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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.
21

Estudo clínico, laboratorial e anatomopatológico dos órgãos linfohematopoiéticos na síndrome de emagrecimento progressivo dos calitriquídeos mantidos em cativeiro / Clinical, laboratorial and pathological study of lymphohematopoietic organs in the wasting marmoset syndrome

Luciana Cintra 30 August 2010 (has links)
A síndrome de emagrecimento progressivo (SEP) é responsável por elevada morbidade e mortalidade de calitriquídeos mantidos em cativeiro em diferentes instituições. Essa síndrome representa um desafio aos médicos veterinários por suas características ainda pouco esclarecidas e são poucos os estudos multidisciplinares que visam à avaliação dos diferentes sistemas, como os órgãos linfo-hematopoiéticos. O objetivo foi caracterizar a evolução e duração da SEP, associando os dados clínicos, laboratoriais e anatomopatológicos dos órgãos linfo-hematopoiéticos de saguis naturalmente acometidos por SEP no cativeiro. Foram analisadas as fichas clínicas, necroscópicas e os resultados das amostras de sangue e urina de 47 saguis doentes, Callithrix spp., machos e fêmeas, que foram a óbito devido a SEP e eram provenientes de dois criadouros diferentes do estado de São Paulo. Os fragmentos dos órgãos linfo-hematopoiéticos, intestino delgado e do fígado foram processados e avaliados. Os resultados caracterizaram que a SEP acomete calitriquídeos de espécies diferentes, adultos, sem predisposição sexual, mantidos sob condições estáveis de manejo por em média 42 meses e a duração clínica varia de 41 dias a 1 ano e 7 meses. As características clínicas na fase inicial foram predominantemente sinais gastrintestinais e na fase terminal, sinais gastrintestinais e extra-intestinais. A anemia macrocítica normo ou hipocrômica com policromasia, esferocitose, presença de corpúsculos de Heinz e hemoglobinúria foi a alteração hematológica mais frequente. As lesões dos órgãos linfo-hematopoiéticos foram características de anemia hemolítica ou foram inespecíficas e reacionais caracterizadas por hiperplasia ou depleção das células da medula óssea, baço e linfonodo e lesões degenerativas no fígado. Na SEP, a associação clínica, laboratorial e anatomopatológica possibilitou a caracterização da evolução e duração clínica, da anemia e das alterações dos órgãos linfo-hematopoiéticos, cujas lesões foram consideradas secundárias à desnutrição crônica e progressiva decorrente da severa enterite atrófica. / Wasting marmoset syndrome (WMS) causes high morbidity and mortality of marmosets and tamarins kept in captivity in different colonies. WMS challenges the veterinarian due to its unclear and not established features and there are few multidisciplinary studies that carried out an evaluation of different systems, such the lymphohematopoietic system. The aim was described the duration and evolution of illness based on an association of clinical, laboratory and pathological aspects of WMS. Medical record, laboratory data and pathological findings were analyzed of 47 Callithrix spp., males and females, sick marmosets that died due to WMS in two different colonies in São Paulo state. Tissue samples of small intestine, lymphohematopoietc system and liver were histological processed and evaluated. The results showed that WMS affects adult marmosets of different species; there are no sex-related differences, and the marmosets are at least 42 months under similar general management at colony. The clinical duration of WMS is from 41 days to 1 year and 7 months. The clinical features were gastrointestinal symptoms in the beginning and extra-gastrointestinal and gastrointestinal signs in the end. Normochromic or hypochromic macrocytic anemia with polychromasia, spherocytes, Heinz bodies, and hemoglobinuria is the common hematological result. The lymphohematopoietic system lesions were the common findings of hemolytic anemia or unspecific and reacting features such as hyperplasia or depletion of cell numbers of bone marrow, spleen and lymph node, and degenerative lesions of liver. The clinical, laboratory and pathological association allowed the characterization of evolution and duration of the WMS, the anemia and the lesions of lymphohematopoietic organs which lesions were considered secondary to chronic and progressive malnutrition as a result of severe atrophic.
22

Mapeamento genético e caracterização fenotípica do mutante anêmico induzido por Ethyl-nitroso-urea. / Genetic mapping and phenotypic characterization of an anemic mutant by ethylnitrosourea.

Carolina Cavalcante da Cruz 24 September 2009 (has links)
A mutagênese química utilizando o agente mutagênico N-ethyl-N-nitrosourea (ENU) seguida da observação do fenótipo deu origem a um mutante Anêmico. O tipo de herança é autossômica dominante, com morte intra útero dos mutantes homozigotos. O mapeamento genético foi feito utilizando-se marcadores microssatélites, sendo selecionados marcadores polimórficos entre as linhagens BALB/c e C57BL/6 envolvidas no mapeamento. Estabeleceu-se um painel de microssatélites distribuídos por todo o genoma do camundongo, que permitisse a localização do cromossomo portador da mutação. O gene mutante foi localizado no cromossomo 7 entre os marcadores D7Mit301 e D7Mit131 delimitando um intervalo entre 46,5cM e 51cM de 4,5cM. Através das análises fenotípicas do mutante Anêmico e estudo dos genes candidatos neste intervalo, foi selecionado o gene Hbb responsável pela síntese das globinas b-major e b-minor , sendo o gene que mais se identifica com as características do mutante, localizado a 50cM. A deficiência deste gene leva a uma das mais severas anemias humana, a b-Talassemia major. / Chemical mutagenesis, using the mutagenic agent N-ethyl-N-nitrosourea (ENU), and followed by observation of the phenotype, originated in an Anaemic mutant. The inheritance-type is dominant auto-somic, with intra-uterus death of the homozygotic mutants. Genetic mapping was undertaken by means of micro-satellite markers, polymorphic markers being selected from among the BALB/c and C57BL/6 lineages involved in the mapping itself. A panel was established of the micro-satellites distributed throughout the whole mouse genome, thereby permitting localization of the mutation bearing chromosome. The mutant gene was located in chromosome 7 between markers D7Mit301 and D7Mit131, these delimiting an interval between 46,5cM and 51cM of 4,5cM. Selection of the Hbb gene responsible for synthesis of the b-major and b-minor globins came about through phenotypic analysis of the Anaemic mutant and a study of candidate genes within this interval, the selected gene being that which was most identified with the mutants characteristics and located at 50cM. A deficiency in this gene leads to one of the most severe forms of human anaemia, b-Talhassemia major.
23

Contribution à l'amélioration de la sécurité transfusionnelle

El Kenz, Hanane 06 November 2014 (has links)
L’objectif de notre travail est de contribuer à l’amélioration de la sécurité transfusionnelle. Pour ce faire, nous sommes partis de notre expérience personnelle en banque de sang hospitalière. Le risque infectieux lié aux transfusions, inscrit dans l’esprit de chacun depuis l’affaire du « scandale du SIDA » en France, est aujourd’hui un des risques les mieux maîtrisés. Actuellement, les risques transfusionnels les plus importants sont essentiellement de type immunologique ou liés à des erreurs humaines. Nous avons donc mis en évidence trois axes de travail correspondant chacun à un type de réaction transfusionnelle spécifique choisis parmi ces deux derniers risques. Les données d’hémovigilance internationales publiées nous ont confortés dans l’idée que ces trois sujets représentent une part importante des réactions transfusionnelles notifiées ces dix dernières années. Nous avons choisi de travailler sur la prévention des réactions transfusionnelles hémolytiques de type ABO, des réactions transfusionnelles hémolytiques chez les patients atteints d’anémie hémolytique auto-immune et des réactions d’hyperkaliémie post-transfusionnelle.<p>Notre premier travail a consisté en la démonstration de la faisabilité d’une automatisation complète du contrôle ultime au lit du malade par vérification de la compatibilité entre le groupe ABO du patient et celui de la poche de sang à transfuser. Cet appareil utilise une nouvelle technique de détection d’hémagglutination entièrement conçue et validée au sein de notre laboratoire de recherche et brevetée par l’ULB.<p>La seconde partie du travail consiste en l’évaluation d’un nouvel algorithme de prise en charge transfusionnelle des patients atteints d’anémie hémolytique autoimmune en incluant la réalisation d’un génotypage érythrocytaire permettant ainsi, d’une part, d’éviter les réactions hémolytiques transfusionnelles et, d’autre part, d’éviter de nouvelles alloimmunisations chez ces patients.<p>Dans la dernière partie du travail, nous nous sommes intéressés aux effets des liquides de conservation des poches de sang sur le relargage de potassium à partir d’unités de globules rouges irradiées destinées aux patients immunodéprimés. Nous avons pu observer des différences entre les deux solutions de conservation que nous utilisons et nous avons pu ainsi émettre de nouvelles recommandations visant à prévenir ces hyperkaliémies transfusionnelles.<p> / Doctorat en Sciences biomédicales et pharmaceutiques / info:eu-repo/semantics/nonPublished
24

Autoimmune Hemolytic Anemia After mRNA COVID Vaccine

Fatima, Zainab, Reece, Blair R., Moore, J S., Means, Robert T. 01 January 2022 (has links)
Discussion of the hematologic complications of vaccination for severe acute respiratory syndrome coronavirus-2 (COVID-19) has primarily focused on the development of vaccine-associated immune thrombosis with thrombocytopenia (VITT). Other hematologic complications are uncommon. We report the case of a patient who developed immunoglobulin G (IgG)-mediated autoimmune hemolytic anemia (AIHA) after the Moderna COVID-19 messenger ribonucleic acid (mRNA) vaccine.
25

Triagem neonatal de deficiência de glicose-6-fosfato desidrogenase e prevalência das mutações G202A (G6PD A-) e C563T (G6PD Mediterrâneo) em Mato Grosso/Brasil / Neonatal Screening for glucose-6-phosphate dehydrogenase deficiency and prevalence of G202A (G6PD A-) and C563T (G6PD mediterranean) mutations in Mato Grosso / Brazil

Ferreira, Maria de Fatima de Carvalho 12 August 2014 (has links)
Objetivos: A deficiência de glicose-6-fosfato desidrogenase (G6PD) está associada a um maior risco de encefalopatia bilirrubínica e de crise hemolítica aguda grave desencadeada por drogas como a primaquina e a dapsona. Conhecer a prevalência dessa deficiência enzimática em área onde a malária e a hanseníase ainda estão presentes e conhecer a prevalência das principais mutações traz subsídios para planejamento de estratégias com vistas à redução de riscos associados a esta deficiência enzimática. Métodos: Estudo descritivo transversal conduzido em uma região do centro-oeste do Brasil. Exame de triagem para deficiência de G6PD foi realizado em 3573 recémnascidos. Exame confirmatório foi necessário em 188 crianças triadas como possíveis portadores de deficiência. Nas crianças em que foi confirmada a deficiência de G6PD foi feita pesquisa das mutações G202A (G6PD A-) e C563T (G6PD Mediterrâneo) por PCR. Resultados: A deficiência de G6PD foi confirmada em 63 crianças, sendo 60 meninos (95,2%) e três meninas (4,8%). O percentual de exames falso-positivos na fase de triagem foi de 66,5%, estando o percentual de falso-positivos associado à temperatura e tempo de transporte das amostras. Entre as crianças que confirmaram deficiência de G6PD, foi mais frequente a história de anemia em familiares e de icterícia neonatal. Houve associação entre hematócrito baixo e deficiência enzimática, mas não com hemoglobina, contagem de reticulócitos ou neutrófilos. A prevalência da deficiência de G6PD (IC95%) foi de 1,76% (1,37; 2,24) entre os recém-nascidos triados e de 3,34% entre os meninos (2,58; 4,25). A mutação C563T não foi identificada em nenhuma criança, mas a mutação G202A estava presente em 58 crianças - 92,06% (IC95%: 83,29 - 97,03): 56/60 meninos e em 2/3 meninas homozigotas. Foi identificado um menino com Kernicterus portador da mutação G202A em hemizigose. Conclusão: O elevado percentual de falso-positivos na etapa de triagem, o tempo necessário entre coleta e confirmação da presença de deficiência enzimática, associado ao alto custo da triagem universal, não apoiam a inclusão da triagem de deficiência de G6PD no programa de triagem neonatal brasileiro. Na região avaliada, a prevalência observada em meninos indica que a triagem de deficiência de G6PD deva ser realizada antes do uso de drogas como a primaquina e a dapsona somente em meninos. Foi elevada a prevalência da mutação G202A, de classe III, sendo esta mutação associada a uma menor morbidade. A identificação de um menino com Kernicterus com deficiência de G6PD indica que há necessidade de se planejar estratégias para minimizar o risco dessa morbidade associada à deficiência enzimática / Objective: Glucose-6-phosphate dehydrogenase (G6PD) deficiency is associated with an increased risk of bilirubin encephalopathy in neonates and acute hemolytic crisis triggered by drugs such as primaquine and dapsone. In an area where malaria and Hansen\'s disease are still present, knowing the prevalence of this enzyme defect and determining the prevalence of major mutations is important for planning strategies for reducing the risks associated with this enzyme deficiency. Methods: Sectional study was conducted in a Midwestern region of Brazil. Screening for G6PD deficiency was performed in 3,573 neonates. Confirmatory tests were necessary for 188 positively screened children. After confirmation, PCR investigation was utilized to identify the mutations. Results: G6PD deficiency was confirmed in 63 children: 60 boys (95.2%) and 3 girls (4.8%). The percentage of false-positive cases in the screening phase, 66.5% and was associated with the temperature and transportation time of the samples. Family history of anemia and jaundice was more frequent among the children with confirmed G6PD deficiency. An association between a low hematocrit and enzyme deficiency was observed. However, there was no association with hemoglobin reticulocyte or neutrophils counts. The prevalence of G6PD deficiency (CI95%) was 1.76% (1.37; 2.24) among all screened neonates and 3.34% (2.58; 4.25) among male children. The C563T mutation was not identified in any child. The G202A mutation was present in 58 children - 92.06% (CI95%: 83.29 - 97.03), 56/60 boys and 2/3 homozygous girls. One boy with a hemizygous G202A mutation was identified as having Kernicterus. Conclusion: The high percentage of false-positive results when first screening for G6PD deficiency; the long delay time between the test and result; along with the high cost of the this screening test, are all factors that do not support adding this test to the already established Brazilian neonatal screening programs. The prevalence observed among boys does indicate that screening for G6PD deficiency should be performed in this region before the use of drugs such as primaquine and dapsone only in boys. This study found a high prevalence of the G202A mutation, a Class III variant associated with lower morbidity. The identification of a G6PD deficient boy with Kernicterus reinforces the necessity for strategies to abolish the morbidity associated with this enzyme deficiency
26

Triagem neonatal de deficiência de glicose-6-fosfato desidrogenase e prevalência das mutações G202A (G6PD A-) e C563T (G6PD Mediterrâneo) em Mato Grosso/Brasil / Neonatal Screening for glucose-6-phosphate dehydrogenase deficiency and prevalence of G202A (G6PD A-) and C563T (G6PD mediterranean) mutations in Mato Grosso / Brazil

Maria de Fatima de Carvalho Ferreira 12 August 2014 (has links)
Objetivos: A deficiência de glicose-6-fosfato desidrogenase (G6PD) está associada a um maior risco de encefalopatia bilirrubínica e de crise hemolítica aguda grave desencadeada por drogas como a primaquina e a dapsona. Conhecer a prevalência dessa deficiência enzimática em área onde a malária e a hanseníase ainda estão presentes e conhecer a prevalência das principais mutações traz subsídios para planejamento de estratégias com vistas à redução de riscos associados a esta deficiência enzimática. Métodos: Estudo descritivo transversal conduzido em uma região do centro-oeste do Brasil. Exame de triagem para deficiência de G6PD foi realizado em 3573 recémnascidos. Exame confirmatório foi necessário em 188 crianças triadas como possíveis portadores de deficiência. Nas crianças em que foi confirmada a deficiência de G6PD foi feita pesquisa das mutações G202A (G6PD A-) e C563T (G6PD Mediterrâneo) por PCR. Resultados: A deficiência de G6PD foi confirmada em 63 crianças, sendo 60 meninos (95,2%) e três meninas (4,8%). O percentual de exames falso-positivos na fase de triagem foi de 66,5%, estando o percentual de falso-positivos associado à temperatura e tempo de transporte das amostras. Entre as crianças que confirmaram deficiência de G6PD, foi mais frequente a história de anemia em familiares e de icterícia neonatal. Houve associação entre hematócrito baixo e deficiência enzimática, mas não com hemoglobina, contagem de reticulócitos ou neutrófilos. A prevalência da deficiência de G6PD (IC95%) foi de 1,76% (1,37; 2,24) entre os recém-nascidos triados e de 3,34% entre os meninos (2,58; 4,25). A mutação C563T não foi identificada em nenhuma criança, mas a mutação G202A estava presente em 58 crianças - 92,06% (IC95%: 83,29 - 97,03): 56/60 meninos e em 2/3 meninas homozigotas. Foi identificado um menino com Kernicterus portador da mutação G202A em hemizigose. Conclusão: O elevado percentual de falso-positivos na etapa de triagem, o tempo necessário entre coleta e confirmação da presença de deficiência enzimática, associado ao alto custo da triagem universal, não apoiam a inclusão da triagem de deficiência de G6PD no programa de triagem neonatal brasileiro. Na região avaliada, a prevalência observada em meninos indica que a triagem de deficiência de G6PD deva ser realizada antes do uso de drogas como a primaquina e a dapsona somente em meninos. Foi elevada a prevalência da mutação G202A, de classe III, sendo esta mutação associada a uma menor morbidade. A identificação de um menino com Kernicterus com deficiência de G6PD indica que há necessidade de se planejar estratégias para minimizar o risco dessa morbidade associada à deficiência enzimática / Objective: Glucose-6-phosphate dehydrogenase (G6PD) deficiency is associated with an increased risk of bilirubin encephalopathy in neonates and acute hemolytic crisis triggered by drugs such as primaquine and dapsone. In an area where malaria and Hansen\'s disease are still present, knowing the prevalence of this enzyme defect and determining the prevalence of major mutations is important for planning strategies for reducing the risks associated with this enzyme deficiency. Methods: Sectional study was conducted in a Midwestern region of Brazil. Screening for G6PD deficiency was performed in 3,573 neonates. Confirmatory tests were necessary for 188 positively screened children. After confirmation, PCR investigation was utilized to identify the mutations. Results: G6PD deficiency was confirmed in 63 children: 60 boys (95.2%) and 3 girls (4.8%). The percentage of false-positive cases in the screening phase, 66.5% and was associated with the temperature and transportation time of the samples. Family history of anemia and jaundice was more frequent among the children with confirmed G6PD deficiency. An association between a low hematocrit and enzyme deficiency was observed. However, there was no association with hemoglobin reticulocyte or neutrophils counts. The prevalence of G6PD deficiency (CI95%) was 1.76% (1.37; 2.24) among all screened neonates and 3.34% (2.58; 4.25) among male children. The C563T mutation was not identified in any child. The G202A mutation was present in 58 children - 92.06% (CI95%: 83.29 - 97.03), 56/60 boys and 2/3 homozygous girls. One boy with a hemizygous G202A mutation was identified as having Kernicterus. Conclusion: The high percentage of false-positive results when first screening for G6PD deficiency; the long delay time between the test and result; along with the high cost of the this screening test, are all factors that do not support adding this test to the already established Brazilian neonatal screening programs. The prevalence observed among boys does indicate that screening for G6PD deficiency should be performed in this region before the use of drugs such as primaquine and dapsone only in boys. This study found a high prevalence of the G202A mutation, a Class III variant associated with lower morbidity. The identification of a G6PD deficient boy with Kernicterus reinforces the necessity for strategies to abolish the morbidity associated with this enzyme deficiency
27

Autoantikūniai ant šunų eritrocitų ir trombocitų: nustatymas ir funkcinė svarba / Auto-antibodies on canine erythrocytes and platelets: detection and functional significance

Kučinskienė, Gintarė 30 December 2005 (has links)
In this study, we demonstrated that membrane immunofluorescence (MIF) with canine erythrocytes is a much more sensitive diagnostic technique compared with the Coombs test to detect auto-antibodies on RBC. We also demonstrate how the evaluation of the MIF test can be made more precisely which results in a more clear interpretation. Till nowadays the Evans syndrome (combined thrombocytopenia and anemia) is not very well diagnosed in dogs. Only a few studies with low animal numbers tested auto-antibodies on RBC and thrombocytes. Here we describe the frequency of Evans syndrome based on the evaluation of a large data set with 557 dogs. The novelty of the thesis also lies in making a research of the amount of CICs in sera of AIHA/AITP patients is described as well as the cytotoxic potential of patient’s sera for canine leucocytes. These new aspects of diagnosis (AIHA) and pathogenesis (AIHA/AITP) are not only relevant for dogs but also for humans and can be used for better differential diagnosis in medicine. The new findings with respect to circulating immune complexes and cytotoxicity are also offer new therapeutic concepts. Besides, the study has resulted in the characterization of monoclonal antibodies which allow for the detection of so far undetectable canine differentiation antigens (CD molecules) on canine erythrocytes (CD235) and thrombocytes (CD42a). The identified mAbs are useful in the identification of relevant target structures for autoantibodies on these cells.
28

Identification de causes génétiques du syndrome d’Evans pédiatrique / Identifying genetic causes of pediatric Evans syndrome

Lévy, Eva 11 May 2016 (has links)
Le syndrome d'Evans est défini par l'existence concomitante ou séquentielle de cytopénies auto-immunes, le plus souvent, anémie hémolytique et thrombopénie immunologique. Chez l'enfant, il peut être secondaire à une infection, une maladie auto-immune systémique ou un déficit immunitaire primitif. Alternativement, chez une grande partie des patients, l'étiologie n'est pas clairement identifiée. Les patients atteints de syndrome d'Evans présentent parfois d'autres atteintes, telles une auto-immunité d'organe, une lymphoprolifération bénigne ou un déficit immunitaire. L'objectif de ce travail était d'identifier des causes génétiques chez des enfants présentant un syndrome d'Evans sans étiologie sous-jacente identifiée. Nous avons centré notre étude sur des formes sévères à début pédiatrique en faisant l'hypothèse qu'une maladie monogénique serait plus fréquente dans ce groupe de patients. Nous avons mis à profit les technologies de séquençage haut débit « nouvelle génération » (NGS) pour réaliser et analyser le séquençage de l'exome de patients et de certains de leurs apparentés afin de mettre en évidence des gènes candidats potentiels. Ce travail a permis l'identification de 4 gènes candidats : LRBA, CTLA-4, STAT3 (mutations gain de fonction) et NFKBIA. L'implication des 3 premiers gènes dans de nouvelles maladies monogéniques où l'auto-immunité est au premier plan a été confirmée par d'autres équipes au cours de ce travail. Pour chacun de ces gènes, nous avons poursuivi 2 objectifs complémentaires : d'une part, tenter de valider l'implication des gènes identifiés dans la maladie des patients. Nous avons pour cela utilisé des approches et techniques variées : biochimie et protéomique afin d'identifier des partenaires protéiques, microscopie confocale pour localiser les protéines et leurs interactions, tests cellulaires in vitro pour mettre en évidence un défaut fonctionnel, marquages en cytométrie en flux pour identifier des modifications dans les sous-populations lymphocytaires. D'autre part, nous avons recherché d'autres mutations de ces gènes chez des patients de phénotype clinique similaire. Nous avons ainsi constitué et exploré 3 cohortes de patients présentant des mutations de LRBA, CTLA-4 ou STAT3. Nous avons rassemblé une cohorte de 18 patients porteurs d'une mutation de LRBA, répartis dans 11 familles. Cela nous a permis de préciser et d'étendre le spectre clinique de cette maladie de découverte récente, avec en particulier des atteintes articulaires sévères s'associant à un diabète précoce, ou des entéropathies. Nous avons identifié 15 nouvelles mutations de transmission autosomique récessive dans le gène LRBA, codant une protéine de fonction inconnue dont l'absence entraine une maladie principalement caractérisée par une poly-auto-immunité. Nous avons identifié 29 partenaires protéiques potentiels de LRBA et précisé la localisation de LRBA dans les différents compartiments cellulaires. Nous avons également établi une cohorte de 12 patients dans 10 familles présentant un déficit en CTLA-4 par haplo-insuffisance. Au delà de la mise en évidence de 9 nouvelles mutations, nous avons décrit une famille où la variation est transmise de façon autosomique récessive. Dans les déficits en LRBA et CTLA-4, nous avons mis en évidence une diminution du pourcentage de lymphocytes T régulateurs parmi les PBMC et une diminution de l'expression de CTLA-4 dans les lymphocytes T activés. Ceci corrobore l'interaction entre ces 2 protéines décrite en parallèle par une autre équipe. Nous avons montré que les spectres cliniques des déficits en LRBA et CTLA-4, fortement chevauchant dans les premières descriptions publiées, pourraient se différencier, malgré l'implication des lymphocytes T régulateurs dans ces 2 maladies. (...) / Evans syndrome is defined by the occurence of autoimmune cytopenias, either at the same time or sequential, mainly autoimmune hemolytic anemia and immune thrombocytopenia. In children, it may be secondary to infections, systemic autoimmune disease, or primary immune deficiency, though in most patients, its etiology isn't obvious. Patients affected with Evans syndrome can also present other features, such as autoimmunity toward a particular organ, benign lymphoproliferation or immunodeficiency. The main goal of this work was to identify genetic causes in children presenting an Evans syndrome without a known underlying etiology. We focused our study on severe, early onset forms of the disease, with the hypothesis that a monogenic disease would be more frequent in this group of patients. Taking advantage of high throughput "Next Generation" sequencing (NGS) techniques, we sequenced and analyzed exome from patients and their relatives in search for adequate candidate genes. We identified 4 candidate genes: LRBA, CTLA-4, STAT3 (gain-of-function mutations), and NFKBA. Implication of the first 3 genes in new monogenic diseases with autoimmunity as a key feature was also confirmed by others during the course of this work. For each gene, we pursued 2 complementary goals: First, we sought to validate the implication of the gene in the patients' disease. To do so, we used various techniques and approaches: biochemistry and proteomics to identify protein partners, confocal microscopy to localize proteins and interactions, in vitro cellular assays to bring to light functional defect, flow cytometry to identify changes in lymphocytes subpopulations. We also looked for other mutations of each gene in patients with a similar clinical presentation. Hence we created and explored 3 cohorts of patients presenting with mutations of LRBA, CTLA-4 or STAT3. We constituted a cohort of 18 patients with LRBA mutations within 11 families. We then were able to precise and extend the clinical spectrum of this recently described disease. In particular, we observed patients with severe chronic arthritis associated with diabetes mellitus or enteropathies. We identified 15 new mutations of autosomal recessive transmission in the LRBA gene, coding a protein of unknown function, which absence is responsible for a disease mainly characterized by autoimmune features. We identified 29 candidate protein partners of LRBA and precized LRBA localisation in cell compartiments. We also established a cohort of 12 patients within 10 families presenting CTLA-4 haploinsufficiency. Beyond describing 9 new mutations, we report a family with autosomal recessive transmission.In LRBA and CTLA-4 deficiencies, we showed a decrease of regulatory T lymphocyte subset proportion among PBMC and a decrease of CTLA-4 expression in activated T cells. These results support the interaction between these 2 proteins, described concurrently by another team. We showed that the clinical spectra of these 2 diseases, although widely overlapping in first published reports, could be different despite a role of regulatory T cells in both. Hence, organ-specific autoimmunity and lymphoproliferation are more frequent in LRBA deficiency whereas granuloma and hypogammaglobulinemia are more present in CTLA-4 deficiency. Theses results suggests a role of genetic modifyers, which remain to identify. Among our cohort of patients with Evans syndrome, we also identified 5 patients within 5 families presenting gain-of-function mutations of STAT3. 3 of those mutations were reported by others during our work and appeared de novo in our patients. Functional validation of the 4th one is in progress. The last mutation follows a recessive transmission and could exemplify a new transmission modality of this disease. (...)

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