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  • About
  • The Global ETD Search service is a free service for researchers to find electronic theses and dissertations. This service is provided by the Networked Digital Library of Theses and Dissertations.
    Our metadata is collected from universities around the world. If you manage a university/consortium/country archive and want to be added, details can be found on the NDLTD website.
431

FcRn-mediated IgG recycling in macrophages is a driver of cardiometabolic disease

Zahr, Tarik January 2024 (has links)
Immunoglobulins are key mediators of humoral immunity and can be appreciated in an isotype-dependent manner in autoimmune diseases, and to an extent, immune-mediated metabolic diseases. The most common isotype is Immunoglobulin G (IgG), yet there is little understanding of the role IgG plays in the pathogenesis of macrophage-driven metabolic disorders like atherosclerosis, metabolic dysfunction-associated steatotic liver disease (MASLD), and metabolic dysfunction-associated steatohepatitis (MASH). The contents of this dissertation introduce IgG as an activator of the macrophage inflammasome and its deposition in atherosclerotic plaques and fatty livers as a driver of disease progression. The presence of IgG in these depots and its accumulation is dictated by the neonatal Fc receptor (FcRn) in macrophages. IgG levels are known to be determined by recycling, especially in macrophages, rather than by production, and FcRn, encoded by the gene Fcgrt, is the sole receptor responsible. Interestingly, we uncover a myriad of roles for FcRn involved in regulating the biological properties of macrophages, such as their transcriptional and secretory profiles and their polarization amidst an immune response. Taken together, we identify FcRn as a hitherto unknown contender in the manipulation of macrophage function and regulation of IgG in the development of macrophage-associated cardiometabolic diseases using a multitude of methodologies. These findings highlight the importance of macrophage IgG recycling in metabolism and may warrant the potential to explore this phenomenon for therapeutic pursuits.
432

The relationship of dietary beta-carotene intake and serum beta- carotene levels to the development of oral lesions in smokeless tobacco users

Carcaise-Edinboro, Patricia 14 April 2009 (has links)
This study was designed to assess the relationship of dietary and serum beta-carotene to the development of oral lesions in smokeless tobacco users. Eighty eight smokeless tobacco users without oral lesions and 18 with lesions participated in the study. Dietary intake of beta-carotene, personal health habits and selected dietary intake were analyzed by questionnaire. Serum levels were assessed by high pressure liquid chromotography. No correlation between dietary beta-carotene intake and serum beta-carotene levels was observed. Results of t-test analysis indicated no significant difference in the mean serum or dietary intake of beta-carotene between the groups. Mean serum beta-carotene for group-I, users without oral lesions and group-2, users with oral lesions were 12.3 ug/dl(I.02 SE), and 10.6 ug/dl(1.59 SE), respectively. Stepwise regression techniques were employed to assess the influence of selected variables on serum beta-carotene. The effects of smoking, smokeless tobacco exposure, alcohol consumption, and age as well as other dietary indices were evaluated. Age (1.015,p<0.001) was the only factor found to influence serum beta-carotene levels. The small sample size and variability within groups may have decreased the likelihood of observing statistical significance for serum beta-carotene between groups. / Master of Science
433

Early marginal bone loss around dental implants: a retrospective cohort

Alyaeesh, Abdulaziz 20 June 2024 (has links)
AIM: To evaluate marginal bone loss around dental implants at the 2nd stage abutment surgery and retrospectively evaluate the association of pre-surgical variables. MATERIAL AND METHODS: Eighty-seven subjects (41 Males and 46 females) were enrolled in this cohort. The subjects' ages ranged from 23 to 80 years. Two endosseous implant brands were utilized: Nobel Biocare and Straumann Bone Level . Clinical measurements (mesial, distal, buccal, and lingual) were recorded from the coronal margin of the implant platform to the bone margin with a periodontal probe (Williams periodontal probe, Hu-Friedy) at the time of implant placement and at the 2nd stage abutment surgery. The pre-surgical variables (medication intake, implant site, bone graft volume, membrane type, and smoking) were evaluated using Chi-square test. RESULTS: The marginal bone loss (MBL) difference was calculated. The Mean clinical MBL: Mesial = 0.71 mm, Distal = 0.56mm, Buccal/Labial = 0.65 mm, and Lingual/Palatal = 0.56 mm. The test showed no statistically significant difference between test and control subjects in each of the variables, with the exception of thyroid medication. A statistically significant (P value = 0.011) association was found between levothyroxine and MBL at the mesial measurement. CONCLUSION: This limited cohort study suggests that medication-controlled hypothyroidism patients may experience an increased risk of marginal alveolar bone loss around dental implants at the 2nd stage abutment surgery. The final determination will be recalculated when the study population reaches the estimated requirement of 200 subjects.
434

Studies relating to fecapentaene-12

Piccariello, Thomas January 1989 (has links)
The glyceryl enol ether fecapentaene-12 (FP-12) is a direct-acting mutagen that is formed by bacteria in the lower part of the gastrointestinal tract from a precursor of unknown structure. Two major unsolved questions concerning FP-12 are the structure of its precursor and the nature of its interaction (if any) with DNA. The structure of the biosynthetic precursor of FP-12 is thought to be that of a plasmalogen with an intact pentaenyl ether moiety. A synthesis of the perhydro analog of the proposed precursor structure is described, and approaches to the synthesis of the precursor itself are also described. Comparison of chromatographic data for the saturated model precursor and natural precursor provided evidence for the structure of the latter. The nature of the interactions of FP-12 with DNA was probed by model studies of the reaction of nucleoside bases with FP-12 and two proposed FP-12 metabolites. No adducts were formed between FP-12 or between the various putative polyenal metabolites and guanosine, cytosine, or thymidine. A model epoxy ether did react with a guanosine derivative, however, indicating that an epoxy ether derivative of FP-12, if formed, would be capable of reacting with DNA. / Ph. D.
435

Innovations in Functional Data Analysis with Applications in Neuroscience and Women's Health

Stoms, Madison Emily January 2024 (has links)
Functional data analysis (FDA) offers a robust statistical framework for handling complex data arising from a variety of fields. The presented dissertation focuses on the development and application of innovative FDA methods to analyze scientific data. We introduce three novel approaches tailored to distinct health-related topics: the mechanisms of neural activation during skilled movement and the role of the menstrual cycle in clinical studies performed on women. In the realm of neuroscience, we propose a functional clustering method designed to analyze high-dimensional, temporal data collected across multiple trials of varying conditions. Leveraging two datasets involving motor neuron behavior in mice, our method identifies latent neuron subgroups and conducts group-specific dimensionality reduction. Through simulations and real-data analyses, we demonstrate the method's efficacy in capturing subtle differences between groups, offering insights into the underlying mechanisms of voluntary movement. Turning to women's health, we address the often-overlooked effects of the menstrual cycle in clinical research. We develop a method to estimate menstrual cycle day using hormone values derived from a single spot urine sample. We leverage patterns of hormonal variation obtained from two sources of data, which follow a collection of women across a full cycle. Through simulations and real data applications, we demonstrate our ability to obtain accurate estimations of cycle day within three days of the truth in optimal settings. This work paves the way for improved model accuracy and statistical power in clinical studies performed on women. Furthermore, we propose an innovative analysis strategy to model menstrual cycle day as an effect modifier on the relationship between hormone levels and breast cancer risk, providing insights into the cyclic variations of hormone levels and their implications on breast cancer etiology. This dissertation aims to advance our understanding of complex health-related processes and empower clinicians and researchers to develop more personalized interventions. The dissertation structure comprises detailed chapters discussing the development, application, and results of each method, highlighting the pivotal role of functional data analysis in advancing scientific research and discovery.
436

Testing a dual process model in understanding the development of binge eating behaviors among Chinese adolescent boys and girls in Hong Kong. / Dual process model

January 2001 (has links)
Tang Wai-yee. / Thesis (M.Phil.)--Chinese University of Hong Kong, 2001. / Includes bibliographical references (leaves 51-61). / Abstracts in English and Chinese.
437

Molecular epidemiology of human papillomavirus infection in Chinese women with cervical cancer and precancerous lesions.

January 2000 (has links)
by Chan Pui Chung, Denise. / Thesis (M.Phil.)--Chinese University of Hong Kong, 2000. / Includes bibliographical references (leaves 119-135). / Abstracts in English and Chinese. / ACKNOWLEDGEMENTS --- p.i / ABSTRACT --- p.iii / ABSTRACT (CHINESE VERSION) --- p.v / TABLE OF CONTENTS --- p.vi / LIST OF TABLES --- p.x / LIST OF FIGURES --- p.xii / LIST OF ABBREVIATIONS --- p.xiv / Chapter CHAPTER 1 --- INTRODUCTION --- p.1 / Chapter 1.1 --- Biology of Human Papillomaviruses --- p.2 / Chapter 1.1.1 --- Taxonomy --- p.2 / Chapter 1.1.2 --- Genomic organisation --- p.2 / Chapter 1.1.3 --- "Types, subtypes and variants" --- p.4 / Chapter 1.2 --- Epidemiology of cervical cancers --- p.6 / Chapter 1.2.1 --- Incidence --- p.8 / Chapter 1.2.2 --- Cervical cancers screening programme --- p.10 / Chapter 1.3 --- Association between human papillomavirus and cervical cancers --- p.11 / Chapter 1.3.1 --- Infection --- p.11 / Chapter 1.3.2 --- Multistep pathogenesis of cervical cancers --- p.13 / Chapter 1.3.3 --- Geographical distribution --- p.14 / Chapter 1.3.4 --- Age distribution of HPV infection --- p.15 / Chapter 1.3.5 --- Oncogenic property of HPV --- p.15 / Chapter 1.3.6 --- Sequence variation --- p.20 / Chapter 1.4 --- Project design --- p.23 / Chapter CHAPTER 2 --- MATERIALS AND METHODS --- p.25 / Chapter 2.1 --- Evaluation of HPV DNA extraction methods for paraffin-embedded tissues --- p.26 / Chapter 2.1.1 --- Study population --- p.26 / Chapter 2.1.2 --- Paraffin-embedded tissue collection --- p.26 / Chapter 2.1.3 --- DNA extraction --- p.26 / Chapter 2.1.3.1 --- Phenol-chloroform extraction --- p.27 / Chapter 2.1.3.2 --- Microwave extraction --- p.28 / Chapter 2.1.3.3 --- QIAGEN spin column extraction --- p.28 / Chapter 2.1.4 --- PCR amplification --- p.29 / Chapter 2.1.4.1 --- PCR amplification for human beta-globin gene --- p.29 / Chapter 2.1.4.2 --- PCR amplification for HPV DNA --- p.30 / Chapter 2.1.5 --- Optimisation of PCRs --- p.30 / Chapter 2.1.5.1 --- Optimisation of beta-globin PCRs --- p.30 / Chapter 2.1.5.2 --- Optimisation of HPV PCRs --- p.31 / Chapter 2.1.5.3 --- Analytical sensitivity of PCRs --- p.31 / Chapter 2.1.5.3.1 --- Analytical sensitivity of beta-globin PCRs --- p.31 / Chapter 2.1.5.3.2 --- Analytical sensitivity of HPV PCRs --- p.32 / Chapter 2.1.5.4 --- Detection of PCR products --- p.32 / Chapter 2.1.6 --- PCR evaluation of DNA extraction methods --- p.33 / Chapter 2.1.6.1 --- Beta-globin PCRs --- p.33 / Chapter 2.1.6.2 --- HPV PCRs --- p.33 / Chapter 2.1.6.2.1 --- MY09/MY11 PCR --- p.33 / Chapter 2.1.6.2.2 --- GP5+/GP6+ PCR --- p.34 / Chapter 2.1.6.3 --- Detection of PCR products --- p.34 / Chapter 2.2 --- Prevalence and genotype distribution of HPV --- p.35 / Chapter 2.2.1 --- Study populations --- p.35 / Chapter 2.2.1.1 --- Women with normal cervices --- p.35 / Chapter 2.2.1.2 --- Women with abnormal cervical cytologies --- p.35 / Chapter 2.2.1.3 --- Women with cervical cancer --- p.35 / Chapter 2.2.2 --- Disease classification --- p.36 / Chapter 2.2.3 --- Specimen collection and preparation --- p.36 / Chapter 2.2.3.1 --- Cervical scrape collection --- p.36 / Chapter 2.2.3.1.1 --- DNA extraction --- p.37 / Chapter 2.2.4 --- HPV DNA detection --- p.37 / Chapter 2.2.4.1 --- MY09/MY11 PCR --- p.38 / Chapter 2.2.4.2 --- GP5+/GP6+ PCR --- p.38 / Chapter 2.2.4.3 --- Detection of PCR products --- p.38 / Chapter 2.2.5 --- HPV genotyping --- p.39 / Chapter 2.3 --- Sequence variation of HPV 16 E7 gene --- p.39 / Chapter 2.3.1 --- Study population --- p.39 / Chapter 2.3.2 --- Optimisation of HPV 16 E7 nested PCR --- p.40 / Chapter 2.3.3 --- HPV 16 E7 nested PCR --- p.41 / Chapter 2.3.3.1 --- Detection of PCR products --- p.42 / Chapter 2.3.4 --- Purification of nested PCR products --- p.42 / Chapter 2.3.5 --- Direct cycle sequencing --- p.42 / Chapter 2.3.5.1 --- Cycle sequencing reaction --- p.42 / Chapter 2.3.5.2 --- Purification of cycle sequencing products --- p.43 / Chapter 2.3.5.3 --- Electrophoresis on DNA sequencer --- p.43 / Chapter 2.3.6 --- Data analysis --- p.44 / Chapter 2.4 --- Statistical methods --- p.44 / Chapter CHAPTER 3 --- RESULTS --- p.45 / Chapter 3.1 --- Evaluation of HPV DNA extraction methods for paraffin-embedded tissues --- p.46 / Chapter 3.1.1 --- Optimised conditions for beta-globin PCRs --- p.46 / Chapter 3.1.2 --- Optimised conditions for HPV PCRs --- p.47 / Chapter 3.1.3 --- Analytical sensitivity of beta-globin and HPV PCRs --- p.48 / Chapter 3.1.4 --- PCR evaluation of DNA extraction methods --- p.48 / Chapter 3.1.4.1 --- PC03/PC07 PCRs --- p.48 / Chapter 3.1.4.2 --- Beta-GPl/Beta-GP2 PCRs --- p.49 / Chapter 3.1.4.3 --- HPV PCRs --- p.49 / Chapter 3.2 --- Prevalence and genotype distribution of HPV --- p.50 / Chapter 3.2.1 --- HPV detection --- p.50 / Chapter 3.2.2 --- HPV typing --- p.50 / Chapter 3.2.3 --- Women with normal cervices --- p.51 / Chapter 3.2.4 --- Women with abnormal cervical cytologies --- p.51 / Chapter 3.2.5 --- Women with cervical cancer --- p.53 / Chapter 3.3 --- Sequence variation of HPV 16 E7 gene --- p.54 / Chapter 3.3.1 --- Optimised conditions for HPV 16 E7 nested PCR --- p.54 / Chapter 3.3.2 --- HPV 16 E7 sequencing --- p.55 / Chapter 3.3.3 --- HPV 16 E7 variants --- p.55 / Chapter 3.3.4 --- Distribution of HPV 16 E7 variants --- p.56 / Chapter CHAPTER 4 --- DISCUSSION --- p.58 / Chapter 4.1 --- Evaluation of HPV DNA extraction methods for paraffin-embedded tissues --- p.59 / Chapter 4.1.1 --- PCR evaluation of DNA extraction methods --- p.59 / Chapter 4.2 --- Prevalence and genotype distribution of HPV --- p.61 / Chapter 4.2.1 --- Women with normal cervices --- p.61 / Chapter 4.2.2 --- Women with abnormal cervical cytologies --- p.62 / Chapter 4.2.3 --- Women with cervical cancer --- p.64 / Chapter 4.3 --- Sequence variation of HPV 16 E7 gene --- p.64 / Chapter CHAPTER 5 --- CONCLUSION --- p.69 / REFERENCES --- p.119
438

Caracterização fenotípica e genotipagem HFE em portadores de doença hepática crônica com sobrecarga de ferro / Phenotypic characteristics and HFE genotyping in patients with liver disease and iron overload

Evangelista, Andréia Silva 10 May 2013 (has links)
A doença hepática associada a sobrecarga de ferro pode ocorrer devido a causas genéticas ou secundárias. Esse estudo avaliou pacientes com hepatopatia crônica com sobrecarga de ferro submetidos à pesquisa das mutações HFE no período de 2007-2009 e classificou como portadores de hemocromatose hereditária HFE (HH-HFE) aqueles que apresentavam as mutações C282Y/C282Y ou C282Y/H63D e como sobrecarga de ferro não HFE aqueles que apresentavam outras mutações no gene HFE como C282Y/-, H63D/- e H63D/H63D ou pacientes sem qualquer uma dessas mutações mencionadas. Os objetivos do estudo foram 1) analisar e correlacionar os aspectos fenotípicos e genotípicos de grupo de indivíduos com doença hepática crônica e sobrecarga de ferro; 2) caracterizar o quadro clínico, laboratorial e anatomopatológico, em busca de achados compatíveis com o fenótipo de hemocromatose; 3) Correlacionar o quadro clínico com as mutações no gene HFE. Foram analisados 108 indivíduos portadores de hepatopatia crônica selecionados a partir de saturação de transferrina (ST) > 45% e ferritina sérica > 350 ng/mL. Foram estudados e comparados 16 pacientes no grupo HH-HFE com 92 no grupo sobrecarga de ferro não HFE. Da casuística geral, a idade média ao diagnóstico da doença foi de 46,69 anos (16-77), com 70,73% constituída por indivíduos de cor branca, 77,57% do sexo masculino e 64,8% tinham cirrose hepática. A frequência de cirrose hepática não diferiu entre os grupos, entretanto, artropatia, carcinoma hepatocelular, diabetes e osteoporose foram mais frequentes no grupo HH- HFE (53,8% x 15,9%, 31,2% x 7,06%, 56,2% x 30%, 72,7% x 32,1%, respectivamente, p < 0,05). Os pacientes com mutações HFE diagnósticas de HH apresentaram maior chance de ter carcinoma hepatocelular (OR= 5,0, p= 0,032) quando comparados com os portadores de outros genótipos HFE e aqueles sem mutação. Os níveis de ST, ferro e ferritina também foram maiores naquele grupo, bem como os graus de siderose 3 e 4 (p= 0,026). A ST foi a variável que se correlacionou independentemente com o diagnóstico das mutações C282Y/C282Y e C282Y/H63D. A frequência de fatores de risco para sobrecarga de ferro não diferiu entre os grupos. Observou-se, entretanto, que no grupo HH-HFE havia maior número de pacientes sem qualquer fator de risco detectado (p= 0,019). Níveis de ST > 82% apresentaram maior valor preditivo negativo para o diagnóstico de HH-HFE do que os de ferritina, ferro, capacidade total de ligação de ferro e de transferrina. Concluímos que os portadores de HH-HFE têm maiores graus de sobrecarga de ferro quando comparados ao grupo de sobrecarga de ferro não-HFE; em indivíduos com doença hepática crônica. ST > 82% tem maior acurácia para diagnóstico de HH-HFE; portadores de mutações C282Y em homozigose ou em heterozigose composta com H63D têm maior chance de apresentar carcinoma hepatocelular do que os portadores de outras mutações no gene HFE e pacientes sem mutação / Chronic liver disease related to iron overload may occur due to genetic or secondary causes. This study analyzed patients with chronic liver diseases and iron overload who were tested for HFE mutations from 2007 to 2009. Patients with C282Y/C282Y or C282Y/H63D mutations were diagnosed with HFE hereditary hemochromatosis (HFE-HH) and those with other HFE genotypes (C282Y/-, H63D/- or H63D/H63D) or individuals without HFE mutations (wild type) were designed as non-HFE iron overload. The aims of this study were: 1) to analyze and to establish correlations between phenotypic and genotypic aspects of individuals with chronic liver disease and with iron overload; 2) to charachterize the clinical manifestations, laboratory and histological findings consistent with the phenotype of hemochromatosis; 3) to verify associations between clinical manifestations and HFE mutations. One hundred and eight patients with chronic liver diseases and with iron overload, defined as transferrin saturation (TS) > 45% and serum ferritin levels > 350 ng/mL were included. Sixteen patients had HH-HFE and were compared with 92 patients with non-HFE iron overload group. The average of age at diagnosis was 46.69 years (16-77), 70.73% were Caucasians, 77.57% were male and 64.8% had hepatic cirrhosis. The proportion of hepatic cirrhosis was similar in both groups, nevertheless arthropathy, hepatocellular carcinoma, diabetes and osteoporosis were more frequent in the HFE-HH group (53,8% x 15,9%, 31,2% x 7,06%, 56,2% x 30%, 72,7% x 32,1%, respectively, p < 0,05). The HFE C282Y/C282Y or C282Y/ H63D genotypes had a higher chance to develop hepatocellular carcinoma (OR= 5.0, p= 0.032) when compared with the other HFE genotypes and with those wild type. The levels of TS, serum iron and ferritin were greater in HFE-HH group, as well as hepatic siderosis grade 3 and 4 (p= 0.026). TS was the biochemical marker of iron overload with the higher independent correlation with the presence of C282Y/C282Y and C282Y/H63D mutations. The frequency of risk factors for iron overload was not different between the groups, however, in HFE-HH group a greater number of patients without any risk factor was detected (p= 0.019). TS > 82% had a higher predictive negative value for diagnosing HFE-HH when compared to the levels of ferritin, serum iron, total iron binding capacity and transferrin. We concluded that the HFE-HH patients had a greater iron overload than patients with chronic liver diseases with non-HFE iron overload. TS > 82% had more accuracy to diagnose HFE-HH. The carriers of C282Y/C282Y or C282Y/H63D mutations had a higher probability to develop hepatocellular carcinoma, when compared to the patients with HFE genotypes and patients wild type
439

"Estudo clínico e endoscópico em pacientes com úlcera péptica gastroduodenal após 1 ano de erradicação do Helicobater pylori. Avaliação da relação entre o surgimento da esofagite erosiva e a cepa do Helicobacter pylori erradicado" / Clinical and endoscopic study in patients who have peptic gastroduodenal ulcer, 1 year after the eradication from Helicobacter pylori. Valuation of the relationship between the appearence of erosive esophagitis and the strains from the eradicated Helicobacter pylori

Batista, Carlos Alexandre Gonçalves 13 April 2006 (has links)
Atualmente, muitas são as diretrizes na literatura quanto à influência do Helicobacter pylori na Doença do Refluxo Gastroesofágico. Alguns autores acreditam que o H. pylori poderia ter um efeito protetor para o desenvolvimento na DRGE e outros até mesmo concluem que o agente possa ser um fator agravante na doença. Muitas publicações nos alertam para o desenvolvimento de sintomas da DRGE, ou mesmo da esofagite, em uma porcentagem razoável de pacientes erradicados pelo esquema tríplice para tratar o H. pylori, sendo que aproximadamente 10% teriam DRGE. Na verdade, por essas dúvidas, ainda não foi estabelecido um consenso quanto à importância do H. pylori na etiopatogenia da DRGE e suas complicações. Fato também discutido, seria a importância das cepas para a formação da esofagite em pacientes submetidos à erradicação. Talvez as mais virulentas, assim como a presença da “ilha de patogenicidade"(cagA) ou algumas cepas vacuolizantes (vacA), teriam uma maior relação com a prevenção da esofagite. Outro mecanismo importante, apontado por muitos, para a formação da esofagite em pacientes erradicados seria a elevação do índice de Massa Corpórea nesse grupo de pacientes erradicados associados ou não à presença da hérnia hiatal e justificados pela melhor qualidade de vida após melhora dos sintomas depois da erradicação. Em nosso estudo, 148 pacientes com úlcera péptica ativa ou cicatrizada receberam esquema tríplice de erradicação para o Helicobacter pylori e foram submetidos a exame endoscópico e ao teste histopatológico das amostras colhidas por biópsias de corpo e antro, teste respiratório com Carbono 14 e urease, antes e após o tratamento. Realizamos a genotipagem do agente, através do PCR, separando amostras de corpo e de antro, para determinar as cepas do agente. Os pacientes foram seguidos ambulatorialmente por um ano e avaliados quanto à melhora ou piora dos sintomas relacionados a DRGE (pirose) e sintomas considerados inespecíficos como a dor epigástrica; também procuramos quantificar o ganho ou perda do IMC. Encontramos 28 pacientes (18,9%) com esofagite erosiva (24 grau A e 4 grau B de Los Angeles) endoscópica após o tratamento do agente. Deste grupo, somente 3 pacientes que não tinham sintomas desenvolveram pirose (2%). A grande maioria dos pacientes se beneficiou com o tratamento, mostrando que 69 46,6%) melhoraram da pirose e outra grande maioria melhorou dos sintomas inespecíficos. Em 18 pacientes ulcerosos com esofagite, a análise de fragmentos de corpo foi cagA positiva (64,3%) e em amostras de antro 21 eram cagA positivos (75%). Assim como no grupo geral, as cepas vacuolizantes s1b/m1 e s1b foram, respectivamente, as mais encontradas no grupo da esofagite endoscópica. Houve ligeiro aumento nos Índices de Massa Corpórea em pacientes com e sem esofagite, sendo estatisticamente mais significativo nos 120 pacientes sem esofagite. Apesar do aparecimento da esofagite erosiva endoscópica em número razoável de pacientes, a sintomatologia não foi fator determinante, pois muitos melhoraram dos sintomas após o tratamento, e a erradicação não foi importante para determinar o grau de esofagite erosiva. Não foi encontrada nenhuma relação entre a genotipagem do agente e o desenvolvimento de esofagite endoscópica. O aumento de IMC, também não justifica, em nosso estudo a esofagite em pacientes ulcerosos tratados contra o H. pylori. / Nowadays, there are many directrixes in literature as to the influence of Helicobacter pylori, in the Disease of Gastroesophagic reflux. Some authors believe that H. pylori could have a protective effect to the development of GERD, and others even conclude that the agent may be an aggravating factor in the disease. Many publications allert us to the development of symptoms of GERD, or even the esophagitis,in a reasonable percentage of erradicated patients by the triplicit scheme to treat H. pylori, and 10%, approximately, would have GERD. In fact, due to these doubts, a consensus has not been established yet to the importance of H. pylori in the GERD’s etiopathogenic and its complications. The strains importance to the formation of esophagitis in patients submitted to erradication is another fact that has also been discussed. Maybe the most virulent ones, as the presence of “pathogenical island"(cagA) or some other vacuolating cytotoxin (vacA), would have a larger relation in the esophagitis prevention. Another important mechanism, pointed by many, to the formation of esophagitis in erradicated patients would be the elevation of Body Mass Index in this group of eradicated patients associated or not to the presence of hiatal hernia and justified by a better quality of life due to symptoms’ improvement after erradication. In our studies, 148 patients with active or healed peptic ulcer received triplicit scheme of erradication to the Helicobacter pylori and were submitted to endoscopic exams and histopathologic test of gathered samples by body and antro biopsies, respiratory test with carbon 14 and ureasis, before and after treatment. We have done the agent genotyping, through the PCR, separating samples of body and antro, to determine the agent Cepas. The patients have been followed ambulatorially for a year and evaluated as to the improvement or worsening of the symptoms related to GERD (pyrosis) and symptoms considered non-specific as epigastric pain; we have also tried to quantify the gain or loss of Body Mass Index. We found 28 patients(18.9%) with endoscopic erosive esophagitis (24 degree A and 4 degree B of Los Angeles) after agent’s treatment. In this group, only three patients who had no symptoms developed pyrosis (2%). Most of the patients benefitted from treatment showing that 69 (46.6%) presented improvement in pyrosis and another great majority improved non-specific symptoms. In 18 ulcered patients with esophagitis, the body analysis fragments was positive cagA (64.3%)and in antro samples of 21 were positive cagA (75%). As in the general group, the vacuolizing cepas slb/ml and slb were, respectivelly, the most found in the endoscopic esophagitis group. There was a slight raise in the BMI in patients with and without esophagitis, and it is, statistically more meaningful in the 120 patients without esophagitis. Even though there was the appearance of endoscopic erosive esophagitis in a reasonable number of patients, the symptmology was not a determining factor, because many have got better after the treatment, and erradication was not important to determine the erosive esophagitis. It was not found any relation between the agent genotyping and the development of endoscopic esophagitis. The raise of BMI does not justify in our study the esophagitis in ulcered patients treated against H. pylori.
440

The etiology of depression among Mexican American girls : a qualitative analysis

Lopez-Morales, Sandra Lynn, 1979- 04 October 2012 (has links)
This study uses an integration of ethnographic and case-study qualitative analysis to help explain early adolescent and caregiver perspectives of an increased prevalence of depression in Mexican American girls. This phenomenon has been replicated in numerous other studies and it is important to obtain more information to inform understanding, enhance treatment, and initiate intervention and prevention strategies. The combination of these methods of qualitative inquiry allowed for the triangulation of multiple pieces of data including participant observation, interviewing, and archival research. Retrospective child and caregiver verbal accounts were compared with one another as well as with prior assessment of functioning and participant observation. Fourteen Mexican American or bi-ethnic early adolescents and one of their caregivers were interviewed using an unstructured interview process. Transcribed interviews were analyzed qualitatively. Findings suggest that both girls and caregivers focus on the contribution of negative life events, interpersonal relationship stress, personal characteristics, gender discrimination, and biology on the increased prevalence of depression. It is noteworthy that each of these factors is strongly correlated with the family socio-cultural environment. This study concludes with a proposal to integrate the work of Zayas, Lester, Cabassa, and Fortuna (2005) regarding Latina suicide attempts and the work of Hyde, Mezulis, and Abramson (2008) regarding the increase in girls’ rates of depression during early adolescence to explain the increased prevalence of depression in Mexican American girls yielding additional affective, biological, and cognitive vulnerabilities as well as particular negative life events. / text

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