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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.
91

Recherche et validation de biomarqueurs lipidiques du globule rouge par chromatographie en phase liquide couplée à la spectrométrie de masse. Application au diagnostic et au suivi thérapeutique de la maladie de Gaucher / Research and validation of red blood cell lipid biomarkers based on liquid chromatography-tandem mass spectrometry. Application to the diagnosis and monitoring of Gaucher disease

Chipeaux, Caroline 18 December 2019 (has links)
Chez l’homme, les erreurs innées du métabolisme des lipides sont dues à des déficits enzymatiques, entraînant une accumulation intracellulaire de substrats lipidiques. Il en résulte un large éventail de symptômes tels que des atteintes viscérales, osseuses et dans certains cas neurologiques. En outre, de nombreux patients atteints de ce type de maladie présentent des anomalies hématologiques et vasculaires attribuées à des anomalies rhéologiques du globule rouge (GR). Ces observations ont conduit à l’hypothèse de l’existence d’un lien entre les propriétés anormales du GR et sa composition lipidique. Or actuellement, le profil lipidique du GR normal reste méconnu. Cependant, le diagnostic précoce de ces troubles est d’une importance capitale pour la prise en charge des patients, notamment dans les cas où un traitement correctif est disponible. La maladie de Gaucher (MG) de type 1, qui est une maladie lysosomale caractérisée par un déficit en β-glucocérébrosidase et pour laquelle un traitement enzymatique substitutif (ERT) est proposé, en est le meilleur exemple. D’où l’intérêt de disposer d’un outil simple et rapide de diagnostic de ce type de maladie.Dans le cas de la MG, le diagnostic repose encore sur la mise en évidence, laborieuse, du déficit enzymatique. Néanmoins, des travaux récents suggèrent que les anomalies rhéologiques du GR pourraient être dues à l’accumulation de quatre sphingolipides, le glucosylcéramide, la glucosylsphingosine, la sphingosine et la sphingosine-1-phosphate, qui seraient de bons candidats biomarqueurs. Or, les méthodes actuelles de dosage de ces sphingolipides nécessitent au moins deux étapes chromatographiques, avec pour chacune une étape longue et fastidieuse de préparation de l’échantillon, ce qui ne facilite guère une approche lipidomique de ce sujet. En outre, seul le glucosylcéramide a été dosé dans le GR tandis que les trois autres sphingolipides n’ont été dosés que dans le plasma. Ces candidats biomarqueurs restent donc à valider.Dans cette thèse, nous avons développé et validé une méthode simple et rapide, par UHPLC-MS/MS, de dosage simultané des 4 sphingolipides impliqués dans la MG. L’application de cette méthode à des GR provenant de patients atteints de la MG, en collaboration avec l’Institut National de Transfusion Sanguine et la société Shire, nous a permis de : 1- valider un biomarqueur parmi les quatre proposés et de montrer que les trois autres n’étaient pas suffisamment spécifiques ; 2- vérifier l’efficacité du traitement ERT actuellement proposé et 3- confirmer l’hypothèse de départ reliant les anomalies rhéologiques du GR à sa composition lipidique.De même, une étude systématique des conditions opératoires nous a permis de généraliser la méthode proposée à l’identification et au dosage de l’ensemble des sphingolipides présents dans un GR ainsi que des phospholipides, constituants majoritaires de sa membrane. Appliquée à la quantification simultanée d’une trentaine de sphingolipides et de phospholipides dans le GR normal et celui de la MG, cette méthode nous a permis de mettre en évidence l’implication d’autres lipides polaires dans la maladie de Gaucher, outre les 4 sphingolipides jusqu’alors proposés. De même, il est prévu de l’adapter à moyen terme pour le profilage total, par classe, de tous les lipides présents dans le GR.Enfin, nous avons évalué d’autres techniques de SM telles que la haute résolution et la mobilité ionique (TWIMS et DIMS) dans le but d’affiner la recherche de nouveaux biomarqueurs, notamment par l’identification des lipides isomères non discriminables par les techniques de MS conventionnelles. Grâce à une collaboration avec le Laboratoire de Chimie Physique (LCP, CNRS UMR 8000) nous avons montré la faisabilité de cette approche en séparant en DIMS deux isomères : la galactosylsphingosine 18:1 et la glucosylsphingosine 18:1 et nous poursuivons actuellement cette étude pour séparer d’autres couples d’isomères. / In humans, hereditary disorders of lipid metabolism are due to enzyme deficiencies, resulting in intracellular accumulation of lipid substrates. This results in a wide range of symptoms such as visceral, bone and in some cases neurological disorders. Furthermore, many patients suffering such diseases have hematologic and vascular symptoms attributed to red blood cell (RBC) rheological abnormalities. These observations led to a hypothesis linking RBC abnormal properties to its lipid composition. However, the lipid profile of normal RBC remains unknown to date. Early diagnosis of these conditions is of importance notably when a therapy is available. This is the case for Gaucher disease (GD) type 1, a lysosomal disorder characterized by β-glucocerebrosidase deficiency, where an enzyme replacement therapy (ERT) is proposed. Hence, the availability of a simple and rapid tool of diagnosis of such a disorder is of great importance, notably for a better patient care and monitoring.To the best of our knowledge, standard diagnosis procedures and monitoring of GD patients are still based on the tedious evaluation of enzyme deficiency. Nevertheless, recent works suggest that these rheological disorders may be due to the accumulation of four sphingolipids, glucosylceramide, glucosylsphingosine, sphingosine and sphingosine-1-phosphate, which could be considered as relevant biomarkers. However, most of current determination methods of these sphingolipids require at least two liquid chromatographic runs, each with a time-consuming sample preparation step that does not facilitate a lipidomic approach. In addition, only glucosylceramide was quantified in RBC while the other three sphingolipids were quantified only in plasma. Thus, these biomarker candidates remain to be validated.In this PhD, we describe a simple and rapid UHPLC-MS/MS method of simultaneous determination of the 4 sphingolipids involved in GD in both plasma and RBC. The application of this method to RBC from GD patients, in collaboration with the Institut National de Transfusion Sanguine and Shire (USA), allowed us: 1- to validate one biomarker among the four proposed candidates and to show that the other three candidates are not specific; 2- to check the efficiency of the proposed ERT and 3- to confirm the initial hypothesis linking the RBC rheological abnormalities to its lipid composition.Also, a systematic study of the operating conditions allowed us to generalize the proposed method to the determination of not only all the sphingolipids present in RBC but also all phospholipids, which are the major constituents of its membrane. The application of the later method to the simultaneous quantification of thirty sphingolipids and phospholipids in normal and GD RBCs, allowed us to validate it and to unravel the involvement of other candidate biomarkers of GD, different from the 4 previous sphingolipids. Providing appropriate modifications, this method is intended to be used for the profiling of all lipid classes in plasma and RBC. This is our main objective in the medium-term.Finally, we evaluated other modern MS techniques such as high resolution (HRMS) and ion mobility (TWIMS and DIMS) in order to refine the investigation of new biomarker candidates, including the separation of lipid isomers that cannot be discriminated by conventional MS techniques. Indeed, in collaboration with the Laboratoire de Chimie Physique (LCP, CNRS UMR 8000), we here show the feasibility of this approach by achieving the separation of two isomers, by the DIMS technique: galactosylsphingosine 18:1 and glucosylsphingosine 18:1, which cannot be separated by conventional methods. We are currently pursuing these investigations in order to separate other isomers.
92

Rodina dítěte s postižením / Family with disabled child

Benda, Aleš January 2021 (has links)
This thesis deals with families of a child with inborn and gained disability. The core of the work lies in text analysis based upon a discussion with two mothers with a child with a disability. The analysis pays particular attention to the way of coping with such a difficult life situation. Further it focuses on inner and external factors that help to acquire back a life well- being of those mothers. Theoretical part contains a family theme, specifics of raising and education of a child with a disability and coping strategies. The aim of this work is to be utilised as a source of inspiration for those families that are going through similar life situation.
93

Application of Atmospheric Pressure Chemical Ionization Gas Chromatography in Urine Organic Acid Analysis

Ganepola, Devanjith 11 1900 (has links)
Inborn errors of metabolism (IEM) cause significant morbidity and mortality when left untreated. Urine organic acid (UOA) analysis is often a first-line investigation when an IEM is suspected. UOAs are usually qualitatively analyzed via the current gold standard, GC-EI-MS (Gas Chromatography-Electron Impact-Mass Spectroscopy). The Agilent 7890 GC in tandem with the Waters’ Xevo TQ-S MS contains an easily interchangeable LC-ESI (liquid chromatography-electrospray Ionization) and GC-APCI (Atmospheric Pressure Chemical Ionization) instrument set-up, while maintaining accuracy and sensitivity in both LC and GC applications. Utilizing this novel GC-APCI instrument, this project aims to develop and validate a new UOA method for clinical use. Furthermore, utilizing the machine’s MRM mode would increase sensitivities thus allowing for hopefully quantitative analysis. Chemical standards and patient urine samples were extracted via a liquid-liquid ether extraction and derivatized with BSTFA for proper GC elution. Results were compared on the current gold standard GC-EI-MS instrument and the new GC-APCI-MS instrument. Initial instrument suitability and method setup was then optimized. Source moisture levels were modified to explore the wet proton transfer and the dry charge transfer mechanism using [M+H]+ and [M+*]+ ion peak ratios, respectively. Elution times and APCI ion mass spectra profiles of UOA metabolites of interest were identified from full scan mode in preparation for MRM mode analysis. Exploration into the wet and dry mode settings of the APCI source determined that the former induced via methanol had greater peak areas and signal-to-noise ratios. Suitable MRMs were determined for clinically relevant organic acids from which a quantitative assay was developed for methyl malonic acid and several other compounds. The Waters’ Xevo TQ-S micro with Agilent 7890 GC demonstrated promising GC-APCI-MS detection of urine organic acids. With clear avenues for future work, the APCI technique hints at great benefits for biochemical genetic laboratories. / Thesis / Master of Science (MSc) / Inborn errors of metabolism (IEM) are a class of genetic diseases that when left untreated, cause reduced quality of life and sometimes death in newborns. Urine organic acid (UOA) analysis is used for detection using an instrument called GC-EI-MS (Gas Chromatography Electron Impact Mass Spectroscopy). This project explores how a new instrument, the Agilent 7890 GC and the Waters’ Xevo TQ-S MS, can detect these genetic diseases using a technique called APCI (Atmospheric Pressure Chemical Ionization) while still being accurate and sensitive. UOAs are isolated from urine and run through the new machine. When compared to the currently used technique, results were promising but further optimization is needed. Using the new machine, various UOA compounds that were elevated and/or decreased in newborns with genetics diseases were identified and quantified. With clear avenues for future work, the APCI technique can greatly improve newborn diagnosis of IEMs.
94

Intracellular Processing of Cobalamins in Mammalian Cells

Hannibal, Luciana 20 July 2009 (has links)
No description available.
95

Aplicabilidade clínica da técnica de sequenciamento de nova geração com enfoque em displasias esqueléticas / Clinical applicability of the next generation sequencing technique with a focus on skeletal dysplasias

Yamamoto, Guilherme Lopes 26 September 2017 (has links)
INTRODUÇÃO: Na última década surgiu uma nova técnica, o sequenciamento de nova geração, que, contrário ao método tradicional de Sanger, permite o sequenciamento em paralelo e em larga escala de múltiplos genes, ou até mesmo todos os genes humanos, a menor custo e com uma análise mais acelerada. Essa técnica possibilitou a descoberta de novos genes responsáveis por diversas doenças mendelianas, sendo rapidamente incorporada no contexto clínico. OBJETIVOS: comparar os resultados das técnicas de Sanger e sequenciamento de nova geração em amostras controle; introduzir a técnica de sequenciamento de nova geração no contexto clínico nas casuísticas de doenças ósseas genéticas e RASopatias; avaliar a sensibilidade diagnóstica desta técnica em amostras sem dados clínicos fornecidos. MÉTODOS: o sequenciamento de nova geração (sob a forma de um painel de genes customizado ou do exoma) foi realizado em amostras com mutações identificadas previamente por Sanger e em dois grupos de doenças mendelianas, 144 pacientes com doenças ósseas e 79 com RASopatias, além de 90 amostras sem dados clínicos conhecidos (45 casos e 45 controles). A técnica de Sanger foi aplicada em 29 amostras de doenças ósseas e em 81 amostras para confirmação de variantes identificadas pelo sequenciamento de nova geração. RESULTADOS: A sensibilidade da técnica de sequenciamento de nova geração foi estimada em 95,92% e a especificidade em 98,77%. Na casuística de doenças ósseas, a sensibilidade diagnóstica das amostras sequenciadas por Sanger foi de 69% (20/29), por painel customizado, 60% (75/125) e por exoma, 63% (12/19). Na casuística de RASopatias, a sensibilidade diagnóstica através do exoma foi de 46% (36/79). Como resultado deste trabalho, dois genes novos associados a RASopatias (LZTR1 e SOS2) e um associado a uma displasia esquelética (PCYT1A) foram identificados. Na análise das amostras sem conhecimento prévio da hipótese clínica foi obtida uma sensibilidade diagnóstica de 46,67% (21/45), mas que chegou a 73,08% (14/26) para as hipóteses de erros inatos do metabolismo. CONCLUSÕES: Foi demonstrado que a sensibilidade e a especificidade da técnica do sequenciamento de nova geração são altas e correspondentes a valores encontrados por outros grupos na literatura. Essa técnica foi considerada apropriada não apenas no contexto de pesquisa, demonstrado aqui pela descoberta de três novos genes associados a doenças mendelianas, como também para análises clínicas. Neste estudo a técnica foi aplicada com sucesso no contexto clínico, seja pelo painel customizado, seja pelo exoma, com uma positividade semelhante à encontrada pela técnica de Sanger. Mesmo na análise de amostras sem história clínica prévia foi possível identificar variantes patogênicas em quase metade dos casos, e numa porcentagem ainda maior quando a doença era um erro inato do metabolismo. Essa sensibilidade é comparável à obtida pela espectroscopia de massas em Tandem aplicada à triagem de múltiplas condições simultaneamente, o que sugere que a técnica do sequenciamento de nova geração poderá ser incorporada ao programa de triagem neonatal no futuro, ampliando o emprego de testes genéticos em complementaridade aos testes bioquímicos tradicionais / INTRODUCTION: In the last decade a new technique, the next generation sequencing, has emerged, which, contrary to the traditional Sanger method, performs parallel and high-throughput sequencing of multiple genes, or even all human genes, at a lower cost and with a faster analysis. This technique allowed the discovery of new genes responsible for several Mendelian diseases and has been quickly incorporated into the clinical context. OBJECTIVES: to compare the results of Sanger technique and next generation sequencing in control samples; to apply the next generation sequencing technique in the clinical practice to the cases of genetic skeletal disorders and RASopathies; to evaluate the diagnostic yield of this technique in samples without clinical data provided. METHODS: Next generation sequencing (in the form of a customized gene panel or exome) was performed in samples with mutations previously identified by Sanger sequencing and in two groups of Mendelian diseases, 144 patients with skeletal disorders and 79 patients with RASopathies, besides 90 samples with unknown clinical data (45 cases and 45 controls). The Sanger technique was applied in 29 samples of skeletal disorders and in 81 samples for confirmation of variants identified by next generation sequencing. RESULTS: The sensitivity of the next generation sequencing technique was estimated at 95.92% and the specificity at 98.77%. In the case of skeletal disorders, the diagnostic yield of the samples sequenced by Sanger was 69% (20/29), by customized panel, 60% (75/125), and by exome, 63% (12/19). In the individuals with RASopathies, the diagnostic yield through exome sequencing was 46% (36/79). As a result of this study, two new genes associated with RASopathies (LZTR1 and SOS2) and one associated with a skeletal dysplasia (PCYT1A) were identified. In the analysis of the samples without previous knowledge of the clinical hypothesis, a total diagnostic yield of 46.67% (21/45) was obtained, but it was up to 73.08% (14/26) in the group with hypothesis of inborn errors of metabolism. CONCLUSIONS: It was demonstrated that the sensitivity and specificity of the next generation sequencing technique are high and are similar to values found by other groups in the literature. The technique was considered appropriate not only for research, as demonstrated here by the identification of three new genes associated to Mendelian diseases, but also for clinical analysis. In this study the technique was successfully applied in the clinical context, both by customized panel and by exome, with positivity similar to that obtained by the Sanger technique. Even in the analysis of samples with no previous clinical history, it was possible to identify pathogenic variants in almost half of the cases, and an even greater percentage was obtained when the disease was an inborn error of metabolism. This sensitivity is comparable to that obtained by Tandem mass spectroscopy applied to multi-condition screening, suggesting that the next generation sequencing technique may be incorporated in the future into the neonatal screening program, increasing the use of genetic testing in complementarity to the biochemical tests
96

Aplicabilidade clínica da técnica de sequenciamento de nova geração com enfoque em displasias esqueléticas / Clinical applicability of the next generation sequencing technique with a focus on skeletal dysplasias

Guilherme Lopes Yamamoto 26 September 2017 (has links)
INTRODUÇÃO: Na última década surgiu uma nova técnica, o sequenciamento de nova geração, que, contrário ao método tradicional de Sanger, permite o sequenciamento em paralelo e em larga escala de múltiplos genes, ou até mesmo todos os genes humanos, a menor custo e com uma análise mais acelerada. Essa técnica possibilitou a descoberta de novos genes responsáveis por diversas doenças mendelianas, sendo rapidamente incorporada no contexto clínico. OBJETIVOS: comparar os resultados das técnicas de Sanger e sequenciamento de nova geração em amostras controle; introduzir a técnica de sequenciamento de nova geração no contexto clínico nas casuísticas de doenças ósseas genéticas e RASopatias; avaliar a sensibilidade diagnóstica desta técnica em amostras sem dados clínicos fornecidos. MÉTODOS: o sequenciamento de nova geração (sob a forma de um painel de genes customizado ou do exoma) foi realizado em amostras com mutações identificadas previamente por Sanger e em dois grupos de doenças mendelianas, 144 pacientes com doenças ósseas e 79 com RASopatias, além de 90 amostras sem dados clínicos conhecidos (45 casos e 45 controles). A técnica de Sanger foi aplicada em 29 amostras de doenças ósseas e em 81 amostras para confirmação de variantes identificadas pelo sequenciamento de nova geração. RESULTADOS: A sensibilidade da técnica de sequenciamento de nova geração foi estimada em 95,92% e a especificidade em 98,77%. Na casuística de doenças ósseas, a sensibilidade diagnóstica das amostras sequenciadas por Sanger foi de 69% (20/29), por painel customizado, 60% (75/125) e por exoma, 63% (12/19). Na casuística de RASopatias, a sensibilidade diagnóstica através do exoma foi de 46% (36/79). Como resultado deste trabalho, dois genes novos associados a RASopatias (LZTR1 e SOS2) e um associado a uma displasia esquelética (PCYT1A) foram identificados. Na análise das amostras sem conhecimento prévio da hipótese clínica foi obtida uma sensibilidade diagnóstica de 46,67% (21/45), mas que chegou a 73,08% (14/26) para as hipóteses de erros inatos do metabolismo. CONCLUSÕES: Foi demonstrado que a sensibilidade e a especificidade da técnica do sequenciamento de nova geração são altas e correspondentes a valores encontrados por outros grupos na literatura. Essa técnica foi considerada apropriada não apenas no contexto de pesquisa, demonstrado aqui pela descoberta de três novos genes associados a doenças mendelianas, como também para análises clínicas. Neste estudo a técnica foi aplicada com sucesso no contexto clínico, seja pelo painel customizado, seja pelo exoma, com uma positividade semelhante à encontrada pela técnica de Sanger. Mesmo na análise de amostras sem história clínica prévia foi possível identificar variantes patogênicas em quase metade dos casos, e numa porcentagem ainda maior quando a doença era um erro inato do metabolismo. Essa sensibilidade é comparável à obtida pela espectroscopia de massas em Tandem aplicada à triagem de múltiplas condições simultaneamente, o que sugere que a técnica do sequenciamento de nova geração poderá ser incorporada ao programa de triagem neonatal no futuro, ampliando o emprego de testes genéticos em complementaridade aos testes bioquímicos tradicionais / INTRODUCTION: In the last decade a new technique, the next generation sequencing, has emerged, which, contrary to the traditional Sanger method, performs parallel and high-throughput sequencing of multiple genes, or even all human genes, at a lower cost and with a faster analysis. This technique allowed the discovery of new genes responsible for several Mendelian diseases and has been quickly incorporated into the clinical context. OBJECTIVES: to compare the results of Sanger technique and next generation sequencing in control samples; to apply the next generation sequencing technique in the clinical practice to the cases of genetic skeletal disorders and RASopathies; to evaluate the diagnostic yield of this technique in samples without clinical data provided. METHODS: Next generation sequencing (in the form of a customized gene panel or exome) was performed in samples with mutations previously identified by Sanger sequencing and in two groups of Mendelian diseases, 144 patients with skeletal disorders and 79 patients with RASopathies, besides 90 samples with unknown clinical data (45 cases and 45 controls). The Sanger technique was applied in 29 samples of skeletal disorders and in 81 samples for confirmation of variants identified by next generation sequencing. RESULTS: The sensitivity of the next generation sequencing technique was estimated at 95.92% and the specificity at 98.77%. In the case of skeletal disorders, the diagnostic yield of the samples sequenced by Sanger was 69% (20/29), by customized panel, 60% (75/125), and by exome, 63% (12/19). In the individuals with RASopathies, the diagnostic yield through exome sequencing was 46% (36/79). As a result of this study, two new genes associated with RASopathies (LZTR1 and SOS2) and one associated with a skeletal dysplasia (PCYT1A) were identified. In the analysis of the samples without previous knowledge of the clinical hypothesis, a total diagnostic yield of 46.67% (21/45) was obtained, but it was up to 73.08% (14/26) in the group with hypothesis of inborn errors of metabolism. CONCLUSIONS: It was demonstrated that the sensitivity and specificity of the next generation sequencing technique are high and are similar to values found by other groups in the literature. The technique was considered appropriate not only for research, as demonstrated here by the identification of three new genes associated to Mendelian diseases, but also for clinical analysis. In this study the technique was successfully applied in the clinical context, both by customized panel and by exome, with positivity similar to that obtained by the Sanger technique. Even in the analysis of samples with no previous clinical history, it was possible to identify pathogenic variants in almost half of the cases, and an even greater percentage was obtained when the disease was an inborn error of metabolism. This sensitivity is comparable to that obtained by Tandem mass spectroscopy applied to multi-condition screening, suggesting that the next generation sequencing technique may be incorporated in the future into the neonatal screening program, increasing the use of genetic testing in complementarity to the biochemical tests
97

Estudo genético-clínico das displasias esqueléticas, com enfoque nas osteocondrodisplasias com acometimento do esqueleto axial, associado ao envolvimento epifisário e/ou metafisário / Genetic-Clinical study of skeletal dysplasias, with a focus on osteochondrodysplasias with the involvement of the axial skeleton, associated with epiphyseal and/or metaphyseal findings

Baratela, Wagner Antonio da Rosa 05 March 2018 (has links)
INTRODUÇÃO: As osteocondrodisplasias constituem um grupo heterogêneo de doenças que comprometem a formação, crescimento e desenvolvimento do sistema esquelético. O diagnóstico definitivo, principalmente nas formas com acometimento de coluna, epífise e/ou metáfise, é desafiador, devido à heterogeneidade genética, raridade de algumas formas específicas e da sobreposição de fenótipos clínico-radiológicos. OBJETIVOS: avaliar as características clínico-radiológicas e as bases moleculares de um grupo de pacientes com osteocondrodisplasias com envolvimento do esqueleto axial associado a anomalias epifisárias e/ou metafisárias. MÉTODOS: Foram avaliados clínica-radiologicamente 65 pacientes de 58 famílias (com mediana de idade de 9 anos e 2 meses) com osteocondrodisplasias de acometimento espôndilo-epi-metafisários pertencentes a 15 diferentes grupos da Nosologia de anomalias ósseas genéticas. Os pacientes foram classificados em cinco categorias (I,IIA,IIB,III,IV), levando-se em consideração a certeza do diagnóstico de uma determinada displasia esquelética pelos aspectos clínico-radiológicos (I,IIA,IIB,IV), o conhecimento (I,IIA,IIB) ou não (III,IV) da base molecular e o tamanho/número de éxons a serem analisados. De acordo com esta classificação, um fluxograma foi estabelecido para a decisão de qual técnica de sequenciamento seria empregada: Sanger (I) ou sequenciamento de nova geração, sob a forma de um painel de genes customizado (IIA,III) ou do exoma (IIB,III,IV). RESULTADOS: dentre os 64 pacientes analisados por um teste molecular, variantes consideradas causativas do fenótipo foram encontradas em 61 (95%). De acordo com as categorias estabelecidas, a positividade do teste genético inicial e o número de indivíduos analisados foram: categoria I (13/17), IIA (32/36), IIB (2/2), III (1/3), IV (6/6). Em sete casos (três na categoria I, dois na categoria IIA e dois na categoria III), nos quais a estratégia molecular inicial não obteve sucesso, testes moleculares adicionais foram realizados como complementação, possibilitando a identificação da base molecular das osteocondrodisplasias em questão. Em um paciente na categoria I e nos dois indivíduos da categoria IIA, nos quais não foi possível identificar uma variante patogênica, nenhum teste genético adicional foi realizado. Dentre os casos com resultados positivos, em um paciente na categoria IIB, o resultado final mudou a hipótese diagnóstica inicial; dois pacientes classificados como IIA e III, o quadro clínico presente era leve, contrastando com o quadro típico descrito nas osteocondrodisplasias causadas por mutações nos genes INPPL1 e HSPG2. No grupo de osteocondrodisplasias sem etiologia conhecida (categoria IV), foram identificadas variantes em três novos genes (PCYT1A, FN1 e LONP1). Uma re-análise nos casos negativos permitiu a identificação de mais um paciente com mutação em FN1. Mutações novas em genes previamente conhecidos foram encontradas nos genes COL2A1, COL11A1, CHST3, SLC26A2, HSPG2, ACAN, TRPV4, COMP, SMARCAL1, INPPL1, NPR2, LIFR e CANT1. CONCLUSÕES: o presente estudo mostrou que uma caracterização clínico-radiológica bem elaborada permite uma maior concordância com os testes moleculares. Em algumas situações, a sobreposição fenotípica impediu que o diagnóstico definitivo fosse estabelecido apenas por critérios clínico-radiológicos, exigindo o emprego de testes moleculares adicionais para o correto diagnóstico e, consequentemente, um aconselhamento genético mais preciso. Os achados clínico-radiológicos e moleculares contribuíram para ampliar o espectro fenotípico de algumas osteocondrodisplasias, particularmente aquelas decorrentes de variantes nos genes HSPG2 e INPPL1, além de desvendar as bases genéticas de três osteocondrodisplasias / INTRODUCTION: Osteochondrodysplasias comprise a heterogeneous group of bone disorders affecting formation, growth, and development of the skeleton. An accurate diagnosis could be challenging due to the genetic heterogeneity, rarity of specific types, and overlapping of clinical and radiographic phenotypes. OBJECTIVES: to evaluate the clincal and radiographic characteristics, as well as the molecular basis of a group of patients with spondylo-epi and/or metaphyseal osteochondrodyplasias. METHODS: Sixty-five patients from 58 families (with a median age of 9 years 2 months) with spondylo-epi-metaphyseal osteocondrodysplasias, from 15 different groups from the Nosology of Genetic Bone Disorders, were enrolled. Patients were classified into five categories (I,IIA,IIB,III,IV), considering the diagnostic certainty of a specific osteochondrodysplasia, based on clinical and radiographic findings (I,IIA,IIB,IV), the previous knowledge (I,IIA,IIB), or not (III,IV) of the molecular basis, as well as, the size/number of exons to be tested. According to this classification, a flowchart was established to aid on the molecular testing strategy: Sanger sequencing (I), or next generation sequencing, at the form of a custom targeted gene panel (IIA,III), or exome sequencing (IIB,III,IV). RESULTS: Phenotype causing variants were found in 61 out of 64 patients (95%). Based on the category system described above, the initial molecular testing positivity was: category I (13/17), IIA (32/36), IIB (2/2), III (1/3), and IV (6/6). In seven cases (three in category I, two in category IIA, and two in category III), additional genetic tests applied were able to find the causative mutation, when the initial testing strategy was not successful. For one patient in category I and two in category IIA, in whose no pathogenic mutation was found, no further molecular studies were performed. Among the positive cases, one patient in category IIB had his former clinical diagnosis changed through the molecular testing; two patients form categories IIA and III showed a milder phenotype, in contrast to the expected clinical findings in INPPL1 and HSPG2 osteochondrodysplasias. The molecular basis of three different osteochondrodysplasias (category IV) was unraveled by this study (genes PCYT1A, FN1 e LONP1). A re-analysis of the negative cases allowed the identification of another patient harboring mutation in FN1. Novel variants were found in previously known genes: COL2A1, COL11A1, CHST3, SLC26A2, HSPG2, ACAN, TRPV4, COMP, SMARCAL1, INPPL1, NPR2, LIFR, and CANT1. CONCLUSIONS: The present study showed that a well-elaborated clinical-radiological characterization allows greater correspondence with the molecular testing. In some cases, phenotypic overlap prevented the definitive diagnosis from being established only by clinical-radiological criteria, requiring the use of additional molecular tests for the correct diagnosis, and consequently, a more accurate genetic counseling. The clinical-radiographic, as well as the molecular findings, contributed to expand the clinical phenotype in certain groups, especially the variants found in patients with HSPG2 and INPPL1 osteochondrodysplasias, besides unraveling the molecular basis of three osteochondrodysplasias
98

Estudo genético-clínico das displasias esqueléticas, com enfoque nas osteocondrodisplasias com acometimento do esqueleto axial, associado ao envolvimento epifisário e/ou metafisário / Genetic-Clinical study of skeletal dysplasias, with a focus on osteochondrodysplasias with the involvement of the axial skeleton, associated with epiphyseal and/or metaphyseal findings

Wagner Antonio da Rosa Baratela 05 March 2018 (has links)
INTRODUÇÃO: As osteocondrodisplasias constituem um grupo heterogêneo de doenças que comprometem a formação, crescimento e desenvolvimento do sistema esquelético. O diagnóstico definitivo, principalmente nas formas com acometimento de coluna, epífise e/ou metáfise, é desafiador, devido à heterogeneidade genética, raridade de algumas formas específicas e da sobreposição de fenótipos clínico-radiológicos. OBJETIVOS: avaliar as características clínico-radiológicas e as bases moleculares de um grupo de pacientes com osteocondrodisplasias com envolvimento do esqueleto axial associado a anomalias epifisárias e/ou metafisárias. MÉTODOS: Foram avaliados clínica-radiologicamente 65 pacientes de 58 famílias (com mediana de idade de 9 anos e 2 meses) com osteocondrodisplasias de acometimento espôndilo-epi-metafisários pertencentes a 15 diferentes grupos da Nosologia de anomalias ósseas genéticas. Os pacientes foram classificados em cinco categorias (I,IIA,IIB,III,IV), levando-se em consideração a certeza do diagnóstico de uma determinada displasia esquelética pelos aspectos clínico-radiológicos (I,IIA,IIB,IV), o conhecimento (I,IIA,IIB) ou não (III,IV) da base molecular e o tamanho/número de éxons a serem analisados. De acordo com esta classificação, um fluxograma foi estabelecido para a decisão de qual técnica de sequenciamento seria empregada: Sanger (I) ou sequenciamento de nova geração, sob a forma de um painel de genes customizado (IIA,III) ou do exoma (IIB,III,IV). RESULTADOS: dentre os 64 pacientes analisados por um teste molecular, variantes consideradas causativas do fenótipo foram encontradas em 61 (95%). De acordo com as categorias estabelecidas, a positividade do teste genético inicial e o número de indivíduos analisados foram: categoria I (13/17), IIA (32/36), IIB (2/2), III (1/3), IV (6/6). Em sete casos (três na categoria I, dois na categoria IIA e dois na categoria III), nos quais a estratégia molecular inicial não obteve sucesso, testes moleculares adicionais foram realizados como complementação, possibilitando a identificação da base molecular das osteocondrodisplasias em questão. Em um paciente na categoria I e nos dois indivíduos da categoria IIA, nos quais não foi possível identificar uma variante patogênica, nenhum teste genético adicional foi realizado. Dentre os casos com resultados positivos, em um paciente na categoria IIB, o resultado final mudou a hipótese diagnóstica inicial; dois pacientes classificados como IIA e III, o quadro clínico presente era leve, contrastando com o quadro típico descrito nas osteocondrodisplasias causadas por mutações nos genes INPPL1 e HSPG2. No grupo de osteocondrodisplasias sem etiologia conhecida (categoria IV), foram identificadas variantes em três novos genes (PCYT1A, FN1 e LONP1). Uma re-análise nos casos negativos permitiu a identificação de mais um paciente com mutação em FN1. Mutações novas em genes previamente conhecidos foram encontradas nos genes COL2A1, COL11A1, CHST3, SLC26A2, HSPG2, ACAN, TRPV4, COMP, SMARCAL1, INPPL1, NPR2, LIFR e CANT1. CONCLUSÕES: o presente estudo mostrou que uma caracterização clínico-radiológica bem elaborada permite uma maior concordância com os testes moleculares. Em algumas situações, a sobreposição fenotípica impediu que o diagnóstico definitivo fosse estabelecido apenas por critérios clínico-radiológicos, exigindo o emprego de testes moleculares adicionais para o correto diagnóstico e, consequentemente, um aconselhamento genético mais preciso. Os achados clínico-radiológicos e moleculares contribuíram para ampliar o espectro fenotípico de algumas osteocondrodisplasias, particularmente aquelas decorrentes de variantes nos genes HSPG2 e INPPL1, além de desvendar as bases genéticas de três osteocondrodisplasias / INTRODUCTION: Osteochondrodysplasias comprise a heterogeneous group of bone disorders affecting formation, growth, and development of the skeleton. An accurate diagnosis could be challenging due to the genetic heterogeneity, rarity of specific types, and overlapping of clinical and radiographic phenotypes. OBJECTIVES: to evaluate the clincal and radiographic characteristics, as well as the molecular basis of a group of patients with spondylo-epi and/or metaphyseal osteochondrodyplasias. METHODS: Sixty-five patients from 58 families (with a median age of 9 years 2 months) with spondylo-epi-metaphyseal osteocondrodysplasias, from 15 different groups from the Nosology of Genetic Bone Disorders, were enrolled. Patients were classified into five categories (I,IIA,IIB,III,IV), considering the diagnostic certainty of a specific osteochondrodysplasia, based on clinical and radiographic findings (I,IIA,IIB,IV), the previous knowledge (I,IIA,IIB), or not (III,IV) of the molecular basis, as well as, the size/number of exons to be tested. According to this classification, a flowchart was established to aid on the molecular testing strategy: Sanger sequencing (I), or next generation sequencing, at the form of a custom targeted gene panel (IIA,III), or exome sequencing (IIB,III,IV). RESULTS: Phenotype causing variants were found in 61 out of 64 patients (95%). Based on the category system described above, the initial molecular testing positivity was: category I (13/17), IIA (32/36), IIB (2/2), III (1/3), and IV (6/6). In seven cases (three in category I, two in category IIA, and two in category III), additional genetic tests applied were able to find the causative mutation, when the initial testing strategy was not successful. For one patient in category I and two in category IIA, in whose no pathogenic mutation was found, no further molecular studies were performed. Among the positive cases, one patient in category IIB had his former clinical diagnosis changed through the molecular testing; two patients form categories IIA and III showed a milder phenotype, in contrast to the expected clinical findings in INPPL1 and HSPG2 osteochondrodysplasias. The molecular basis of three different osteochondrodysplasias (category IV) was unraveled by this study (genes PCYT1A, FN1 e LONP1). A re-analysis of the negative cases allowed the identification of another patient harboring mutation in FN1. Novel variants were found in previously known genes: COL2A1, COL11A1, CHST3, SLC26A2, HSPG2, ACAN, TRPV4, COMP, SMARCAL1, INPPL1, NPR2, LIFR, and CANT1. CONCLUSIONS: The present study showed that a well-elaborated clinical-radiological characterization allows greater correspondence with the molecular testing. In some cases, phenotypic overlap prevented the definitive diagnosis from being established only by clinical-radiological criteria, requiring the use of additional molecular tests for the correct diagnosis, and consequently, a more accurate genetic counseling. The clinical-radiographic, as well as the molecular findings, contributed to expand the clinical phenotype in certain groups, especially the variants found in patients with HSPG2 and INPPL1 osteochondrodysplasias, besides unraveling the molecular basis of three osteochondrodysplasias
99

Physiopathologie des maladies métaboliques héréditaires des acyls-Coenzyme A révélée par l’étude d’un modèle animal déficient en 3-hydroxy-3-méthylglutaryl-Coenzyme A lyase

Gauthier, Nicolas 04 1900 (has links)
La plupart des conditions détectées par le dépistage néonatal sont reliées à l'une des enzymes qui dégradent les acyls-CoA mitochondriaux. Le rôle physiopathologique des acyls-CoA dans ces maladies est peu connue, en partie parce que les esters liés au CoA sont intracellulaires et les échantillons tissulaires de patients humains ne sont généralement pas disponibles. Nous avons créé une modèle animal murin de l'une de ces maladies, la déficience en 3-hydroxy-3-methylglutaryl-CoA lyase (HL), dans le foie (souris HLLKO). HL est la dernière enzyme de la cétogenèse et de la dégradation de la leucine. Une déficience chronique en HL et les crises métaboliques aigües, produisent chacune un portrait anormal et distinct d'acyls-CoA hépatiques. Ces profils ne sont pas prévisibles à partir des niveaux d'acides organiques urinaires et d'acylcarnitines plasmatiques. La cétogenèse est indétectable dans les hépatocytes HLLKO. Dans les mitochondries HLLKO isolées, le dégagement de 14CO2 à partir du [2-14C]pyruvate a diminué en présence de 2-ketoisocaproate (KIC), un métabolite de la leucine. Au test de tolérance au pyruvate, une mesure de la gluconéogenèse, les souris HLLKO ne présentent pas la réponse hyperglycémique normale. L'hyperammoniémie et l'hypoglycémie, des signes classiques de plusieurs erreurs innées du métabolisme (EIM) des acyls-CoA, surviennent de façon spontanée chez des souris HLLKO et sont inductibles par l'administration de KIC. Une charge en KIC augmente le niveau d'acyls-CoA reliés à la leucine et diminue le niveau d'acétyl-CoA. Les mitochondries des hépatocytes des souris HLLKO traitées avec KIC présentent un gonflement marqué. L'hyperammoniémie des souris HLLKO répond au traitement par l'acide N-carbamyl-L-glutamique. Ce composé permet de contourner une enzyme acétyl-CoA-dépendante essentielle pour l’uréogenèse, le N-acétylglutamate synthase. Ceci démontre un mécanisme d’hyperammoniémie lié aux acyls-CoA. Dans une deuxième EIM des acyls-CoA, la souris SCADD, déficiente en déshydrogénase des acyls-CoA à chaînes courtes. Le profil des acyls-CoA hépatiques montre un niveau élevé du butyryl-CoA particulièrement après un jeûne et après une charge en triglycérides à chaîne moyenne précurseurs du butyryl-CoA. / Most conditions detected by expanded newborn screening result from deficiency of one of the enzymes that degrade acyl-CoA esters in mitochondria. The role of acyl-CoAs in the pathophysiology of these disorders is poorly understood, in part because CoA esters are intracellular and samples are not generally available from human patients. We created a mouse model of one such condition, deficiency of 3-hydroxy-3-methylglutaryl-CoA lyase (HL), in liver (HLLKO mice). HL catalyses a reaction of ketone body synthesis and of leucine degradation. Chronic HL deficiency and acute crises each produced distinct abnormal liver acyl-CoA patterns, which would not be predictable from levels of urine organic acids and plasma acylcarnitines. In HLLKO hepatocytes, ketogenesis was undetectable. Measures of Krebs cycle flux diminished following incubation of HLLKO mitochondria with the leucine metabolite 2-ketoisocaproate (KIC). HLLKO mice also had suppression of the normal hyperglycemic response to a systemic pyruvate load, a measure of gluconeogenesis. Hyperammonemia and hypoglycemia, cardinal features of many inborn errors of acyl-CoA metabolism, occurred spontaneously in some HLLKO mice and were inducible by administering KIC. KIC loading also increased levels of several leucine-related acyl-CoAs and reduced acetyl-CoA levels. Ultrastructurally, hepatocyte mitochondria of KIC-treated HLLKO mice show marked swelling. KIC-induced hyperammonemia improved following administration of carglumate (N-carbamyl-L-glutamic acid), which bypasses an acetyl-CoA-dependent reaction essential for urea cycle function, thus demonstrating an acyl-CoA-related mechanism for this complication. In a second animal model of an inborn error of acyl-CoA metabolism, short chain acyl-CoA dehydrogenase (SCAD)-deficient mice, the main finding in liver acyl-CoAs is increased butyryl-CoA, particularly during fasting or after enteral loading with medium chain triglyceride precursor of butyryl-CoA.
100

O tratamento da doença de Gaucher no Sistema Único de Saúde: o caso do Rio de Janeiro

Magalhães, Tatiana de Sá Pacheco Carneiro de January 2013 (has links)
Made available in DSpace on 2014-08-26T17:31:46Z (GMT). No. of bitstreams: 2 license.txt: 1748 bytes, checksum: 8a4605be74aa9ea9d79846c1fba20a33 (MD5) 69585.pdf: 1181357 bytes, checksum: 50462d1ba789c7b199ee8460ca90f3b8 (MD5) / Fundação Oswaldo Cruz. Instituto Fernandes Figueira. Departamento de Ensino. Programa de Pós-Graduação em Saúde da Criança e da Mulher. Rio de Janeiro, RJ, Brasil / A Doença de Gaucher (DG) é uma Doença de Depósito Lisossômico (DDL) e seu tratamento baseia - se na terapia de reposição enzimática. Tal terapia foi um marco na vida de pacientes e especialistas, pois mudou a história da evolução da doença, caracterizando um a nova era na Genética Médica. Este trabalho tem como objeto de pesquisa as perspectivas trazidas por profissionais, com experiência em trata r a Doença de Gaucher no Sistema Único de Saúde no estado do Rio de Janeiro. Uma vez que a DG é a única condição d o grupo das DDL a ser contemplada por uma Política Ministerial, promovendo acesso a drogas de alto custo através de um Protocolo Clínico e Diretrizes Terapêuticas (PCDT). O o bjetivo geral foi a nalisar a prática da aplicação do protocolo oficial de tratame nto da DG e o seu entendimento a partir da ótica dos médicos tratadores, profissionais de saúde e gestores do Centro de Referência , o Instituto Estadual de Hematologia Arthur de Siqueira Cavalcanti (HEMORIO). Os objetivos específicos foram primeiramente id entificar a formaçã o profissional dos envolvidos no programa, analisar a ótica desses profissionais sob re as recomendações do PCDT e como estes situam o Centro de Referência (CR) e m seu atual funcionamento , e d iscutir de maneira crítica a visão dos profiss i onais a respeito dos benefícios e de possíveis falhas do programa. Foram realizadas entrevistas temáticas semiestruturadas e a elas aplicou - se a análise de conteúdo. No que tange ao entendimento sobre o PCDT - DG e o seu viii funcionamento, os resultados apontam a importância da existência de um balizador, um programa robusto governamental, revisado por especialistas bem capacitados no tema. O PCDT - DG foi um avanço na saúde, oficializando e garantindo o acesso à medicação de maneira embasada, controlada por câmar as técnicas estaduais, permitindo a efetuação de pregões públicos, uma maneira transparente de aquisiçã o de drogas de alto custo comparada a medidas judiciais . Os sujeitos da pesquisa são favoráveis ao programa, no entanto possuem uma abordagem crítica ao sistema de saúde no que diz respeit o a entraves na rede de assistência cirúrgica e de reabilitação. Um grande gargalo atualmente no SUS não é exclusivo ao programa da DG: certos questionamentos éticos na fomentação do diagnóstico laboratorial por parte da indústria farmacêutica, apesar de haver relações amigáveis entre esses dois atores no CR. Concluímos que muitos avanços foram conquistados a partir da implementação do protocolo e que talvez este possa servir como modelo para garantir acesso ao tratamento de outras DDL. Algumas incongruências do siste ma são questionáveis e discutida s entre gestores, médicos e usuários, entretanto ainda são muito poucos os estudos publicados no Brasil sobre o tema . / Gaucher disease (GD) is a Lysosomal Storage Disease (LSD) and its treatment is based on enzyme replacement therapy. Such therapy was a milestone in patients `s lives and experts in the field, changing the disease natural history . This work aims at present ing the treatment of GD in the Unified Health System i n the state of Rio de Janeiro, as it is the only LSD to be covered by a Ministerial policy , which promotes access to high cost drugs through a Clinical Gui deline (CG) . The overall objective was to analyze the practical application of the CG protocol in the treatment of GD, and how this guideline was interpreted and used by the medical c haracters , health professionals and ma nagers of the Reference Center and the State Institute of Hematology Arthur de Siquei ra Cavalcanti (HEMORIO ). The specific objectives were to identify the training of those involved in the program, to analyze how professionals viewed the recommendations included in the CP, what they thought about the Reference Center for GD and to critical ly discuss the benefits and possi ble shortcomings of the program . Thematic semi - structured interviews were conducted, and the content analysis was applied. Regarding the understanding of the CP - GD and its op eration, the results point the importance of t he existence of a robust government program, reviewed by well - trained experts in the subject. The CP - GD was a health`s breakthrough , ensuring access to medication, controlled by state technical chambers, a llowing the practice of public auctions, a transpar ent way of purchasing high - cost drugs when compared to individual litigation. The steakeholder`s research were x favo rable to the program, although they criticized the health network constraints for specialized care, such as surgical services and rehabilitat ion. Another major bottleneck in the health system, not exclusive for G D is ethical issues regarding laboratory diagnosis by the pharmaceutical industry. We conclude d that many advances have been achieved from the implementation of the CP, and that hopeful ly this can serve as a model to ensure access t o treatment for other LSD. Managers, physicians and users point out some inconsistencies in the system although there is still limited published data on this subject in Brazil.

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