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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.
31

Frequência dos mutantes C282Y e H63D do gene HFE e sua influência no metabolismo do ferro e na expressão da beta talassemia heterozigota

Estevão, Isabeth da Fonseca [UNESP] 27 February 2007 (has links) (PDF)
Made available in DSpace on 2014-06-11T19:26:03Z (GMT). No. of bitstreams: 0 Previous issue date: 2007-02-27Bitstream added on 2014-06-13T20:54:00Z : No. of bitstreams: 1 estevao_if_me_sjrp.pdf: 1151592 bytes, checksum: 9e2d3a0a29b1ad6405857d13d891a9f1 (MD5) / Coordenação de Aperfeiçoamento de Pessoal de Nível Superior (CAPES) / A beta talassemia é um dos mais freqüentes distúrbios genéticos no mundo. Estima-se que 1,5% a 3% da população mundial seja portadora do traço talassêmico. Esses portadores geralmente são oligo ou assintomáticos e têm uma expectativa de vida semelhante à dos não portadores. Entretanto, níveis elevados de ferritina sérica têm sido observados em alguns estudos comparativos entre beta talassemia heterozigota e não portadores e, alguns indivíduos, que nunca foram transfundidos, apresentam sinais clínicos e laboratoriais de sobrecarga de ferro. A fisiopatologia dessa complicação continua em discussão. Vários pesquisadores têm sugerido um efeito modulador da mutação do gene da beta globina e mutações em genes codificadores de proteínas relacionadas ao metabolismo do ferro. Mutações no gene HFE são as mais freqüentemente associadas à hemocromatose hereditária. O objetivo do presente trabalho foi avaliar a freqüência das mutações C282Y e H63D no gene HFE em portadores de beta talassemia heterozigota e analisar sua influência no metabolismo do ferro. Foram estudados 162 portadores de beta talassemia heterozigota, residentes na cidade de São Carlos ou região, caucasóides e, acompanhados no serviço de Hematologia. O diagnóstico de traço talassêmico foi confirmado em todos por meio do eritrograma e da quantificação da Hb A2 e Hb fetal por HPLC. O metabolismo do ferro foi avaliado pelas dosagens de ferro sérico, capacidade total de ligação do ferro, ferritina e saturação da transferrina e, a análise molecular das mutações no gene HFE, pela técnica de PCR-RLFP. Foram realizadas análises de correlação linear de Pearson por idade e gênero entre hemoglobina... / Beta thalassemia is one of the most frequent genetic disorder in the world. It is estimated that 1.5% to 3% of the world population is a thalassemia carrier. These individuals are generally slightly symptomatic or asymptomatic and they have a life expectancy similar to those who are non-carriers. However, high levels of serum ferritin have been observed in some comparative studies between heterozygous for beta thalassemia and non-carriers, and some individuals that were never transfused, present clinic and laboratories signs of iron overload. The physiopathology of this disease continues in discussion. Several researchers have suggested a modulator effect from the mutation of the beta globin gene and mutations in genes related with the iron metabolism. Mutations of the gene HFE are the most frequently associated to the hereditary hemochromatosis. The aim of this study was evaluate the frequency of C282Y and H63D mutations in the HFE gene in beta thalassemia carriers, and analyze its influence in the iron metabolism. 162 beta thalassemia carriers, Caucasoid, residing in the city of Sao Carlos or region and accompanied in the Hematology service were studied. The diagnostic of thalassemia trait was confirmed in every one through a complete erythrogram and quantification of Hb A2 and Hb fetal by HPLC. The iron metabolism was evaluated by serum iron, total iron-binding capacity, serum ferritin and percent saturation of transferring. The molecular analysis of the mutations in the HFE gene was made by PCR-RLFP. There were made analysis of linear Pearson’ correlation, by age and gender, among hemoglobin, Hb A2, VCM and among reticulocytes count and the values of saturation of transferrin and serum ferritin.
32

Hemocromatose hereditária: associação entre as mutações no gene HFE e o estado de ferro em doadores de sangue e pesquisa de mutações nos genes HFE, HJV, HAMP, TFR2 e SLC40A1 em pacientes com sobrecarga de ferro primária / Hereditary hemochromatosis: relationship between HFE gene mutations and iron status in blood donors and HFE, HJV, HAMP, TFR2 and SLC40A1 gene sequencing in primary iron overload patients

Paulo Caleb Júnior de Lima Santos 21 January 2011 (has links)
A hemocromatose hereditária é caracterizada pelo aumento da absorção intestinal de ferro, acarretando progressivo acúmulo no organismo. Os objetivos foram: 1- determinar as frequências das mutações p.C282Y, p.H63D e p.S65C no gene HFE e avaliar os efeitos nas concentrações dos parâmetros do ferro em doadores de sangue; 2- pesquisar mutações nos genes: 2.1- HFE, 2.2- HJV e HAMP, 2.3- TFR2 e SLC40A1, em pacientes portadores de sobrecarga de ferro primária. Participaram 542 doadores de sangue provenientes do Hemocentro da Santa Casa de São Paulo. Foram incluídos 51 pacientes que apresentavam saturação de transferrina ≥ 50% (para mulheres) e ≥ 60% (para homens) e ausência de causas secundárias. Os genótipos para as mutações nos genes HFE foram avaliados pela PCR-RFLP. Foi realizado sequenciamento direto bidirecional para cada éxon dos genes, utilizando o sequenciador Genetic Analizer 3500XL®. Nos doadores de sangue, as frequências dos alelos HFE 282Y, HFE 63D e HFE 65C foram 2,1, 13,6 e 0,6%, respectivamente. Os homens que doaram pela primeira vez, portadores do genótipo HFE 282CY, apresentaram maiores valores de saturação de transferrina; e também os portadores dos genótipos HFE 63DD e 63HD apresentaram maiores concentrações de ferritina sérica, em relação aos de genótipo selvagem. Para os pacientes, 72,5% (37/51) apresentaram ao menos 1 alteração no gene HFE e 11 foram identificados como homozigotos para a mutação p.C282Y. Uma mutação não descrita na literatura (p.V256I) foi identificada no gene HFE e a modelagem molecular (análises de ligação e estrutural) detectou que a mutação não reduziu a afinidade entre as proteínas HFE e β2-microglobulina. No sequenciamento dos éxons dos genes HJV e HAMP foram identificadas as alterações já descritas: HJV p.E302K, HJV p.A310G, HJV p.G320V e HAMP p.R59G. Para o gene TFR2, foram identificados 3 polimorfismos já descritos (p.A75V, p.A617A e p.R752H). No gene SLC40A1 foram observados 6 polimorfismos (rs13008848, rs11568351, rs11568345, rs11568344, rs2304704 e rs11568346) e 1 alteração não descrita previamente na literatura (p.G204S). As conclusões foram: 1- em relação aos doadores de sangue, a presença dos alelos HFE 282Y e HFE 63D foi associada ao maior aporte de ferro nos homens que não doaram sangue anteriormente. 2.1- Para os pacientes com sobrecarga de ferro, a mutação p.C282Y em homozigose, ou em heterozigose composta com a p.H63D, foi a mais frequente alteração encontrada (33,3%). 2.2- O diagnóstico molecular de hemocromatose juvenil (HJ) no Brasil (HJV p.G320V em homozigose) foi relatado. As mutações funcionais HJV p.E302K e HAMP p.R59G foram identificadas, sendo possível que estas alterações possam estar contribuindo para consequências fenotípicas juntas as outras mutações em regiões intrônicas ou regulatórias dos genes. 2.3- Mutações funcionais nos genes TFR2 e SLC40A1 não foram identificadas. / Hereditary hemochromatosis (HH) is characterized by increased intestinal iron absorption, which leads to a progressive accumulation of iron in the body. The aims were: 1- to assess the frequency of HFE gene mutations (p.C282Y, p.H63D and p.S65C) and to identify their relationship to iron status in blood donors; 2- to search in primary iron overload patients: 2.1- HFE, 2.2- HJV and HAMP, 2.3- TFR2 and SLC40A1 gene mutations. Blood donors (n=542) were recruited from Hemocentro of Santa Casa Hospital, Sao Paulo, Brazil. The study included 51 patients with transferrin saturation ≥ 50% (women) and ≥ 60% (men) and absence of secondary causes. The genotypes for HFE mutations were evaluated by PCR-RFLP. Subsequent bidirectional sequencing for each gene was performed using the Genetic Analizer sequencer 3500XL®. The frequencies of HFE 282Y, HFE 63D and HFE 65C alleles were 2.1, 13.6 and 0.6% in blood donors, respectively. The first time male donors carrying heterozygous genotype for the p.C282Y mutation had higher transferrin saturation values; and men carrying HFE 63DD and 63HD genotypes had higher serum ferritin concentrations when compared to the wild genotype. Thirtyseven (72.5%) out of the 51 patients presented at least one HFE mutation and 11 were identified as homozygous for the mutation p.C282Y. One novel mutation (p.V256I) in the HFE gene was indentified and molecular modeling (free energy and structural analysis in silico) showed that p.V256I mutation did not reduce the affinity binding between HFE and β2-microglobulin. Sequencing in the HJV and HAMP genes revealed HJV p.E302K, HJV p.A310G, HJV p.G320V and HAMP p.R59G alterations. Sequencing in the TFR2 gene observed 3 polymorphisms (p.A75V, p.A617A e p.R752H); and sequencing in the SLC40A1 gene identified 6 polymorphisms (rs13008848, rs11568351, rs11568345, rs11568344, rs2304704 e rs11568346) and 1 p.G204S non-described mutation. The conclusions were: 1- for blood donors, the presence of HFE 282Y and HFE 63D alleles were associated with alterations on iron status only in first time male blood donors. 2.1- For patients with iron overload, the p.C282Y mutation in homozygous or in compound heterozygous with p.H63D, was the most frequent molecular change found (33.3%). 2.2- The molecular diagnosis of Juvenil Hemochromatosis (JH) in Brazil (homozygous genotype for the HJV p.G320V) was reported. The HJV p.E302K and HAMP p.R59G functional mutations were found and, it is conceivable that they may be contributing to phenotypic consequences together to other mutations in intronic or regulatory regions. 2.3- Functional mutation in the TFR2 and SLC40A1 genes were not identified.
33

Brain Sites of Movement Disorder: Genetic and Environmental Agents in Neurodevelopmental Perturbations

Palomo, T., Beninger, R. J., Kostrzewa, R. M., Archer, Trevor 01 December 2003 (has links)
In assessing and assimilating the neurodevelopmental basis of the so-called movement disorders it is probably useful to establish certain concepts that will modulate both the variation and selection of affliction, mechanisms-processes and diversity of disease states. Both genetic, developmental and degenerative aberrations are to be encompassed within such an approach, as well as all deviations from the necessary components of behaviour that are generally understood to incorporate "normal" functioning. In the present treatise, both conditions of hyperactivity/hypoactivity, akinesia and bradykinesia together with a constellation of other symptoms and syndromes are considered in conjunction with the neuropharmacological and brain morphological alterations that may or may not accompany them, e.g. following neonatal denervation. As a case in point, the neuroanatomical and neurochemical points of interaction in Attention Deficit and Hyperactivity disorder (ADHD) are examined with reference to both the perinatal metallic and organic environment and genetic backgrounds. The role of apoptosis, as opposed to necrosis, in cell death during grain development necessitates careful considerations of the current explosion of evidence for brain nerve growth factors, neurotrophins and cytokines, and the processes regulating their appearance, release and fate. Some of these processes may posses putative inherited characteristics, like asynuclein, others may to greater or lesser extents be endogenous or semi-endogenous (in food), like the tetrahydroisoquinolines, others exogenous until inhaled or injested through environmental accident, like heavy metals, e.g. mercury. Another central concept of neurodevelopment is cellular plasticity, thereby underlining the essential involvement of glutamate systems and N-methyl-D-aspartate receptor configurations. Finally, an essential assimilation of brain development in disease must delineate the relative merits of inherited as opposed to environmental risks not only for the commonly-regarded movement disorders, like Parkinson's disease, Huntington's disease and epilepsy, but also for afflictions bearing strong elements of psychosocial tragedy, like ADHD, autism and Savantism.
34

MRI susceptometry: Theory and robustness of an external phantom method for measuring bulk susceptibility from MRI field echo phase reconstruction maps applied to human liver iron overload

Holt, Randall William January 1993 (has links)
No description available.
35

Buněčná smrt jako důsledek železem indukovaného buněčného poškození / Cell death as a result of iron-induced cellular damage

Běhounek, Matěj January 2016 (has links)
Iron is an essential trace element for almost all living organisms. Iron overload in cells and tissues, however, leads to their disruption. Most oftenly damaged are parenchymatic organs such as the liver, pancreas and heart. The aim of this thesis was to create cellular in vitro models for the investigation of effects of excess iron on hepatocytes and pancreatic beta cells and on these models to investigate cellular processes which lead to cellular damage during iron overload. We focused on examining the presence of oxidative and endoplasmic reticulum stress and the activation of apoptotic cell death. For our experiments, we used HEP-G2 cell line which represents human hepatocytes and NES2Y cell line which represents human pancreatic beta cells. To study the mechanisms of cellular damage during iron overload, we used two approaches by which we observed both acute and long-term effects of high levels of iron on damage of the tested cell lines. When studying the acute effect of excess iron on the cells, we applied high doses of iron (using 15 mM ferric citrate in medium) that led to the activation of cell death in hours. Long-term effects of iron overload were tested on cells regularly cultivated in the presence of 50 μM and 100 μM ferric citrate over a period of several months. Iron concentrations...
36

Sítios polimórficos do gene hfe em estudos populacionais e em doenças hereditárias ou adquiridas que cursam com sobrecarga de ferro / Population study of polymorphic loci in HFE gene in hereditary or acquire disease course to iron overload

Campos, Wagner Narciso de 31 July 2013 (has links)
Mutações no gene HFE têm sido apontadas como um dos principais fatores para o desenvolvimento de sobrecarga de ferro, especialmente os SNPs (single nucleotide polymorphism) clássicos C282Y e H63D. A sobrecarga de ferro pode ser primária, atribuída diretamente a mutações do gene HFE (hemocromatose hereditária - HH) ou adquirida em decorrência de fatores genéticos e de comorbidades, particularmente, infecção pelo vírus da hepatite C (HCV) e carcinoma hepatocelular (CHC). Desequilíbrio de ligação entre os SNPs principais do gene HFE com alelos dos genes HLA-A e HLA-B podem contribuir com alterações da função das células do sistema imunológico. Neste trabalho, sequenciamos a região codificadora do gene HFE (éxon 2, 3, 4 e 5) de pacientes que apresentam ou não sobrecarga de ferro primária ou adquirida. Assim, estudamos 130 pacientes com hepatite C, 60 pacientes com CHC, 14 pacientes com HH e 100 indivíduos saudáveis. Foram encontrados sete SNPs no gene HFE no sentido 5\' para 3\': i) H63D C>G no éxon 2 (rs1799945); ii) IVS2(+4)T>C no íntron 2 (rs2071303); iii) íntron 3 C>G (rs807209); iv) C282Y G>A no éxon 4 (rs1800562); v) íntron 4 G>A (rs2794717); vi) IVS4(-44) T>C (rs1800708); vii) no íntron 5 a deleção G>del, ainda não foi descrita na literatura. Foram realizadas as reconstruções de haplótipos da região codificadora e os haplótipos estendidos englobando o gene HFE e dez outros loci (HLA-A, HLA-B, HLA-C, HLA-DRB1, HLA-DQB1, TNFa, TNFb, TNFc, TNFd e HLA-G-14pb). Também, normatizamos a nomenclatura do gene de acordo com as regras do The International ImMunoGeneTics Information System - IMGT (http://www.imgt.org/). Diversas ferramentas foram utilizadas para avaliar a associação entre os sítios polimórficos do gene HFE com a sobrecarga de ferro, incluindo testes de associações avaliando alelos, genótipos, desequilíbrio de ligação, haplótipos e diplótipos, testes de diversidades e neutralidade. Finalmente, comparamos os SNPs do gene HFE encontrados na população saudável do presente trabalho com as diversas populações mundiais, disponíveis no sítio 1000genomes (http://www.1000genomes.org/). Os resultados demonstraram que a nossa a população estava mais próxima das populações europeias e americanas, sendo parcialmente próxima das populações africanas e distante das populações asiáticas. O alelo C282Y G, contido no haplótipo da região codificadora HFE*01:03, conferiu susceptibilidade a HH na população brasileira testada, concordando com os achados observados em outras populações mundiais. O diplótipo HFE*01:02:01:01/HFE*01:01:01:05 conferiu susceptibilidade para o desenvolvimento de sobrecarga de ferro em pacientes com CHC causado pelo HCV. Detectamos forte desequilíbrio entre os alelos H63D G e IVS2(+4) C no éxon 2 do gene HFE, e concomitantemente, desequilíbrio desses alelos com alelo HLA-B*44, aparentemente, sem associação com sobrecarga de ferro, mas com aparente origem histórica. Finalmente, o teste de diversidade encontrou diferenças apenas na amostra de HH e o teste de neutralidade não encontrou pressões seletivas na população controle do presente trabalho. Concluindo, este é o primeiro trabalho, avaliando grande segmento da região codificadora do gene HFE em diversas amostras de pacientes apresentando ou não sobrecarga de ferro e em indivíduos controle. / Mutations at the HFE gene have been identified as a major factor for the development of iron overload, especially the classical single nucleotide polymorphism (SNP) C282Y and H63D. Primary iron overload can be directly attributed to mutations in the HFE gene (hereditary hemochromatosis - HH), whereas secondary overload may be acquired due to genetic factors and comorbidities, particularly infection with hepatitis C virus (HCV) and hepatocellular carcinoma (HCC). Linkage disequilibrium between major SNPs at the HFE gene with HLA-A and HLA-B alleles may contribute to alterations in the function of immune cells. We sequenced the coding region of the HFE gene (exon 2, 3, 4 and 5) of patients exhibiting primary or secondary iron overload. Thus, we studied 130 patients with hepatitis C, 60 patients with HCC, 14 patients with HH and 100 healthy individuals. We observed seven SNPs in the HFE gene in 5 \'to 3\' sequence: i) H63D C>G at exon 2 (rs1799945); ii) IVS2(+4)T>C at intron 2 (rs2071303); iii) intron 3 C>G (rs807209); iv) C282Y G>A at exon 4 (rs1800562); v) intron 4 G>A (rs2794717); vi) IVS4(-44) T>C (rs1800708); vii) at intron 5 we detected a yet undescribed G>deletion. We performed haplotype reconstruction of the coding region and extended haplotypes comprising the HFE gene and ten other loci (HLA-A, HLA-B, HLA-C, HLA-DRB1, HLA-DQB1, TNFa, TNFb, TNFc, TNFd and HLA-G14bp). In addition, we normatized the nomenclature of the HFE gene, according to the rules of the International ImMunoGeneTics Information System - IMGT (http://www.imgt.org/). Several tools were used to evaluate the association between HFE polymorphic sites with iron overload, including tests assessing associations of alleles, genotypes, linkage disequilibrium, haplotype and diplotypes, diversity and neutrality tests. Finally, we compare the SNPs at the HFE gene observed in the healthy population with those observed in diverse worldwide populations available at the 1000genomes site (http://www.1000genomes.org/) the results showed that our population was closer to American and European populations, partially close the populations of African and distant of Asian populations. The C282Y allele G, contained in the coding region HFE * 01:03 haplotype, conferred susceptibility to HH in the Brazilian population tested, agreeing with the findings observed in other worldwide populations. The HFE*01:02:01:01/HFE* 01:01:01:05 dyplotype conferred susceptibility to the development of iron overload in patients with HCC caused by HCV. A strong linkage disequilibrium was detected between the H63D G and IVS2 (+4) C alleles in exon 2 of the HFE gene, and concomitantly, a linkage between these alleles with HLA-B*44, apparently not associated with iron overload, but with apparent historical origin. Finally, the test of diversity revealed differences only in the HH sample and the neutrality test detected no selective pressures on the control population of this study. In conclusion, this is the first study evaluating a large segment of the coding region of the HFE gene in several samples of patients exhibiting or not iron overload and in control subjects.
37

Avaliação da qualidade de vida e da percepção de saúde em pacientes com hemocromatose hereditária / Assessment of quality of life and health perception in patients with hereditary hemochromatosis

Fonseca, Paula Fernanda da Silva 30 May 2017 (has links)
Introdução: A hemocromatose hereditária (HH) é uma doença autossômica recessiva caracterizada principalmente pelo aumento da absorção intestinal de ferro e seu acúmulo em órgãos. O diagnóstico da HH baseia-se nas avaliações de exames laboratoriais de ferro, imagem por ressonância magnética (RMN) e/ou testes genéticos. Diferentes genótipos são identificados como resultados de testes genéticos em pacientes com suspeita de sobrecarga de ferro primário. Além disso, questionários como o SF-36 (short form health survey), têm sido cada vez mais utilizados para avaliar o impacto das doenças na qualidade de vida (QV) do paciente. No presente estudo, nossos objetivos foram: avaliar se os domínios de QV avaliados pelo questionário SF-36 são diferentes de acordo com os grupos genotípicos em pacientes com suspeita de HH e desenvolver materiais informativos e educativos sobre HH para pacientes, familiares e profissionais de saúde. Métodos: Foram utilizados os questionários SF-36, PHQ-9 (patient health questionnaire-9) e dados gerais e específicos para avaliar domínios de qualidade de vida e depressão e características gerais da doença. Pacientes com sobrecarga de ferro primária foram incluídos (n=79) e dois grupos genotípicos foram formados: grupo 1: genótipo homozigoto para a mutação HFE p.Cys282Tyr e grupo 2: outros genótipos. Resultados: O grupo 1 apresentou maiores médias de saturação de transferrina (86±19%) e ferritina sérica (1669±1209 ng/mL) comparado ao grupo 2 (71±12%, 1252±750 ng/mL, respectivamente; P=0,001). Quatro domínios foram significativamente diferentes entre os grupos 1 e 2: capacidade funcional (P=0,03), dor (P=0,03), vitalidade (P=0,02) e aspectos sociais (P=0,01). O grupo 1 apresentou valores mais baixos para estes domínios. O grupo brasileiro de hemocromatose hereditária (GBHH) foi criado, o site foi desenvolvido e foram recebidos vários cadastros. O material informativo/educativo foi desenvolvido e distribuído aos pacientes, familiares e profissionais de saúde envolvidos neste estudo. Conclusões: O principal achado deste estudo foi que os pacientes com genótipo homozigoto para p.Cys282Tyr apresentaram um pior cenário de QV avaliado pelo SF-36, em comparação aos pacientes com sobrecarga de ferro sem o mesmo genótipo. O conhecimento desta relação entre genótipos e QV pode ser útil no manejo geral de pacientes com suspeita de HH. Este estudo foi capaz de contribuir para mais informações sobre a HH, aumentando a educação em saúde e a divulgação deste cenário / Background: Hereditary hemochromatosis (HH) is an autosomal recessive disease mainly characterized by increased intestinal absorption of iron and its accumulation in organs. The diagnosis of HH is based on laboratory tests of iron, magnetic resonance imaging (MRI) evaluations and / or genetic testing. Different genotypes are identified as results of genetic tests in patients with suspected of primary iron overload. In addition, questionnaires such as the SF-36 (short form health survey), have been increasingly used to assess the impact of diseases on the patient\'s quality of life (QL). In the present study, our aims were: evaluate if the domains of QL by SF-36 questionnaire are different according to genotypic groups in patients with suspected of HH and develop informative and educational materials about HH for patients, family members and health professionals. Methods: The SF-36, PHQ-9 (Patient health questionnaire-9) questionnaires, general and disease-specific data were used to evaluate the domains of quality of life and depression and general characteristics of the disease. Patients with primary iron overload were included (n=79) and two genotypic groups were formed group 1: homozygous genotype for the HFE p.Cys282Tyr mutation and group 2: other genotypes. Results: Group 1 presented higher mean values of transferrin saturation (86±19%) and serum ferritin (1669±1209 ng/mL) compared to group 2 (71±12%, 1252±750 ng/mL, respectively, P= 0.001). Four domains were significantly different between groups 1 and 2: physical functioning (P= 0.03), bodily pain (P= 0.03), vitality (P= 0.02) and social functioning (P= 0.01). Group 1 presented lower values for these domains. The \"Brazilian group of hereditary hemochromatosis\" (GBHH) was created, the website was developed and several registrations were received. The informative/educational material was developed and distributed to patients, family members and health professionals involved in this study. Conclusion: The main finding of this study was that patients with genotype homozygous for p.Cys282Tyr presented worse scenario of QL evaluated by SF-36, compared to patients with iron overload without the same genotype. The knowledge of this relationship between genotypes and QL may be useful in the general management of patients with suspected of HH. This study was able to contribute with more information about HH, increasing health education and the divulgation of this scenario
38

Frequência dos mutantes C282Y e H63D do gene HFE e sua influência no metabolismo do ferro e na expressão da beta talassemia heterozigota /

Estevão, Isabeth da Fonseca. January 2007 (has links)
Resumo: A beta talassemia é um dos mais freqüentes distúrbios genéticos no mundo. Estima-se que 1,5% a 3% da população mundial seja portadora do traço talassêmico. Esses portadores geralmente são oligo ou assintomáticos e têm uma expectativa de vida semelhante à dos não portadores. Entretanto, níveis elevados de ferritina sérica têm sido observados em alguns estudos comparativos entre beta talassemia heterozigota e não portadores e, alguns indivíduos, que nunca foram transfundidos, apresentam sinais clínicos e laboratoriais de sobrecarga de ferro. A fisiopatologia dessa complicação continua em discussão. Vários pesquisadores têm sugerido um efeito modulador da mutação do gene da beta globina e mutações em genes codificadores de proteínas relacionadas ao metabolismo do ferro. Mutações no gene HFE são as mais freqüentemente associadas à hemocromatose hereditária. O objetivo do presente trabalho foi avaliar a freqüência das mutações C282Y e H63D no gene HFE em portadores de beta talassemia heterozigota e analisar sua influência no metabolismo do ferro. Foram estudados 162 portadores de beta talassemia heterozigota, residentes na cidade de São Carlos ou região, caucasóides e, acompanhados no serviço de Hematologia. O diagnóstico de traço talassêmico foi confirmado em todos por meio do eritrograma e da quantificação da Hb A2 e Hb fetal por HPLC. O metabolismo do ferro foi avaliado pelas dosagens de ferro sérico, capacidade total de ligação do ferro, ferritina e saturação da transferrina e, a análise molecular das mutações no gene HFE, pela técnica de PCR-RLFP. Foram realizadas análises de correlação linear de Pearson por idade e gênero entre hemoglobina... (Resumo completo, clicar acesso eletrônico abaixo) / Abstract: Beta thalassemia is one of the most frequent genetic disorder in the world. It is estimated that 1.5% to 3% of the world population is a thalassemia carrier. These individuals are generally slightly symptomatic or asymptomatic and they have a life expectancy similar to those who are non-carriers. However, high levels of serum ferritin have been observed in some comparative studies between heterozygous for beta thalassemia and non-carriers, and some individuals that were never transfused, present clinic and laboratories signs of iron overload. The physiopathology of this disease continues in discussion. Several researchers have suggested a modulator effect from the mutation of the beta globin gene and mutations in genes related with the iron metabolism. Mutations of the gene HFE are the most frequently associated to the hereditary hemochromatosis. The aim of this study was evaluate the frequency of C282Y and H63D mutations in the HFE gene in beta thalassemia carriers, and analyze its influence in the iron metabolism. 162 beta thalassemia carriers, Caucasoid, residing in the city of Sao Carlos or region and accompanied in the Hematology service were studied. The diagnostic of thalassemia trait was confirmed in every one through a complete erythrogram and quantification of Hb A2 and Hb fetal by HPLC. The iron metabolism was evaluated by serum iron, total iron-binding capacity, serum ferritin and percent saturation of transferring. The molecular analysis of the mutations in the HFE gene was made by PCR-RLFP. There were made analysis of linear Pearson' correlation, by age and gender, among hemoglobin, Hb A2, VCM and among reticulocytes count and the values of saturation of transferrin and serum ferritin. / Orientador: Claudia Regina Bonini Domingos / Coorientador: Antonio José Manzato / Banca: Celso Carlos de Campos Guerra / Banca: Paula Rahal Liberatore / Mestre
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Avaliação da qualidade de vida e da percepção de saúde em pacientes com hemocromatose hereditária / Assessment of quality of life and health perception in patients with hereditary hemochromatosis

Paula Fernanda da Silva Fonseca 30 May 2017 (has links)
Introdução: A hemocromatose hereditária (HH) é uma doença autossômica recessiva caracterizada principalmente pelo aumento da absorção intestinal de ferro e seu acúmulo em órgãos. O diagnóstico da HH baseia-se nas avaliações de exames laboratoriais de ferro, imagem por ressonância magnética (RMN) e/ou testes genéticos. Diferentes genótipos são identificados como resultados de testes genéticos em pacientes com suspeita de sobrecarga de ferro primário. Além disso, questionários como o SF-36 (short form health survey), têm sido cada vez mais utilizados para avaliar o impacto das doenças na qualidade de vida (QV) do paciente. No presente estudo, nossos objetivos foram: avaliar se os domínios de QV avaliados pelo questionário SF-36 são diferentes de acordo com os grupos genotípicos em pacientes com suspeita de HH e desenvolver materiais informativos e educativos sobre HH para pacientes, familiares e profissionais de saúde. Métodos: Foram utilizados os questionários SF-36, PHQ-9 (patient health questionnaire-9) e dados gerais e específicos para avaliar domínios de qualidade de vida e depressão e características gerais da doença. Pacientes com sobrecarga de ferro primária foram incluídos (n=79) e dois grupos genotípicos foram formados: grupo 1: genótipo homozigoto para a mutação HFE p.Cys282Tyr e grupo 2: outros genótipos. Resultados: O grupo 1 apresentou maiores médias de saturação de transferrina (86±19%) e ferritina sérica (1669±1209 ng/mL) comparado ao grupo 2 (71±12%, 1252±750 ng/mL, respectivamente; P=0,001). Quatro domínios foram significativamente diferentes entre os grupos 1 e 2: capacidade funcional (P=0,03), dor (P=0,03), vitalidade (P=0,02) e aspectos sociais (P=0,01). O grupo 1 apresentou valores mais baixos para estes domínios. O grupo brasileiro de hemocromatose hereditária (GBHH) foi criado, o site foi desenvolvido e foram recebidos vários cadastros. O material informativo/educativo foi desenvolvido e distribuído aos pacientes, familiares e profissionais de saúde envolvidos neste estudo. Conclusões: O principal achado deste estudo foi que os pacientes com genótipo homozigoto para p.Cys282Tyr apresentaram um pior cenário de QV avaliado pelo SF-36, em comparação aos pacientes com sobrecarga de ferro sem o mesmo genótipo. O conhecimento desta relação entre genótipos e QV pode ser útil no manejo geral de pacientes com suspeita de HH. Este estudo foi capaz de contribuir para mais informações sobre a HH, aumentando a educação em saúde e a divulgação deste cenário / Background: Hereditary hemochromatosis (HH) is an autosomal recessive disease mainly characterized by increased intestinal absorption of iron and its accumulation in organs. The diagnosis of HH is based on laboratory tests of iron, magnetic resonance imaging (MRI) evaluations and / or genetic testing. Different genotypes are identified as results of genetic tests in patients with suspected of primary iron overload. In addition, questionnaires such as the SF-36 (short form health survey), have been increasingly used to assess the impact of diseases on the patient\'s quality of life (QL). In the present study, our aims were: evaluate if the domains of QL by SF-36 questionnaire are different according to genotypic groups in patients with suspected of HH and develop informative and educational materials about HH for patients, family members and health professionals. Methods: The SF-36, PHQ-9 (Patient health questionnaire-9) questionnaires, general and disease-specific data were used to evaluate the domains of quality of life and depression and general characteristics of the disease. Patients with primary iron overload were included (n=79) and two genotypic groups were formed group 1: homozygous genotype for the HFE p.Cys282Tyr mutation and group 2: other genotypes. Results: Group 1 presented higher mean values of transferrin saturation (86±19%) and serum ferritin (1669±1209 ng/mL) compared to group 2 (71±12%, 1252±750 ng/mL, respectively, P= 0.001). Four domains were significantly different between groups 1 and 2: physical functioning (P= 0.03), bodily pain (P= 0.03), vitality (P= 0.02) and social functioning (P= 0.01). Group 1 presented lower values for these domains. The \"Brazilian group of hereditary hemochromatosis\" (GBHH) was created, the website was developed and several registrations were received. The informative/educational material was developed and distributed to patients, family members and health professionals involved in this study. Conclusion: The main finding of this study was that patients with genotype homozygous for p.Cys282Tyr presented worse scenario of QL evaluated by SF-36, compared to patients with iron overload without the same genotype. The knowledge of this relationship between genotypes and QL may be useful in the general management of patients with suspected of HH. This study was able to contribute with more information about HH, increasing health education and the divulgation of this scenario
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Hémochromatose HFE : influence de facteurs génétiques et non génétiques sur l'expression phénotypique / HFE hemochromatosis : influence of genetic and non genetic factors on phenotypic expression

Saliou, Philippe 18 November 2014 (has links)
L’hémochromatose HFE est une maladie du métabolisme du fer liée au gène HFE dont la principale mutation est C282Y. L’objectif général de ce travail était d’étudier l’influence de facteurs génétiques et non génétiques sur l’expression phénotypique de patients atteints d’hémochromatose HFE. Cette étude prospective incluait les patients C282Y/C282Y etC282Y/H63D inclus en protocole de saignées entre janvier 2004 et décembre 2011 au centre de santé brestois de l’EFS-Bretagne. Dans un premier temps, nous avons étudié l’influence du génotype C282Y/H63D sur la survenue d’une surcharge en fer. Nous avons confirmé que le variant H63D doit être considéré comme un facteur de susceptibilité dont l’expression est liée à la présence de co-facteurs responsables d’une hyper ferritinémie. Ensuite, nous avons étudié le rôle des grossesses et de l’alimentation sur l’expression phénotypique du génotype C282Yhomozygote. Nous avons montré qu’il existe bien une différence d’expressivité clinique liée au sexe chez les patients C282Y/C282Y. Cependant, nos données n’ont pas confirmé l’effet protecteur typiquement attribué aux grossesses pour expliquer la plus lente accumulation de fer chez les femmes. Cette étude a également mis en évidence une association modérée entre la consommation d’aliments riches en fer et le degré de surcharge en fer des patients C282Yhomozygotes traités par phlébotomies. Ce travail contribue à mieux comprendre l’hétérogénéité phénotypique observée dans l’hémochromatose HFE. La finalité est de pouvoir repérer précocement les sujets les plus à risque de développer les surcharges en fer les plus sévères et par conséquent des complications cliniques. / HFE hemochromatosis is a disorder of iron metabolism related to the HFE gene whose mainmutation is C282Y. The overall aim of this study was to investigate the influence of genetic and non genetic factors on phenotypic expression of patients with HFE hemochromatosis. This prospective study included the C282Y/C282Y and C282Y/H63D patients enrolled in a phlebotomy program between 2004 and 2011 in a blood centre of western Brittany (Brest, France). First, weassessed the weight of the C282Y/H63D genotype in the occurrence of iron overload. We confirmed that H63D is a discrete genetic susceptibility factor whose expression is most visible in association with other co-factors responsible for hyper ferritinemia. Then we investigated the effect of pregnancies and iron-rich diet on phenotypic expressivity of the C282Y/C282Y genotype. We have shown that there is a difference in clinical expression related to gender in C282Y/C282Ypatients. However our findings did not confirm that pregnancies protect against iron accumulationin women. This study established a moderate link between dietary iron intake and the degree of iron overload in HFE hemochromatosis patients who come to medical attention. This work contributes to a better understanding of the phenotypic heterogeneity observed in HFE hemochromatosis. The purpose is to identify precociously subjects the most at risk of developing iron overload and therefore clinical complications.

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