/thesis/available/etd-07072009-163036/.
Testo completoLucey, James Vincent. "Regional cerebral blood flow (rCBF) assessed as uptake of '9'9'mTc-HMPAO in the basal ganglia and other brain regions in obsessive-compulsive disorder (OCD) on single photon tomography (SPET)". Thesis, Imperial College London, 1999. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.392900.
Testo completoMarsh, Victoria Mary Chuck. "Sharing findings on sickle cell disorder in international collaborative biomedical research : an empirical ethics study in coastal Kenya". Thesis, University of Oxford, 2012. http://ora.ox.ac.uk/objects/uuid:b693b762-5ce8-4109-82ea-4cf7ba38675e.
Testo completoGUOBADIA, EDWIN AHUNWAN. "The Effects of a Sickle Cell Disease Education Intervention Among College Students". ScholarWorks, 2015. http://scholarworks.waldenu.edu/dissertations/1682.
Testo completoGuobadia, Edwin Ahunwan. "The Effects of a Sickle Cell Disease Education Intervention Among College Students". ScholarWorks, 2015. https://scholarworks.waldenu.edu/dissertations/1697.
Testo completoHuang, Sha Ph D. Massachusetts Institute of Technology. "The relevance of red blood cell deformability in the pathophysiology of blood disorders". Thesis, Massachusetts Institute of Technology, 2014. http://hdl.handle.net/1721.1/93062.
Testo completoCataloged from PDF version of thesis.
Includes bibliographical references (pages 136-144).
Red blood cells (RBCs) play a crucial role in delivering oxygen to the body tissues. During the 120 days of their lifespan, average RBCs would circulate for approximately 500,000 times and undergo repeated deformations in small blood capillaries and splenic cords. Increased RBC clearance in the spleen is considered as one of the direct consequences of reduced RBC deformability. On the other hand, deformability is also indirectly impacting on RBC functionality through its complex connections with underlying molecular mechanisms. With the aid of microfabrication and microfluidic, we are able to perform high-throughput single cell deformability measurement. Overall, we established RBC deformability as an important biomarker for several blood related real world problems such as malaria and blood storage lesion. The ultimate goal is through our quantitative assessment of population-wide single cell deformability, we could aid in the decision-making of various clinical scenarios including drug screening and blood transfusion. Malaria is the most deadly parasitic disease affecting hundred millions of people worldwide. Infected RBCs are found to be less deformable and therefore more susceptible to splenic RBC clearance. In this thesis, we identified several clinically used anti-malarial drugs that are capable of altering RBC deformability and ultimately modifying RBC retention in spleen. We also employed a rodent malarial model, confirming the important connection of RBC deformability with splenic RBC retention and consequently malarial anemia in vivo. Blood storage lesion is another important application of our work. Taking the advantage of device high-throughput, we profiled hundreds of single RBC deformability from a large population and identified subpopulations that are less deformable. These subpopulations also exhibited higher osmotic fragility and were therefore predicted to pose higher transfusion risk according clinical standard. Furthermore, a deformability based sorting device was also developed to filter the less deformable blood subpopulations, improving overall blood quality.
by Sha Huang.
Ph. D.
Sampaio, Thiago Pacheco de Almeida. "Relação entre a concentração de serotonina no plasma rico em plaquetas e a resposta à terapia comportamental baseada em exposição com prevenção de resposta no transtorno obsessivo-compulsivo". Universidade de São Paulo, 2007. http://www.teses.usp.br/teses/disponiveis/5/5142/tde-20022009-141000/.
Testo completoINTRODUCTION: Both gold standard treatments for obsessive-compulsive disorder (pharmacotherapy with serotonin reuptake inhibitors, and behavioral with exposure and response prevention [ERP]) are equally effective. Studies have demonstrated similar neurobiological changes elicited by these different treatments in OCD patients. These findings are suggestive that the clinical response to ERP is directly related to an increase of the 5-HT concentration in the brain. The platelet 5-HT concentration have been shown as a representative measure of central serotonergic system and used as a biological marker of the synaptic transmition. OBJECTIVE: To compare the platelet 5-HT concentration (basal and variation in 8 weeks) and the clinical response to ERP treatment. METHODS: 30 OCD patients were included and 29 started the treatment. 27 patients compleated at list 4 weeks and 24 completed all 8 weeks (16 sesions) ERP protocol. Patients had the basal and final (after 8 weeks) platelet 5-HT concentrations dosed and the clinical response measured by Y-BOCS, CGI and measures of secondary symptoms as well (depression, anxiety and disability). RESULTS: Data shows a positive correlation between the basal concentration of 5-HT and the 4 week ERP response (p<0,05). There were higher basal concentration and reduction in 8 weeks of platelet 5-HT concentration in the responders group compared with non-responders. Nevertheless, this differences was not significant (p>0,05). CONCLUSION: In the studied sample data suggest that high basal 5-HT platelet concentration is a biologic predictor of fast onset (4 weeks) of clinical response to ERP. Probably larger samples would show the basal 5-HT platelet concentration as a predictor of 8 weeks ERP outcome. Controlled trials are needed to confirm these findings
Wahlund, Björn. "Affective disorders : multivariate investigations of clinical and biological variables /". Stockholm, 1997. http://diss.kib.ki.se/1998/91-628-2725-1.
Testo completoLindoff, Claes. "Haemostasis during pregnancy and perimenopausal age studies of fibrinolytic components and coagulation factors involved in vascular disease /". Lund : Dept. of Obstetrics and Gynaecology, Lund University, 1994. http://catalog.hathitrust.org/api/volumes/oclc/39750405.html.
Testo completoBoyd, Helen Kathryn. "Erythropoietin and other growth factors in the anaemia of chronic disorders". Thesis, University of Newcastle Upon Tyne, 1991. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.241268.
Testo completoPinto, Joana Isabel Monteiro. "Healthy pregnancy and prenatal disorders followed by blood plasma metabolomics". Doctoral thesis, Universidade de Aveiro, 2015. http://hdl.handle.net/10773/14784.
Testo completoThe work presented in this thesis aimed to investigate the impact of healthy pregnancy and selected prenatal disorders on the metabolome and lipidome of maternal blood plasma, in order to define new potential biomarkers for non-invasive prediction and diagnosis. Chapter 1 describes the present status and challenges of the clinically relevant prenatal disorders, along with a presentation of the metabolomics strategy applied and the state of the art of metabolomics in prenatal research. All experimental details are described in Chapter 2, comprising sample metadata, sample collection and preparation, data acquisition protocols and data analysis procedures. The plasma metabolome and lipidome viewed by 1D and 2D NMR experiments are presented in Chapter 3. In this chapter, the use of Multiple Quantum NMR spectroscopy was explored, for the first time, for assignment of complex lipid mixtures. Chapter 4 contributes to filling in some existing gaps regarding human plasma degradability during handling and storage, as well as the importance of fasting conditions at collection. The use of heparin collection tubes resulted in no interference of the polysaccharide and full conservation of spectral information, while EDTA tubes produced a number of interfering signals from free and Ca2+/Mg2+ complexed EDTA, the impact of which on metabolomic analysis is discussed. Regarding temperature stability, large changes in lipoproteins and choline compounds were observed in plasma kept at room temperature for 2.5 hours, whereas short-term storage at -20ºC was found suitable up to 7 days, with storage at -80ºC being recommended, particularly for long-term periods (at least up to 2.5 years). Regarding freeze-thaw cycles, no more than 3 consecutive cycles were found advisable, while the use of non-fasting conditions (instead of fasting) was found acceptable. Chapter 5 presents the first NMR metabolomics study of maternal plasma throughout pregnancy, including correlation between plasma and urine metabolites. Some of the metabolic alterations observed confirmed known metabolic effects, while novel changes were observed, suggesting adjustments in energy and gut microflora metabolisms (citrate, lactate and dimethyl sulfone) and alterations in glomerular filtration rate (creatine and creatinine). Correlations studies unveiled specific lipoprotein/protein metabolic aspects of healthy pregnancy with impact on the excreted metabolome, providing further understanding of pregnancy metabolism. In Chapter 6, the impact of prenatal disorders on maternal plasma metabolome and lipidome is described for fetal chromosomal disorders (CD), including Trisomy 21 (T21). High classification rates were obtained for CD (88-89%) and T21 (85-92%) in 1st and 2nd trimesters, based on variable selection of NMR data. In addition, novel metabolic deviations were found through plasma/urine correlations, namely in low density and very low density lipoproteins (LDL+VLDL), sugar and gut microflora metabolisms. Changes in plasma phospholipid profile, namely in phosphatidylcholines, were further confirmed and characterised by hydrophilic interaction liquid chromatography-mass spectrometry (HILIC-LC/MS). In Chapter 7, metabolic biomarkers of pre- and post-diagnosis GDM were sought by NMR metabolomics of whole maternal plasma and plasma lipid profile in the 2nd trimester. Metabolic alterations found to be predictive of GDM comprised increases in cholesterol, fatty acids, triglycerides and small metabolites changes in glucose, amino acids, betaine, urea, creatine and metabolites related with gut microflora. Post-diagnosis GDM was successfully classified using a 26-resonance plasma biomarker corresponding to 10 metabolites and lipids, advancing the possibility of using a multi-metabolite biomarker as a complementary tool in the clinical management of GDM. Chapter 8 describes the results obtained for prenatal disorders shown to have lower impact on maternal plasma metabolome, namely diagnosed fetal malformations and pre-diagnosis premature rupture of membranes, preterm delivery and preeclampsia. Finally, Chapter 9 describes the general conclusions and future perspectives in the context of this thesis, highlighting how this work contributes with new knowledge on prenatal disease mechanisms and possible biomarkers for prenatal diagnosis and prediction methods.
O trabalho apresentado nesta tese teve como principal objetivo investigar o impacto da gravidez saudável e algumas doenças pré-natais no metaboloma e lipidoma de plasma sanguíneo materno, com vista à definição de novos biomarcadores para a previsão e diagnóstico não invasivos daquelas doenças. O Capítulo 1 descreve a perspectiva atual e os desafios das doenças pré-natais mais relevantes, assim como a estratégia metabolómica e estado da arte na investigação pré-natal. Todos os detalhes experimentais do trabalho realizado estão descritos no Capítulo 2, incluindo as condições de amostragem, recolha e preparação das amostras, bem como os protocolos de aquisição e análise dos dados. No Capítulo 3 descreve-se o metaboloma e lipidoma de plasma detectados por RMN 1D e 2D. Neste capítulo, a utilização de espectroscopia de RMN de quantum-múltiplo foi explorada, pela primeira vez, para caracterização de misturas lipídicas complexas. O Capítulo 4 contribui para colmatar algumas falhas no conhecimento sobre a degradibilidade do plasma humano durante o manuseamento da amostra e armazenamento, e a importância de condições de colheita como o jejum. A utilização de tubos de colheita com heparina não mostrou interferência do polissacarídeo nos espectros conservando-se toda a informação espectral, enquanto que os tubos com EDTA deram origem a sinais interferentes provenientes do EDTA livre e complexado com Ca2+/Mg2+, cujo impacto na análise metabolómica é discutido. Relativamente à estabilidade do plasma à temperatura ambiente, foram observadas alterações nas lipoproteínas e compostos de colina a partir de 2.5 horas, enquanto que o armazenamento a -20ºC mostrou ser adequado até 7 dias, sendo o armazenamento a -80ºC aconselhado, particularmente para períodos de tempo longos (pelo menos até 2.5 anos). Relativamente aos ciclos de congelação-descongelação, não se aconselham mais de 3 ciclos consecutivos, enquanto que o efeito da colheita das amostras em não-jejum (em vez de jejum) foi considerado aceitável. O Capítulo 5 apresenta o primeiro estudo de metabolómica por RMN do plasma materno ao longo da gravidez, incluindo correlação entre plasma e urina. Algumas das alterações metabólicas observadas confirmaram efeitos metabólicos conhecidos, tendo outras sido observadas pela primeira vez sugerindo alterações no metabolismo energético, na microflora bacteriana (citrato, lactato e dimetil sulfona) e na taxa de filtração glomerular (creatina e creatinina). Os estudos de correlação revelaram aspetos metabólicos específicos das lipoproteínas/proteínas com impacto no metaboloma excretado. No Capítulo 6 descreve-se o impacto das doenças cromossómicas (CD), incluindo Trissomia 21 (T21) no metaboloma e lipidoma de plasma materno. Obtiveram-se elevadas taxas de classificação para CD (88-89%) e T21 (85-92%) no 1º e 2º trimestres baseadas na seleção de variáveis dos dados de RMN. A correlação de plasma e urina revelou novos desvios metabólicos, nomeadamente no metabolismo das lipoproteínas de baixa densidade e de muito baixa densidade (LDL+VLDL), dos açúcares e da microflora bacteriana. As alterações observadas no perfil de fosfolípidos do plasma, nomeadamente das fosfatidilcolinas, foram confirmadas e caracterizadas por cromatografia liquida hidrofílica acoplada a espetrometria de massa (HILIC-LC/MS). No Capítulo 7 apresentam-se os resultados obtidos na prospecção de biomarcadores metabólicos de diabetes mellitus gestacional (GDM) pré- e pós-diagnóstico por metabolómica de RMN de plasma materno do 2º trimestre. Observaram-se alterações metabólicas com poder de previsão de GDM, nomeadamente um aumento no colesterol, ácidos gordos, triglicerídeos e pequenas variações metabólicas na glucose, aminoácidos, betaína, ureia, creatina e metabolitos relacionados com a microflora bacteriana. O grupo de GDM pós-diagnóstico foi bem classificado utilizando como biomarcador um conjunto de 26 ressonâncias do espectro de plasma correspondendo a lípidos e 10 metabolitos de baixo peso molecular, sugerindo-se a possibilidade de usar este marcador conjunto na gestão clínica da GDM. O Capítulo 8 descreve os resultados obtidos para as doenças pré-natais que mostraram ter um menor impacto no metaboloma de plasma materno, nomeadamente as malformações fetais (FM), e os estados de pré-diagnóstico da rutura prematura das membranas (PROM), parto pré-termo (PTD) e pré-eclampsia. Finalmente, no Capítulo 9 são descritas as conclusões gerais e perspetivas futuras no contexto desta tese, realçando-se como este trabalho contribui para o novo conhecimento dos mecanismos das doenças pré-natais e possíveis biomarcadores para a sua previsão e diagnóstico.
Kadkhodaei-Elyaderani, Manizheh. "HPLC detection of haemoglobinopaties". Thesis, University of Salford, 1996. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.308175.
Testo completoTillfors, Maria. "Social Phobia : The Family and the Brain". Doctoral thesis, Uppsala : Acta Universitatis Upsaliensis : Univ.-bibl. [distributör], 2001. http://publications.uu.se/theses/91-554-5096-2/.
Testo completoMichelgård, Palmquist Åsa. "Positron Emission Tomography (PET) Studies in Anxiety Disorders". Doctoral thesis, Uppsala universitet, Institutionen för neurovetenskap, 2010. http://urn.kb.se/resolve?urn=urn:nbn:se:uu:diva-129713.
Testo completoPissiota, Anna. "Fear, Startle, and Fear-Potentiated Startle : Probing Emotion in the Human Brain". Doctoral thesis, Uppsala University, Department of Psychology, 2003. http://urn.kb.se/resolve?urn=urn:nbn:se:uu:diva-3479.
Testo completoThe present thesis explored the neurobiological basis of three aspects of defense behaviors in humans. Positron emission tomography methodology was used, and changes in regional cerebral blood flow (rCBF) were measured as an index of neural activity. Firstly, brain function was studied in a group of patients suffering from combat-related posttraumatic stress disorder, using a symptom provocation paradigm with combat sounds in order to elicit fear. Exposure to auditory trauma reminders relative to neutral sounds was associated with increased rCBF in sensorimotor areas, the cerebellar vermis, the periaqueductal gray matter, and the right amygdala, whereas decreased activity was observed in the retrosplenial area of the posterior cingulate cortex. Secondly, the neural circuitry mediating the acoustic startle response and its habituation was studied in a group of healthy subjects. During acoustic startle stimulation as compared to a resting condition, increased rCBF was found in a medial posterior area of the pons corresponding to the nucleus reticularis pontis caudalis. As a result of startle repetition, altered activity was found in the cerebellum, pointing to its involvement in startle habituation. Thirdly, neural activity associated with startle modulation by phobic fear was studied in a group of subjects with specific animal phobias during exposure to pictures of their feared and non-feared objects, paired and unpaired with acoustic startle stimuli. As a result of startle potentiation, increased rCBF was found in the left amygdaloid-hippocampal region, and medially in the affective division of the anterior cingulate cortex. In conclusion, these results provide evidence for the involvement of limbic and paralimbic brain areas during fear provocation and fear-potentiated startle and for a similar neurocircuitry underlying startle in humans and animals.
Shennan, Andrew Hoseason. "Ambulatory blood pressure measurement in pregnancy and pre-eclampsia". Thesis, Imperial College London, 1997. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.286663.
Testo completoO'Shaughnessy, D. F. "A study of thalassaemia and other globin gene variants in the Pacific". Thesis, University of Oxford, 1989. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.279894.
Testo completoFall, Lewis. "Redox regulation of haemostasis : modulation by inspiratory hypoxia and physical exercise". Thesis, University of South Wales, 2012. https://pure.southwales.ac.uk/en/studentthesis/redox-regulation-of-haemostasis-modulation-by-inspiratory-hypoxia-and-physical-exercise(712686ec-639c-4d2f-b779-47e1b3b21da1).html.
Testo completoLotti, Francesco. "Transcriptional targeting of lentiviral vectors to the erythroblastic progeny of hematopoietic stem cells". Thesis, Open University, 2003. http://oro.open.ac.uk/54805/.
Testo completoPinto, Joana Isabel Monteiro. "Metabonomics of the blood of pregnant women for diagnosis of prenatal disorders". Master's thesis, Universidade de Aveiro, 2010. http://hdl.handle.net/10773/3156.
Testo completoA aplicação da metabonómica na pesquisa de novos biomarcadores de doenças tem ganho um interesse crescente na investigação e desenvolvimento, tanto ao nível do processamento analítico como do tratamento de dados. Nomeadamente, a análise metabonómica usando espectroscopia de Ressonância Magnética Nuclear (NMR) fornece uma grande quantidade de dados de uma forma rápida e não invasiva sobre a composição de amostras complexas como o plasma sanguíneo. Uma vez que as doenças pré-natais têm um elevado impacto no metabolismo materno e fetal, sendo responsáveis por várias complicações durante e depois da gravidez, esta estratégia foi aplicada ao estudo destas doenças através da análise de sangue de senhoras grávidas (colhido entre 15-24 semanas de gestação), com o objectivo de investigar possíveis metabolitos marcadores ou com poder de previsão para a diabetes gestacional e malformações fetais. Num primeiro passo, foram estudados os perfis metabólicos em RMN dos controlos (n=20) e gravidezes com diagnóstico ou suspeita de malformações fetais (n=11) e pré-diabetes gestacional (com posterior diagnóstico clínico entre 22-34 semanas de gestação). A análise multivariada (análise de componentes principais, PCA; análise discriminante pelo método de mínimos quadrados parcias, (PLS-DA) e duas versões deste último, interval PLS-DA e ortogonal PLS-DA (OPLS-DA)) foram aplicados com o objectivo de pesquisar por correlações de solidez estatística entre a composição do plasma e a ocorrência das doenças em estudo. Os resultados mostraram que as amostras controlo e doença podem ser diferenciadas com base no seu perfil metabólico, nomeadamente mostrando níveis mais elevados de compostos que contêm colina em mulheres que desenvolveram diabetes gestacional mais tarde na gravidez. Adicionalmente, níveis mais elevados de piruvato, manose e compostos que contêm colina, e níveis mais baixos de vários aminoácidos e acetato foram encontrados nas gravidezes afectadas por malformações fetais. Numa segunda etapa do trabalho, as mesmas amostras foram analisadas por espectroscopia de Infravermelho com Transformadas de Fourier (FTIR), um método mais barato e acessível para eventual uso clínico. O perfil dos espectros de FTIR também revelou algumas diferenças entre controlos e doenças, no entanto a sua interpretação específica torna-se difícil devido à grande sobreposição de bandas característica de espectros de infravermelho. Estes resultados mostraram que a análise metabonómica de plasma de mulheres grávidas por RMN e FTIR pode ser uma ferramenta poderosa para obter informação bioquímica sobre a saúde pré-natal e encontrar possíveis novos marcadores com potencial para prever doenças, particularmente no caso do diabetes gestacional. ABSTRACT: The use of Metabonomics to search for new disease biomarkers has gained increasing interest in the research community and continuous developments, both at the analytical and data processing levels have boosted this area into new quests in biomarker research. Namely, Nuclear Magnetic Resonance (NMR)-metabonomics provides a large amount of compositional data on complex samples such as blood plasma, in a rapid and non-invasive manner. Since prenatal diseases have a high impact on both maternal and fetal metabolisms, being responsible for a range of complications both during and after pregnancy, this strategy was hereby applied to the study of prenatal diseases, through the analysis of blood (collected at 15-24 gestational weeks), in order to probe for possible marker/predictor metabolites for gestational diabetes and fetal malformations. In the first stage of this work, the plasma metabolic profiles of controls (n=20) and pregnancies affected by diagnosed or suspected fetal malformations (n=11) and pre-gestational diabetes (with posterior clinical diagnosis at 22-34 gestational weeks) were evaluated by NMR spectroscopy. Multivariate analysis (principal component analysis, PCA; partial least squares discriminant analysis, PLS-DA and two extended versions of the latter, interval PLS-DA (iPLS-DA) and orthogonal PLS-DA (OPLS-DA) were applied in order to search for consistent statistical correlations between plasma composition and the occurrence of the diseases. It was found that controls and diseased subjects could be differentiated with basis on their plasma profile, namely showing higher levels of choline-containing compounds in pregestational diabetic women. In addition, higher contents of pyruvate, mannose and choline-containing compounds and lower contents of several amino acids and acetate were found in pregnancies affected by fetal malformations. In a second stage of the work, the same samples were analysed by Fourier Transform Infrared (FTIR) spectroscopy, a cheaper and more-accessible method, more suited to straightforward clinical use. The FTIR spectral profiles also revealed some differences between controls and diseased subjects, the interpretation of which posing a harder challenge than that of NMR. These results have shown that NMR and FTIR metabonomics of pregnant women blood plasma may be a powerful tool to gain insight into prenatal diseases and find possible new markers with potential predictive value, particularly in the case of gestational diabetes.
Hawdon, Jane Melinda. "Metabolic adaptation and disordered blood glucose homeostasis in the neonate". Thesis, University of Newcastle Upon Tyne, 1995. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.240735.
Testo completoChurchill, David. "Twenty four hour ambulatory blood pressure monitoring in pregnancy". Thesis, University of Birmingham, 1995. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.391325.
Testo completoAnsari, Mohammed Toseef. "Changes in coagulation, fibrinolysis, and endothelial perturbation markers in the lower limb venous blood associated with prolonged cramped sitting in healthy adult male volunteers in a simulation of prolonged travel". Click to view the E-thesis via HKUTO, 2005. http://sunzi.lib.hku.hk/hkuto/record/B31556991.
Testo completoDarr, Aamra Rashid. "The social implications of thalassaemia major among Muslims of Pakistani origin : family experience and service delivery". Thesis, University College London (University of London), 1991. http://discovery.ucl.ac.uk/1317782/.
Testo completoWilson, James L. "Development of functional magnetic resonance imaging at high field for neuro-psychiatric disorders". Thesis, University of Oxford, 2003. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.275200.
Testo completoSegura, Castell Mónica. "Peripheral blood biomarkers in Psychiatric Diseases". Doctoral thesis, Universitat Internacional de Catalunya, 2012. http://hdl.handle.net/10803/83727.
Testo completoActualment, hi ha una forta incidència de les patologies psiquiàtriques, representant un 13% del total de les malalties i 450 milions de persones afectades. L’etiologia de les patologies psiquiàtriques és desconeguda. Tot i així, evidències científiques suggereixen un mal desenvolupament del sistema nerviós (SN). El diagnòstic és poc precís, i els manuals internacionals (ICD-10 i DSM-IV) identifiquen les patologies d’acord a un llistat de símptomes, però sense cap causa biològica subjacent de la patologia. L’objectiu de la tesi és la identificació de biomarcadors potencials –relacionats en el desenvolupament del SN- en sang perifèrica de pacients diagnosticats amb diferents patologies mentals, com ara els trastorns de l’espectre autista (TEA), esquizofrènia i desordres bipolars. És pretén contribuir amb la millora del diagnòstic, el pronòstic i el tractament de les persones que les pateixen. La tesi s’estructura en 4 capítols: 1) estudi de les neurotrofines en els TEA, on els resultats evidencien la relació d’aquesta família de molècules amb la patologia, 2) estudi de la Latrofilina-3 (LPHN3) en els TEA, on s’ha obtingut associació amb el nivell cognitiu més baix dels TEA, 3) estudi del receptor EPH A4 en les patologies d’esquizofrènia i desordres bipolars, resultats del qual no mostren associació i, per últim 4) estudi de la Ankirina-3 (ANK3) en l’esquizofrènia i els desordres bipolars, en el qual si que es troba una relació amb els desordres bipolars, però no amb l’esquizofrènia.
Actualmente, hay una fuerte incidencia de las patologías psiquiátricas, representando un 13% del total de las enfermedades y 450 millones de personas afectadas. La etiología de las patologías psiquiátricas es desconocida. Aún así, evidencias científicas sugieren un mal desarrollo del sistema nervioso (NS). El diagnóstico es poco preciso, y los manuales internacionales (ICD-10 y DSM-IV) identifican las patologías de acuerdo a un listado de síntomas, pero sin ninguna causa biológica subyacente de la patología. El objetivo de la tesis es la identificación de biomarcadores potenciales –relacionados con el desarrollo del SN- en sangre periférica de pacientes diagnosticados con diferentes patologías mentales, como son los trastornos del espectro autista (TEA), esquizofrenia y desordenes bipolares. Se pretende contribuir en la mejora del diagnóstico, el pronóstico i el tratamiento de las personas que las padecen. La tesis se estructura en 4 capítulos: 1) estudio de las neurotrofinas en los trastornos del espectro autista (TEA), en el cual los resultados evidencian la relación de esta familia de moléculas con la patología, 2) estudio de la Latrofilina-3 (LPHN3) en los TEA, donde se ha obtenido una asociación con el nivel cognitivo más bajo de los TEA, 3) estudio del receptor EPH A4 en las patologías de la esquizofrenia y los desordenes bipolares, resultados del cual no muestran asociación y, por último 4) estudio de la Ankirina-3 (ANK3) en la esquizofrenia y los desordenes bipolares, en el cual si que se ha encontrado una relación con los desordenes bipolares, pero no con la esquizofrenia.
Goldenberg, Neil A. "Development of the clot formation and lysis (CloFAL) global assay and its application to the investigation of bleeding disorders in children and adults /". Connect to abstract via ProQuest. Full text is not available online, 2008. http://proquest.umi.com/pqdweb?did=1545571881&sid=1&Fmt=2&clientId=18952&RQT=309&VName=PQD.
Testo completoTypescript. Includes bibliographical references (leaves 136-146). Free to UCD Anschutz Medical Campus. Online version available via ProQuest Digital Dissertations;
Wettergren, Lena. "Quality of life in patients with malignant blood disorders : a clinical and methodological study /". Stockholm : [Karolinska institutets bibl.], 2002. http://diss.kib.ki.se/2002/91-7349-365-1/.
Testo completoSlick, Nichole. "Implementing Shared-Decision Making: Factors Present with Adolescents and Young Adults with Blood Disorders". Kent State University / OhioLINK, 2021. http://rave.ohiolink.edu/etdc/view?acc_num=kent1619092978581083.
Testo completoMurugan, Brandon Dean. "Proteomic investigation of blood-based biomarkers for the diagnosis of HIV-associated neurocognitive disorders". Master's thesis, University of Cape Town, 2015. http://hdl.handle.net/11427/16722.
Testo completoBackground: South Africa has the fourth highest prevalence of Human Immunodeficiency Virus (HIV) in the world, with over 340 000 new infections in 2013 alone. Implementation of Highly Active Antiretroviral Treatment (HAART) regimens, has improved the lives of many HIV-infected individuals, and has led to a decrease in the incidence of extreme forms of HIV-associated dementia. However, the extended lifespan afforded by HAART has also resulted in an increase in the prevalence of milder forms of HIV-associated Neurocognitive Disorders (HAND). Clinical diagnosis of such cognitive decline currently relies on neurocognitive assessments, as no definitive biochemical test exists. A point-of-care test designed for use with easily accessible samples (e.g. blood) would be of great utility in both HAND research and clinical diagnosis, prognostication, and provision of timeous therapy. A blood-based biomarker test would also be less subjective than neurocognitive testing, which can be adversely affected by the patient's level of education as well as operator competency. Recently, Professor Simon Lovestone (University of Oxford) developed a panel of blood-based biomarkers for the diagnosis of Alzheimer's disease. Due to pathological similarities between HAND and Alzheimer's disease, it is hypothesised that there may be applicability of this panel to diagnosis of HAND. The differential protein expression profile of patients with and without HAND is thus compared. Aims and Objectives: The aim of this study was to assess the applicability of a set of Alzheimer's disease biomarkers to the diagnosis of HAND. In order to achieve this, targeted proteomic assays were developed to measure the markers in human serum. This assay was then applied to defined patient cohorts. Methods: Targeted proteomic assays were developed in order to quantify candidate markers in patient blood serum. Parallel Reaction Monitoring assays were developed on a Thermo Q Exactive Quadrupole-Orbitrap mass spectrometer, for application to defined patient samples collected from Groote Schuur Hospital (Cape Town, South Africa). Patient samples were divided into groups according to HAND severity (based on the HIV Dementia Scale), namely: Normal (HIV+), Minor Neurocognitive Disorders and HIV-associated Dementia. Discovery proteomic analysis was performed on pooled patient samples in order to determine the optimal peptides for identification and quantitation of candidate proteins. Targeted methods were then developed and refined using the same pooled samples. Finally, patient samples (N=81) from the three classes were analysed in a statistically rigorous manner. Data were normalised to correct for possible loading inconsistencies by two independent methods. Quantitative differences were investigated using t-tests and non-parametric statistical tests where appropriate. Results: Statistical assessment of final data indicated no significant differences in proteins between patient classes. Discussion and Conclusions: It is likely that the inflammatory nature of HIV itself influences the levels of these markers in HIV-positive patient samples to a greater degree than neurocognitive effects. Alternatively, possible co-infection by TB may have confounded the results. Regardless, it was concluded that the candidate Alzheimer's biomarkers were not applicable to diagnosis of HAND. Further analysis on a larger sample cohort is recommended, utilising the assays optimised herein. Prospective studies to obtain viable biomarkers for definitive diagnosis may lie in proteomic analysis of model infection systems and cerebrospinal fluid.
Jenkins, Meredith E. "An examination of the human fibrinogen-like protein2 sequence variations and genetic expression by human endothelial cells /". unrestricted, 2005. http://etd.gsu.edu/theses/available/etd-07222005-093438/.
Testo completoTitle from title screen. Roberta Attanasio, committee chair; P.C. Tai, W.C. Hooper, committee members. Electronic text (57 p. : col. ill.) : digital, PDF file. Description based on contents viewed Aug. 15, 2007. Includes bibliographical references (p. 55-57).
Ungerstedt, Johanna S. "Coagulation and inflammation in experimental endotoxemia in vitro and in vivo : monitoring method and effects of nicotinamide /". Stockholm, 2003. http://diss.kib.ki.se/2003/91-7349-477-1/.
Testo completoBrooks, Mirella. "Health Related Hardiness and Psychosocial Adaptation in Individuals With Inherited Bleeding Disorders and Other Chronic Illnesses". Diss., University of Hawaii at Manoa, 2005. http://hdl.handle.net/10125/22046.
Testo completoAnsari, Mohammed Toseef. "Changes in coagulation, fibrinolysis, and endothelial perturbation markers in the lower limb venous blood associated with prolongedcramped sitting in healthy adult male volunteers in a simulation ofprolonged travel". Thesis, The University of Hong Kong (Pokfulam, Hong Kong), 2005. http://hub.hku.hk/bib/B31556991.
Testo completoXie, Bingjiao, e 謝冰姣. "Association of arterial stiffness and blood pressure variability with silent brain lesions in healthy hypertensive elderly Chinese". Thesis, The University of Hong Kong (Pokfulam, Hong Kong), 2015. http://hdl.handle.net/10722/212629.
Testo completoTaylor, James Michael. "Validation of a new method for platelet HPA-1 phenotyping". Virtual Press, 1999. http://liblink.bsu.edu/uhtbin/catkey/1133736.
Testo completoDepartment of Biology
Wang, Qin. "Short Term Trend Analysis of Hospital Admissions Due to Red Blood Cell Disorders: Big Data Perspective". University of Cincinnati / OhioLINK, 2015. http://rave.ohiolink.edu/etdc/view?acc_num=ucin1428070351.
Testo completoLilliehöök, Inger. "Studies of blood eosinophil and neutrophil granulocytes in healthy and diseased dogs /". Uppsala : Swedish Univ. of Agricultural Sciences (Sveriges lantbruksuniv.), 1999. http://epsilon.slu.se/avh/1999/91-576-5409-3.pdf.
Testo completoCheng, Xi. "Prevalence, profile, predictors, and natural history of aspirin resistance measured by the ultegra rapid platelet function assay-asa in patients with coronary artery disease". Click to view the E-thesis via HKUTO, 2005. http://sunzi.lib.hku.hk/hkuto/record/B33708708.
Testo completoPedersen, Cameron James. "Biophotonic Investigation of Cardiac Structure and Hemodynamics During Embryogenesis UsingOptical Coherence Tomography". Case Western Reserve University School of Graduate Studies / OhioLINK, 2020. http://rave.ohiolink.edu/etdc/view?acc_num=case1575392583935489.
Testo completoWeidung, Bodil. "Blood pressure in very old age : determinants, adverse outcomes, and heterogeneity". Doctoral thesis, Umeå universitet, Geriatrik, 2016. http://urn.kb.se/resolve?urn=urn:nbn:se:umu:diva-128713.
Testo completoBakgrund: Högt blodtryck är den största bidragande orsaken till sjukdom och död i världen. Man har ännu inte fastslagit om högt blodtryck ökar risken för sjukdom och död även i mycket hög ålder, vilket kan definieras som 80 år och äldre. Detta beror bland annat på att endast en liten andel av forskningen hittills har fokuserat på den här åldersgruppen. Mycket gamla människor skiljer sig från yngre på olika sätt som skulle kunna påverka riskerna med högt blodtryck. Till exempel är det vanligare med sjukdomar och att ha många samtidiga sjukdomstillstånd bland mycket gamla människor än i yngre åldersgrupper. Då andelen mycket gamla människor i befolkningen ökar kraftigt får dessa frågor allt större betydelse. Det är vanligt med sjunkande blodtryck i mycket hög ålder, något som verkar föregå sjukdom och död. Tidigare studier har funnit att sjunkande blodtryck skulle kunna bero på ökande sjuklighet, högre ålder och högre begynnelseblodtryck. Man vet ännu inte vilka enskilda faktorer som bäst förklarar blodtrycksförändringen i mycket hög ålder, oberoende av andra faktorer. Tidigare studier har visat att lägre blodtryck kan vara förenat med en ökad risk för tidig död bland mycket gamla människor. Det är oklart om risken för tidig död bättre kan förklaras av andra faktorer, s.k. störfaktorer. Störfaktorer kan till exempel vara sjukdomar som både påverkar blodtrycket och risken. Fynd från tidigare studier av personer som är minst 65 år tyder på att sambandet mellan blodtryck och död kan skilja sig mellan grupper med hög eller låg gånghastighet, vilket används som ett ungefärligt mått på hälso-tillståndet. Detta skulle även kunna ha betydelse för mycket gamla människor eftersom deras hälsotillstånd kan skilja sig mycket mellan individer. Man har också utrett huruvida sambandet mellan blodtryck och död skiljer sig mellan grupper med och utan kognitiv svikt, som till exempel kan bero på demenssjukdom, men inte kommit fram till entydiga resultat. Ett fåtal studier har utrett strokerisken med högt blodtryck i mycket hög ålder. På grund av motsägelsefulla resultat är det ännu oklart om högt blodtryck ökar risken för stroke bland mycket gamla människor. Man har sett tecken på att sambandet mellan blodtryck och strokerisk skulle kunna skilja sig mellan grupper av mycket gamla människor med och utan kognitiv svikt, samt mellan grupper med och utan hjälpbehov i dagliga aktiviteter. Dagliga aktiviteter innefattar bland annat att tvätta sig, klä sig, gå på toaletten, äta och resa sig från en stol. Frågeställningar: I den här avhandlingen undersöktes huvudsakligen tre frågeställningar. Den första var vilka faktorer som påverkar hur blodtrycks-nivåerna förändras över tid i mycket hög ålder. Den andra frågeställningen var om olika blodtrycksnivåer är förenade med ökad risk för tidig död i mycket hög ålder och huruvida risken skiljer sig mellan grupper av mycket gamla människor med olika gånghastighet eller olika grader av kognitiv svikt. Den tredje frågeställningen var om olika blodtrycksnivåer är förenade med ökad risk för stroke i mycket hög ålder och om risken skiljer sig mellan grupper av mycket gamla människor med och utan kognitiv svikt eller hjälpbehov i dagliga aktiviteter. Även skillnader mellan gånghastighets-grupper testades. Metod: Avhandlingen bygger på befolkningsmaterialet Umeå85+/Gerontologisk regional databas (GERDA). Umeå85+/GERDA innehåller information från individer i åldrarna 85, 90 och 95 år och äldre, boende i Västerbotten, Sverige och Österbotten/Pohjanmaa, Finland. Informationen är insamlad vart femte år under perioden 2000-2015. Umeå85+/GERDA innehåller information om socioekonomiska faktorer, sjukdomar och läkemedel. Informationen inhämtades med hjälp av ett standardiserat frågeformulär som deltagarna besvarade under ett hembesök, samt med hjälp av journaler, boendepersonal och anhöriga. Det gjordes även hälsorelaterade mätningar och tester under hembesöken, bl.a. av blodtryck och gånghastighet i vanlig takt. Skattningsskalorna Mini-Mental State Examination (MMSE) och Barthel Activities in daily living (ADL) index användes för att skatta kognitiv funktion respektive hjälpbehov i dagliga aktiviteter. Deltagarna delades in i två gånghastighetsgrupper. Personer med högre gånghastighet (minst 0,5 m/s) utgjorde en grupp. I den andra gruppen var personer med lägre gånghastighet (under 0,5 m/s) och de som inte klarade av att genomföra testet på grund av bestående begränsningar av gångfunktionen. Deltagarna grupperades också med avseende på olika grader av kognitiv svikt. Gruppindelningen baserades på MMSE-poäng; mycket svår kognitiv svikt (0-10 poäng), svår kognitiv svikt (11-17 poäng) och mild kognitiv svikt (18-23 poäng). Deltagare utan kognitiv svikt utgjorde en egen grupp (24-30 poäng). Deltagarna delades även in i grupper med och utan hjälpbehov i dagliga aktiviteter, baserat på Barthel ADL index (under 20 respektive 20). Blodtrycksförändring observerades över tiden mellan två Umeå85+/GERDA-insamlingar, vilket var 5 år. Dödsdatum och datum för stroke inhämtades från dödsbevis, befolkningsregister, journaler och sjukvårdens diagnoskodsregister i upp till 5 år. Frågeställningarna utreddes med hjälp av statistiska metoder, baserat på materialet från Umeå85+/GERDA. Sambanden prövades med avseende på störfaktorer och skillnader mellan grupper. Resultat: Förändringar av det systoliska blodtrycket undersöktes bland 297 deltagare. I genomsnitt sjönk blodtrycket med 2,6 mm Hg per år. För nästan två tredjedelar (62%) av deltagarna sjönk blodtrycket med minst 5 mm Hg på 5 år. Ungefär en fjärdedel (26%) hade minst 5 mm Hg stigande blodtryck på 5 år. Ett antal faktorer var förenade med förändring av det systoliska blodtrycket över 5 år, oberoende av varandra. Sjunkande systoliskt blodtryck var förenat med ett högre begynnelseblodtryck, senare undersökningsår, att ha antidepressiv behandling, att få en hjärtinfarkt, att påbörja läkemedels-behandling med diuretika eller få ökat hjälpbehov i dagliga aktiviteter. Man vet ännu inte vad som är orsak och verkan i dessa samband. Frågeställningen om olika blodtrycksnivåer är förenade med ökad risk för tidig död undersöktes i ett urval av 806 deltagare. Inom 5 år avled nästan två tredjedelar (61%) av deltagarna. Risken för tidig död var mindre bland deltagare med högre blodtryck, jämfört med dem som hade lägre blodtryck. Största skillnaden uppmättes mellan deltagare med minst 165 mm Hg i systoliskt blodtryck, där risken var halverad, jämfört med dem som hade 125 mm Hg eller lägre. Detta samband verkar bero på störfaktorer, främst sjukdomar, som både orsakar lågt blodtryck och den ökade risken för tidig död. Gånghastighetsgrupperna utgjordes av 312 deltagare med högre gånghastighet och 433 med lägre gånghastighet, varav 136 inte kunde genomföra mätningen på grund av bestående begränsning av gångfunktionen. Sambandet mellan blodtryck och risken att dö inom 5 år verkade skilja sig mellan gånghastighetsgrupperna. Gruppen med lägre gånghastighet uppvisade samma samband som hela urvalet och hade ökad risk för tidig död med lägre blodtryck. Även här verkade sambandet förklaras av störfaktorer. Personer med högre gånghastighet uppvisade ett annat samband, där högre systoliskt blodtryck på minst 165 mm Hg var förenat med en fördubblad risk för tidig död, jämfört med 126-139 mm Hg. Högre diastoliskt blodtryck på över 80 mm Hg var också förenat med ökad risk för tidig död, jämfört med 75-80 mm Hg. Sambandet berodde inte på störfaktorer. Grupperna med svår, måttlig och mild kognitiv svikt innehöll 118, 166 och 289 deltagare vardera. Gruppen utan kognitiv svikt innehöll 542 deltagare. Dessa grupper verkade också skilja sig något med avseende på sambandet mellan blodtryck och risken för tidig död, men skillnaderna var inte statistiskt säkerställda. Särskilt gruppen med mycket svår kognitiv svikt uppvisade ett annorlunda samband mellan systoliskt blodtryck och risken för tidig död, jämfört med övriga deltagare. Bland dessa deltagare var risken för tidig död mer än fyrdubblad med höga blodtryck på minst 165 mm Hg, jämfört med 126-139 mm Hg. De med blodtryck 125 mm Hg eller lägre hade dubbelt så hög risk för tidig död, jämfört med 126-139 mm Hg. Dessa samband var oberoende av störfaktorer. Frågeställningen om strokerisk med högt blodtryck utreddes i ett urval av 955 deltagare. Inom 5 år fick 94 deltagare en stroke, vilket motsvarar en av tio. Högre blodtryck var förenat med ökad risk för stroke, jämfört med lägre blodtryck. Risken att få en stroke inom 5 år var fördubblad bland deltagare med högt systolisk blodtryck på minst 160 mm Hg, jämfört med under 140 mm Hg, eller med höga diastoliska blodtryck på minst 90 mm Hg, jämfört med under 90 mm Hg. Sambanden var oberoende av en mängd andra riskfaktorer. Strokerisken med högt blodtryck verkade inte påverkas av gånghastigheten, den kognitiva nivån, eller hjälpbehovet i dagliga aktiviteter. Slutsatser: Blodtrycket verkar sjunka hos de flesta i mycket hög ålder. Sjunkande systoliskt blodtryck kan till stor del förklaras av högre begynnelseblodtryck, senare undersökningsår, att ha antidepressiv läkemedelsbehandling, att få en hjärtinfarkt, att påbörja läkemedels-behandling med diuretika eller få ökat hjälpbehov i dagliga aktiviteter. Lågt blodtryck verkar i mycket hög ålder vara ett tecken på olika underliggande sjukdomsprocesser, som ökar risken att dö inom 5 år. Detta samband verkar särskilt gälla personer med lägre gånghastighet, vilket kan vara ett tecken på sämre hälsa. Högt blodtryck verkar endast vara förenat med ökad risk för tidig död i särskilda grupper, som kan utmärkas av högre gånghastighet eller mycket svår kognitiv svikt. Även lågt systoliskt blodtryck kan vara förenat med ökad risk för tidig död bland personer med mycket svår kognitiv svikt. I dessa grupper kan sambandet vara oberoende av störfaktorer. Högre blodtryck verkar vara förenat med ökad risk för stroke i mycket hög ålder, oberoende av en mängd andra sjukdomstillstånd. Det finns sannolikt en gräns för hur lågt blodtryck som är gynnsamt med avseende på strokerisken, men det är ännu inte klarlagt var den gränsen går. Sambandet mellan högt blodtryck och strokerisk verkar inte skilja sig mellan grupper med olika hög gånghastighet, kognitiv nivå, eller hjälpbehov i dagliga aktiviteter. Dessa fynd kan bidra till en bättre förståelse för blodtrycksförändring, risker med högt och lågt blodtryck i mycket hög ålder samt hälsotillståndets betydelse för dessa risker.
Schwartz, Sari D. "Atypical depression, body mass, and left vetricular mass analysis of data from CARDIA /". Download the thesis in PDF, 2005. http://www.lrc.usuhs.mil/dissertations/pdf/Schwartz2005.pdf.
Testo completoKnöfler, Ralf, e Werner Streif. "Strategies in Clinical and Laboratory Diagnosis of Inherited Platelet Function Disorders in Children". Saechsische Landesbibliothek- Staats- und Universitaetsbibliothek Dresden, 2014. http://nbn-resolving.de/urn:nbn:de:bsz:14-qucosa-136597.
Testo completoAngeborene Thrombozytenfunktionsstörungen stellen eine seltene und heterogene Gruppe von Erkrankungen dar, welche meist durch eine leichte bis mittelschwere Blutungsneigung auffallen. Typische Blutungssymptome sind Hämatomneigung, Epistaxis, Menorrhagien sowie Schleimhaut- und perioperative Blutungen. Die Durchführung der Thrombozytenfunktionsdiagnostik bei Kindern wird erschwert durch die altersabhängig begrenzte Blutprobenmenge, schwierige Venenverhältnisse und das Fehlen von Referenzbereichen für Kinder unterschiedlichen Alters. Aufgrund der meist komplizierten und zeitaufwendigen Tests ist die Thrombozytendiagnostik auf spezialisierte Zentren begrenzt. Mit hoher Wahrscheinlichkeit wird eine relevante Anzahl von Kindern mit nichtdiagnostizierten bzw. unkorrekt klassifizierten, klinisch relevanten Thrombozytopathien übersehen. Die Erhebung der Blutungsanamnese und die Bewertung der Blutungssymptome sind erforderlich für eine stufenweise erfolgreiche Gerinnungsdiagnostik. Vor Durchführung einer Thrombozytenfunktionsdiagnostik sollten das Vorliegen einer Thrombozytopenie, einer von-Willebrand-Erkrankung und sekundärer Gerinnungsstörungen ausgeschlossen werden. Die Lichttransmissionsaggregometrie gilt noch immer als Standardmethode für die Beurteilung der Thrombozytenfunktion. Nach Möglichkeit sollte stets versucht werden, den vorliegenden spezifischen Thrombozytenfunktionsdefekt zu klassifizieren, da dies für eine adäquate Behandlung und eine gezielte genetische Beratung notwendig ist
Dieser Beitrag ist mit Zustimmung des Rechteinhabers aufgrund einer (DFG-geförderten) Allianz- bzw. Nationallizenz frei zugänglich