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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.
1

Estudo de custos em doenças crônicas não transmissíveis : manejo da cardiopatia isquêmica e diagnóstico precoce de câncer hereditário

Schlatter, Rosane Paixão January 2016 (has links)
Este estudo teve como objetivo realizar estudos de custos sob a perspectiva do Sistema Único de Saúde em dois temas relevantes para a saúde da população: o manejo clínico da cardiopatia isquêmica e os exames de diagnóstico molecular para rastreamento precoce de câncer hereditário. O estudo contempla a revisão teórica de avaliações econômicas e custos em saúde que consistiram no arcabouço conceitual para os dois temas. Para o estudo na área de cardiopatia isquêmica foi realizada uma coorte restrospectiva com 330 pacientes acompanhados em ambulatório especializado para os quais foram identificados e valorados os recursos utilizados em nível ambulatorial e hospitalar.Os resultados são apresentados no artigo 1. Nos estudos para avaliação de método diagnóstico, o câncer hereditário foi o tema escolhido, realizando-se a identificação dos custos operacionais na realização de diferentes testes para verificação de mutação do gene BRCA1 no câncer de mama hereditário no artigo 2 e para a identificação da mutação do gene TP53 p.R337H relacionado à predisposição de câncer familial no artigo 3. Esses três estudos poderão subsidiar pesquisas em outras áreas clínicas e futuras avaliações de custo-efetividade de estratégias terapêuticas nos temas abordados. / This study aimed to do direct costs analysis from the perspective of the Brazilian public health system, covering two topics which are relevant to the health of the Brazilian population: the clinical management of ischemic cardiomyopathy and of molecular diagnostic technologies for early screening in cancer genetics. The study includes a theoretical review of economic evaluations and of appropriation of costs related to health that composed the conceptual framework for the two topics. For the study of ischemic cardiomyopathy, we did a retrospective cohort with 330 patients followed in a specialized ambulatory, for whom the resources utilized in ambulatory and in-patient level were identified and valuated were used as model. The results are presented in article 1. In the studies to evaluation of diagnosis method, hereditary cancer was the chosen subject and we did the identification of operational costs involved in the testing for the mutation of the BRCA1 gene in hereditary breast cancer in article 2 and in the testing for the mutation of the TP53 p.R337H gene, which relates to the predisposition to familial cancer, in article 3. These three studies may subsidize research in other clinical fields, as well as future cost-effectiveness evaluations of therapeutic strategies regarding the broached subjects.
2

Estudo de custos em doenças crônicas não transmissíveis : manejo da cardiopatia isquêmica e diagnóstico precoce de câncer hereditário

Schlatter, Rosane Paixão January 2016 (has links)
Este estudo teve como objetivo realizar estudos de custos sob a perspectiva do Sistema Único de Saúde em dois temas relevantes para a saúde da população: o manejo clínico da cardiopatia isquêmica e os exames de diagnóstico molecular para rastreamento precoce de câncer hereditário. O estudo contempla a revisão teórica de avaliações econômicas e custos em saúde que consistiram no arcabouço conceitual para os dois temas. Para o estudo na área de cardiopatia isquêmica foi realizada uma coorte restrospectiva com 330 pacientes acompanhados em ambulatório especializado para os quais foram identificados e valorados os recursos utilizados em nível ambulatorial e hospitalar.Os resultados são apresentados no artigo 1. Nos estudos para avaliação de método diagnóstico, o câncer hereditário foi o tema escolhido, realizando-se a identificação dos custos operacionais na realização de diferentes testes para verificação de mutação do gene BRCA1 no câncer de mama hereditário no artigo 2 e para a identificação da mutação do gene TP53 p.R337H relacionado à predisposição de câncer familial no artigo 3. Esses três estudos poderão subsidiar pesquisas em outras áreas clínicas e futuras avaliações de custo-efetividade de estratégias terapêuticas nos temas abordados. / This study aimed to do direct costs analysis from the perspective of the Brazilian public health system, covering two topics which are relevant to the health of the Brazilian population: the clinical management of ischemic cardiomyopathy and of molecular diagnostic technologies for early screening in cancer genetics. The study includes a theoretical review of economic evaluations and of appropriation of costs related to health that composed the conceptual framework for the two topics. For the study of ischemic cardiomyopathy, we did a retrospective cohort with 330 patients followed in a specialized ambulatory, for whom the resources utilized in ambulatory and in-patient level were identified and valuated were used as model. The results are presented in article 1. In the studies to evaluation of diagnosis method, hereditary cancer was the chosen subject and we did the identification of operational costs involved in the testing for the mutation of the BRCA1 gene in hereditary breast cancer in article 2 and in the testing for the mutation of the TP53 p.R337H gene, which relates to the predisposition to familial cancer, in article 3. These three studies may subsidize research in other clinical fields, as well as future cost-effectiveness evaluations of therapeutic strategies regarding the broached subjects.
3

Estudo de custos em doenças crônicas não transmissíveis : manejo da cardiopatia isquêmica e diagnóstico precoce de câncer hereditário

Schlatter, Rosane Paixão January 2016 (has links)
Este estudo teve como objetivo realizar estudos de custos sob a perspectiva do Sistema Único de Saúde em dois temas relevantes para a saúde da população: o manejo clínico da cardiopatia isquêmica e os exames de diagnóstico molecular para rastreamento precoce de câncer hereditário. O estudo contempla a revisão teórica de avaliações econômicas e custos em saúde que consistiram no arcabouço conceitual para os dois temas. Para o estudo na área de cardiopatia isquêmica foi realizada uma coorte restrospectiva com 330 pacientes acompanhados em ambulatório especializado para os quais foram identificados e valorados os recursos utilizados em nível ambulatorial e hospitalar.Os resultados são apresentados no artigo 1. Nos estudos para avaliação de método diagnóstico, o câncer hereditário foi o tema escolhido, realizando-se a identificação dos custos operacionais na realização de diferentes testes para verificação de mutação do gene BRCA1 no câncer de mama hereditário no artigo 2 e para a identificação da mutação do gene TP53 p.R337H relacionado à predisposição de câncer familial no artigo 3. Esses três estudos poderão subsidiar pesquisas em outras áreas clínicas e futuras avaliações de custo-efetividade de estratégias terapêuticas nos temas abordados. / This study aimed to do direct costs analysis from the perspective of the Brazilian public health system, covering two topics which are relevant to the health of the Brazilian population: the clinical management of ischemic cardiomyopathy and of molecular diagnostic technologies for early screening in cancer genetics. The study includes a theoretical review of economic evaluations and of appropriation of costs related to health that composed the conceptual framework for the two topics. For the study of ischemic cardiomyopathy, we did a retrospective cohort with 330 patients followed in a specialized ambulatory, for whom the resources utilized in ambulatory and in-patient level were identified and valuated were used as model. The results are presented in article 1. In the studies to evaluation of diagnosis method, hereditary cancer was the chosen subject and we did the identification of operational costs involved in the testing for the mutation of the BRCA1 gene in hereditary breast cancer in article 2 and in the testing for the mutation of the TP53 p.R337H gene, which relates to the predisposition to familial cancer, in article 3. These three studies may subsidize research in other clinical fields, as well as future cost-effectiveness evaluations of therapeutic strategies regarding the broached subjects.
4

Tumeurs des maxillaires avec anomalies du développement : à partir des modèles de tumeurs kératokystiques odontogènes et du chérubinisme / Developmental disease associated to jaw bone tumors : from 2 models keratocystic odontogenic tumor and Cherubism

Kadlub, Natacha 25 September 2015 (has links)
Afin de mieux comprendre les bases physiopathologiques des tumeurs osseuses des mâchoires, nous avons étudié deux modèles de tumeurs associées à des mutations génétiques connues : la tumeur kératokystique odontogène (TKO), liée à la mutation de PTCH1, et le chérubinisme, lié à la mutation de SH3BP2. Au regard des travaux d’oncogénétique, nous formulons l’hypothèse que le développement des tumeurs ostéolytiques bénignes des mâchoires de l’enfant et leur agressivité repose sur un mécanisme génétique. Nous avons montré que la présence d’une mutation de PTCH1 (germinale avec syndrome de Gorlin) dans les TKO était un facteur de mauvais pronostic, stimulant un centre tumoral secondaire, responsable de lésions à distance, mais que cette agressivité pouvait aussi être liée à des mécanismes inflammatoires. Dans le chérubinisme, nous avons montré que la mutation était responsable du phénotype, mais que le type de mutation n’influençait pas le pronostic ni l’agressivité. L’agressivité tumorale est liée au phénotype des cellules géantes multinucléées (cellules myéloïdes à différenciation macrophagique ou ostéoclastique). Nous avons montré, que le modèle murin ne pouvait pas s’appliquer à la pathologie humaine, avec notamment un rôle très secondaire du TNF-α. Enfin nous avons démontré le rôle important de NFATc1 dans la physiopathologie du chérubinisme qui nous a permis de proposer, le tacrolimus, comme le premier agent thérapeutique efficace. Nos résultats suggèrent que les mutations induisent la pathologie et que les changements du microenvironnement (liés à la flore buccale ou à l’éruption dentaire) entretiennent la pathologie. / To determine pathophysiological bases of jawbone tumors, we studied two genetic models of jawbone tumors: keratocystic odontogenic tumors (KOT) associated to PTCH1 mutation and cherubism associated to SH3BP2 mutation. From oncogenetic theory, we postulate that genetic background controls the development of benign children jawbone tumors. From our work, we demonstrated that PTCH1 mutation (germline mutation in Gorlin syndrome) was an unfavorable prognosis factor for KOT, leading to distant and independent daughter tumors. Moreover, we showed, that chorionic inflammation was associated with a high recurrence rate. In cherubism, SH3BP2 mutation produced cherubism phenotype, but the type of mutation did not affect the aggressiveness of the disease. Cherubism aggressiveness was determined by the phenotype of giant multinucleated cells (whether osteoclasts or macrophages). Furthermore, we showed that murine model could not be transposed to human pathology; indeed it appeared that TNF- α did not play a critical role in human cherubism. On the other side, we showed that NFATc1 played a crucial role in cherubism pathophysiology; this observation allowed us to propose, the tacrolimus, as an effective treatment for this disease. Our results suggest that genetic background induced tumor development, and that microenvironment changes (due to flora of the oral cavity and to teeth eruptions) are responsible to the maintenance and the progression of the disease.
5

Tumeurs des maxillaires avec anomalies du développement : à partir des modèles de tumeurs kératokystiques odontogènes et du chérubinisme / Developmental disease associated to jaw bone tumors : from 2 models keratocystic odontogenic tumor and Cherubism

Kadlub, Natacha 25 September 2015 (has links)
Afin de mieux comprendre les bases physiopathologiques des tumeurs osseuses des mâchoires, nous avons étudié deux modèles de tumeurs associées à des mutations génétiques connues : la tumeur kératokystique odontogène (TKO), liée à la mutation de PTCH1, et le chérubinisme, lié à la mutation de SH3BP2. Au regard des travaux d’oncogénétique, nous formulons l’hypothèse que le développement des tumeurs ostéolytiques bénignes des mâchoires de l’enfant et leur agressivité repose sur un mécanisme génétique. Nous avons montré que la présence d’une mutation de PTCH1 (germinale avec syndrome de Gorlin) dans les TKO était un facteur de mauvais pronostic, stimulant un centre tumoral secondaire, responsable de lésions à distance, mais que cette agressivité pouvait aussi être liée à des mécanismes inflammatoires. Dans le chérubinisme, nous avons montré que la mutation était responsable du phénotype, mais que le type de mutation n’influençait pas le pronostic ni l’agressivité. L’agressivité tumorale est liée au phénotype des cellules géantes multinucléées (cellules myéloïdes à différenciation macrophagique ou ostéoclastique). Nous avons montré, que le modèle murin ne pouvait pas s’appliquer à la pathologie humaine, avec notamment un rôle très secondaire du TNF-α. Enfin nous avons démontré le rôle important de NFATc1 dans la physiopathologie du chérubinisme qui nous a permis de proposer, le tacrolimus, comme le premier agent thérapeutique efficace. Nos résultats suggèrent que les mutations induisent la pathologie et que les changements du microenvironnement (liés à la flore buccale ou à l’éruption dentaire) entretiennent la pathologie. / To determine pathophysiological bases of jawbone tumors, we studied two genetic models of jawbone tumors: keratocystic odontogenic tumors (KOT) associated to PTCH1 mutation and cherubism associated to SH3BP2 mutation. From oncogenetic theory, we postulate that genetic background controls the development of benign children jawbone tumors. From our work, we demonstrated that PTCH1 mutation (germline mutation in Gorlin syndrome) was an unfavorable prognosis factor for KOT, leading to distant and independent daughter tumors. Moreover, we showed, that chorionic inflammation was associated with a high recurrence rate. In cherubism, SH3BP2 mutation produced cherubism phenotype, but the type of mutation did not affect the aggressiveness of the disease. Cherubism aggressiveness was determined by the phenotype of giant multinucleated cells (whether osteoclasts or macrophages). Furthermore, we showed that murine model could not be transposed to human pathology; indeed it appeared that TNF- α did not play a critical role in human cherubism. On the other side, we showed that NFATc1 played a crucial role in cherubism pathophysiology; this observation allowed us to propose, the tacrolimus, as an effective treatment for this disease. Our results suggest that genetic background induced tumor development, and that microenvironment changes (due to flora of the oral cavity and to teeth eruptions) are responsible to the maintenance and the progression of the disease.
6

Tumeurs des maxillaires avec anomalies du développement : à partir des modèles de tumeurs kératokystiques odontogènes et du chérubinisme / Developmental disease associated to jaw bone tumors : from 2 models keratocystic odontogenic tumor and Cherubism

Kadlub, Natacha 25 September 2015 (has links)
Afin de mieux comprendre les bases physiopathologiques des tumeurs osseuses des mâchoires, nous avons étudié deux modèles de tumeurs associées à des mutations génétiques connues : la tumeur kératokystique odontogène (TKO), liée à la mutation de PTCH1, et le chérubinisme, lié à la mutation de SH3BP2. Au regard des travaux d’oncogénétique, nous formulons l’hypothèse que le développement des tumeurs ostéolytiques bénignes des mâchoires de l’enfant et leur agressivité repose sur un mécanisme génétique. Nous avons montré que la présence d’une mutation de PTCH1 (germinale avec syndrome de Gorlin) dans les TKO était un facteur de mauvais pronostic, stimulant un centre tumoral secondaire, responsable de lésions à distance, mais que cette agressivité pouvait aussi être liée à des mécanismes inflammatoires. Dans le chérubinisme, nous avons montré que la mutation était responsable du phénotype, mais que le type de mutation n’influençait pas le pronostic ni l’agressivité. L’agressivité tumorale est liée au phénotype des cellules géantes multinucléées (cellules myéloïdes à différenciation macrophagique ou ostéoclastique). Nous avons montré, que le modèle murin ne pouvait pas s’appliquer à la pathologie humaine, avec notamment un rôle très secondaire du TNF-α. Enfin nous avons démontré le rôle important de NFATc1 dans la physiopathologie du chérubinisme qui nous a permis de proposer, le tacrolimus, comme le premier agent thérapeutique efficace. Nos résultats suggèrent que les mutations induisent la pathologie et que les changements du microenvironnement (liés à la flore buccale ou à l’éruption dentaire) entretiennent la pathologie. / To determine pathophysiological bases of jawbone tumors, we studied two genetic models of jawbone tumors: keratocystic odontogenic tumors (KOT) associated to PTCH1 mutation and cherubism associated to SH3BP2 mutation. From oncogenetic theory, we postulate that genetic background controls the development of benign children jawbone tumors. From our work, we demonstrated that PTCH1 mutation (germline mutation in Gorlin syndrome) was an unfavorable prognosis factor for KOT, leading to distant and independent daughter tumors. Moreover, we showed, that chorionic inflammation was associated with a high recurrence rate. In cherubism, SH3BP2 mutation produced cherubism phenotype, but the type of mutation did not affect the aggressiveness of the disease. Cherubism aggressiveness was determined by the phenotype of giant multinucleated cells (whether osteoclasts or macrophages). Furthermore, we showed that murine model could not be transposed to human pathology; indeed it appeared that TNF- α did not play a critical role in human cherubism. On the other side, we showed that NFATc1 played a crucial role in cherubism pathophysiology; this observation allowed us to propose, the tacrolimus, as an effective treatment for this disease. Our results suggest that genetic background induced tumor development, and that microenvironment changes (due to flora of the oral cavity and to teeth eruptions) are responsible to the maintenance and the progression of the disease.
7

Molekulargenetische Veränderungen in nicht kleinzelligen Bronchialkarzinomen, detektiert durch komparative genomische Hybridisierung (CGH) / Molecular genetic changes in non small cell lung cancer, detected by comparative genomic hybridization (CGH)

Hellms, Timo 22 January 2013 (has links)
No description available.
8

Implication des remaniements géniques dans l'inactivation des gènes de prédisposition au cancer du sein / Germline large rearrangements in the inactivation of genes implied in breast cancer predisposition

Rouleau, Etienne 07 December 2011 (has links)
Parmi les cancers du sein, 5 à 10% serait associé à une prédisposition génétique familiale. La prise en charge des patients prédisposés nécessite une bonne définition des risques de cancer. L’identification de l’altération moléculaire causale dans chacune de ces familles est donc un enjeu essentiel dans la prise en charge médicale. Deux gènes, BRCA1 et BRCA2, sont associés à une prédisposition majeure au cancer du sein et de l’ovaire depuis le milieu des années 1990, expliquant environ 15% des formes héréditaires. L’analyse moléculaire de ces deux gènes est désormais réalisée en routine pour la recherche de variations nucléotidiques et plus récemment de remaniements géniques ce qui a permis d’améliorer le taux de détection de mutations délétères. Cependant, pour près de 85% des familles avec une agrégation familiale ou un âge anormalement jeune de cancer du sein, aucune mutation délétère n’a pu être mise en évidence. Dans ce contexte, mon travail de thèse a eu pour objectif de tester plusieurs hypothèses permettant d’expliquer les risques de cancer du sein observés chez des familles montrant l’absence de mutation des gènes BRCA1 et BRCA2. Nous avons ainsi recherché des mécanismes d’altération rarement explorés pour les gènes BRCA1 et BRCA2, et enfin analysé d’autres gènes candidats dont le gène CDH1 et huit autres gènes impliqués dans la réparation de l’ADN. Nous avons pu mieux caractériser des remaniements sur les gènes BRCA1 et BRCA2. Enfin, nous avons pu évaluer l’impact de variants de signification inconnue et des réarrangements détectés par l’étude de leurs transcrits. Dans un premier temps, nous avons mis en place et validé de nouvelles approches techniques de détection et de caractérisation : la CGH-array dédiée, la qPCR-HRM et le peignage moléculaire. Ces techniques ont ensuite été utilisées pour étudier les remaniements géniques et leur fréquence pour onze gènes candidats à la prédisposition au cancer du sein à partir de 472 familles négatives aux mutations délétères BRCA1 et BRCA2. Parmi ces 11 gènes, nous pouvons conclure que les remaniements géniques détectés concernent principalement les gènes BRCA1 et BRCA2, et à un moindre degré le gène CHEK2. En appliquant ces techniques, nous avons pu décrire de nouveaux événements, deux larges délétions et une duplication intronique, pour les gènes CDH1 et BARD1, ouvrant de nouvelles perspectives sur l’étude des transcrits alternatifs. Nous avons en particulier pu décrire la grande diversité des réarrangements délétères en 5’ du gène BRCA1. L’enjeu est ensuite l’interprétation de ces événements. Notre étude des transcrits a permis de décrire un variant exonique d’épissage entraînant une délétion de l’exon 23 au niveau du transcrit BRCA1. Nous avons aussi validé la pathogénicité d’un réarrangement en phase de l’exon 3 de BRCA2 par une étude quantitative du transcrit et une évaluation de la coségrégation. Au final, moins de 1% de nouveaux remaniements ont été mis en évidence. Ce travail est riche d’enseignement pour les nouvelles investigations à mettre en place pour les familles prédisposées. En dehors de la technique d’identification, il est nécessaire de développer des stratégies de validation basées principalement sur la quantification des effets de ces altérations au niveau de l’ARN et des protéines. Cependant, il manque encore de nombreux chaînons pour expliquer l’héritabilité des cancers du sein. Les études sur les nouveaux gènes candidats et l’avènement des techniques de séquençage pangénome à haut débit, devraient permettre d’avoir une meilleure vision des phénomènes pathobiologiques liés à la prédisposition au cancer du sein. / Five to 10% of breast cancers are linked to a genetic predisposition. The management of patients at risk requires a good definition in the risk of cancer. The identification of causal molecular alterations in each of these families is a key issue in medical care. Two genes, BRCA1 and BRCA2, are related with the greatest susceptibility to breast cancer and ovarian cancer since the mid-1990s, accounting for about 15% of hereditary forms. Molecular analysis of these two genes is now routinely performed for the detection of nucleotide variations and more recently large rearrangements which have improved the detection rate of deleterious mutations. However, for more than 85% of families, no mutation explains familial aggregation or unusual young age of breast cancer onset. In this context, my thesis aimed at testing several hypotheses to explain the risks of breast cancer observed in families without any identified mutations in the BRCA1 and BRCA2 genes. We investigated some mechanisms of genic rearrangements rarely explored for BRCA1 and BRCA2 genes, and finally investigated other candidate genes, especially CDH1 gene and eight other genes involved in double-strand DNA repair. We have better characterized some rearrangements in the BRCA1 and BRCA2 genes. Finally, we applied RNA quantitative approaches to better assess the impact from variants of unknown significance and detected rearrangements. Initially, we developed and validated new technical approaches for detection and characterization such as dedicated CGH-array, qPCR-HRM and molecular combing. Rare large germline rearrangements and their frequency in eleven candidate genes for susceptibility to breast cancer were studied among 472 families negative by routine testing for BRCA1 and BRCA2 genes. Of these 11 genes, we conclude that genic rearrangements are found then mainly in the BRCA1 and BRCA2 genes, and to a lesser extent in the CHEK2 gene. We were able to describe two large intronic deletions and one duplication for the CDH1 and BARD1 genes, opening new perspectives on the regulation of their alternative transcript. In particular, we described the wide diversity of new rearrangements involving the 5' region of the BRCA1 gene. Then, it is necessary to validate and interpret those new events. Our transcript analysis described a new exonic variant causing the splice deletion of exon 23 in BRCA1 gene. We have developed tools to validate an in-frame large rearrangement of BRCA2 exon 3 with some transcript quantitative approaches and disease cosegregation.Finally, less than 1% of new rearrangements have been identified. This work is instructive for further investigations to establish molecular etiology in those families with breast cancer predisposition. Not only by applying new technologies, it is necessary to develop other strategies based primarily on quantifying effects of these alterations on transcription and traduction. However, it still lacks many links to explain the heritability of breast cancer. The combination of new candidate genes studies and the advent of high-throughput sequencing are expected to give a better vision of pathobiological phenomena related to the breast cancer predisposition.

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