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Manifestações bucais em pacientes com hipogamaglobulinemia / Oral manifestations in patients with hypogammaglobulinemiaFernandes, Karin Sá 01 July 2010 (has links)
A hipogamaglobulinemia é uma alteração da imunidade humoral caracterizada por baixos níveis séricos de anticorpos podendo ter causas primárias e secundárias. Estes pacientes apresentam uma susceptibilidade a infecções bacterianas de repetição ou crônicas, principalmente do trato respiratório. Além disso, há alta prevalência de doenças gastrointestinais infecciosas e inflamatórias, hepatite C, doenças auto-imunes, doenças linfoproliferativas e granulomatosas. Ainda que a doença seja conhecida desde 1954 há poucos trabalhos na literatura sobre manifestações bucais nestes pacientes. Alguns estudos sugerem uma maior prevalência de lesões liquenóides, doença periodontal, candidíase pseudomembranosa, úlcera aftosa recorrente e hipoplasia de esmalte. Desta forma, o objetivo deste trabalho foi avaliar a prevalência das manifestações e alterações bucais, e caracterizar a saúde bucal de pacientes com hipogamaglobulinemias e correlacioná-las com o estado imunológico do paciente, comparativamente a um grupo de pacientes saudáveis. Para tanto avaliamos 100 pacientes com hipogamaglobulinemias atendidos no Ambulatório de Imunologia e Alergia do Hospital das Clínicas da Faculdade de Medicina da Universidade de São Paulo e 93 pacientes normorreativos da Clínica Odontológica da Faculdade de Odontologia da Universidade de São Paulo, sendo realizado exame clínico bucal, anamnese e compilação de exames laboratoriais recentes. Do total de pacientes com hipogamaglobulinemias, 59 pacientes apresentaram alguma alteração bucal, sendo as mais frequentes lesões de cárie (21), hipoplasia de esmalte (21), gengivite (18), periodontite (8), boca seca (6), língua geográfica (5) e úlcera aftosa recorrente (2). Vinte e sete pacientes apresentaram queixas de úlcera aftosa recorrente com frequência. Dos 93 pacientes do grupo controle, 84 (90,3%) apresentaram alguma alteração bucal, sendo as mais frequentes lesões de cárie (66), gengivite (31), periodontite (44) e candidíase (3). Dezoito pacientes apresentaram queixas de úlcera aftosa recorrente com freqüência. Concluímos que os pacientes com hipogamaglobulinemias, apesar de apresentarem diminuição das imunoglobulinas do sangue, e alguns pacientes apresentarem uma diminuição de células da imunidade celular, não se encontrou relação positiva entre a incidência de cárie e IgA, doença periodontal e IgA e doença periodontal e CD4. / The hypogammaglobulinemia is an alteration in humoral immunity characterized by low levels of antibodies may have primary and secondary causes. These patients have a susceptibility to recurrent bacterial infections or chronic diseases, mainly respiratory tract. Moreover, there is a high prevalence of infectious and inflammatory gastrointestinal diseases, hepatitis C, autoimmune diseases, lymphoproliferative diseases and granulomatous disease. Although the disease is known since 1954 there are few available studies on oral manifestations in these patients. Some studies suggest a higher prevalence of lichenoid lesions, periodontal disease, pseudomembranous candidiasis, recurrent aphthous ulcer and enamel hypoplasia. Thus, the objective was to assess the prevalence of manifestations diseases and to characterize the oral health of patients with hypogammaglobulinemia and correlate with the immune status, compared with healthy patients. For that evaluated 100 patients with hypogammaglobulinemia in the Outpatient Immunology and Allergy Hospital of the Faculty of Medicine, University of São Paulo and 93 healthy patients of School of Dentistry, University of São Paulo, and was conducted oral clinical examination, medical history and compilation of recent laboratory tests. Of all patients with hypogammaglobulinemia, 59 patients showed abnormalities of the mouth, with 21 patients exhibited caries, 21 enamel hypoplasia, 18 gingivitis, 8 periodontitis, 6 dry mouth, 5 geographic tongue and 2 recurrent aphthous ulcer. Twenty-seven patients complained of frequent recurrent aphthous ulcer. Of the 93 control group patients, 84 (90.3%) showed abnormalities, being the most frequent caries (66), gingivitis (31), periodontitis (44) and candidiasis (3). Eighteen patients complained of recurrent aphthous ulcers frequently. We conclude that patients with hypogammaglobulinemia, despite showing decreased blood immunoglobulins, and some patients had a decrease of cells in cellular immunity, we did not find a positive relationship between the incidence of caries and IgA, IgA and periodontal disease and periodontal disease and CD4.
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Deficiências concomitantes da proteína reguladora Fator H e do componente C9 do complemento. / Concomitant deficiences of complement factor H regulatory protein and C9 component.Falcão, Dayseanne Araujo 28 June 2007 (has links)
O paciente, um menino brasileiro de família japonesa e pais consagüíneos, é portador de deficiência concomitante de C9 (C9D) e Fator (F) H. Detectamos níveis reduzidos de FH (16,8µg/mL), C3 e FB no seu soro. O Western Blot confirmou a ausência da proteína de 150 kDa (FH). Sua mãe também apresentou níveis reduzidos de FH (140,5µg/mL), C3 e FB, enquanto o pai e a irmã apresentaram níveis reduzidos de FH. C9 também estava reduzido no soro do paciente (5,6µg/mL). O seqüenciamento do cDNA de FH do paciente revelou a presença de uma substituição homozigota G453A, codificando uma His127Arg. Esta substituição é também homozigota na mãe e provavelmente altera a estrutura terciária do FH e/ou seu perfil de secreção, uma vez que o FH é produzido pelos fibroblastos do paciente. O seqüenciamento de fragmentos do DNA genômico de C9 do paciente revelou a ausência da mutação Arg95, principal causa de C9D entre japoneses. O paciente é portador de uma mutação missense que possivelmente impede a secreção de FH, contudo, não pudemos identificar mutações envolvidas na C9D do paciente. / Our proband, Brazilian from a family of Japanese descent and history of consanguinity, carries C9 (C9D) and FH deficiencies. He was referred with severe recurrent pneumonia. FH (16,8 µg/mL), C3 and FB were present in the patient at low levels. Western blot assays confirmed the complete absence of 150 kDa (FH). His mother also had FH (140,5 µg/mL), C3 and FB low levels, while his father and sister presented only FH low levels. C9 was present in low levels (5,6 µg/mL) and only a very faint ~70 kDa band (expected size) was detected. Sequencing of proband?s FH cDNA revealed a homozygous G453A substitution, encoding a His127Arg. This substitution is also homozygous in the mother and may alter FH protein tertiary structure and/or its secretion profile, as we detected FH production in patient?s fibroblast. Sequencing of proband?s C9 genomic DNA fragments revealed the absence of Arg95 mutation, main cause of C9D in other C9D Japanese patients. The proband carries a missense mutation that may impair the FH secretion, but we couldn?t identify mutations explaining its C9D.
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Manifestações bucais em pacientes com hipogamaglobulinemia / Oral manifestations in patients with hypogammaglobulinemiaKarin Sá Fernandes 01 July 2010 (has links)
A hipogamaglobulinemia é uma alteração da imunidade humoral caracterizada por baixos níveis séricos de anticorpos podendo ter causas primárias e secundárias. Estes pacientes apresentam uma susceptibilidade a infecções bacterianas de repetição ou crônicas, principalmente do trato respiratório. Além disso, há alta prevalência de doenças gastrointestinais infecciosas e inflamatórias, hepatite C, doenças auto-imunes, doenças linfoproliferativas e granulomatosas. Ainda que a doença seja conhecida desde 1954 há poucos trabalhos na literatura sobre manifestações bucais nestes pacientes. Alguns estudos sugerem uma maior prevalência de lesões liquenóides, doença periodontal, candidíase pseudomembranosa, úlcera aftosa recorrente e hipoplasia de esmalte. Desta forma, o objetivo deste trabalho foi avaliar a prevalência das manifestações e alterações bucais, e caracterizar a saúde bucal de pacientes com hipogamaglobulinemias e correlacioná-las com o estado imunológico do paciente, comparativamente a um grupo de pacientes saudáveis. Para tanto avaliamos 100 pacientes com hipogamaglobulinemias atendidos no Ambulatório de Imunologia e Alergia do Hospital das Clínicas da Faculdade de Medicina da Universidade de São Paulo e 93 pacientes normorreativos da Clínica Odontológica da Faculdade de Odontologia da Universidade de São Paulo, sendo realizado exame clínico bucal, anamnese e compilação de exames laboratoriais recentes. Do total de pacientes com hipogamaglobulinemias, 59 pacientes apresentaram alguma alteração bucal, sendo as mais frequentes lesões de cárie (21), hipoplasia de esmalte (21), gengivite (18), periodontite (8), boca seca (6), língua geográfica (5) e úlcera aftosa recorrente (2). Vinte e sete pacientes apresentaram queixas de úlcera aftosa recorrente com frequência. Dos 93 pacientes do grupo controle, 84 (90,3%) apresentaram alguma alteração bucal, sendo as mais frequentes lesões de cárie (66), gengivite (31), periodontite (44) e candidíase (3). Dezoito pacientes apresentaram queixas de úlcera aftosa recorrente com freqüência. Concluímos que os pacientes com hipogamaglobulinemias, apesar de apresentarem diminuição das imunoglobulinas do sangue, e alguns pacientes apresentarem uma diminuição de células da imunidade celular, não se encontrou relação positiva entre a incidência de cárie e IgA, doença periodontal e IgA e doença periodontal e CD4. / The hypogammaglobulinemia is an alteration in humoral immunity characterized by low levels of antibodies may have primary and secondary causes. These patients have a susceptibility to recurrent bacterial infections or chronic diseases, mainly respiratory tract. Moreover, there is a high prevalence of infectious and inflammatory gastrointestinal diseases, hepatitis C, autoimmune diseases, lymphoproliferative diseases and granulomatous disease. Although the disease is known since 1954 there are few available studies on oral manifestations in these patients. Some studies suggest a higher prevalence of lichenoid lesions, periodontal disease, pseudomembranous candidiasis, recurrent aphthous ulcer and enamel hypoplasia. Thus, the objective was to assess the prevalence of manifestations diseases and to characterize the oral health of patients with hypogammaglobulinemia and correlate with the immune status, compared with healthy patients. For that evaluated 100 patients with hypogammaglobulinemia in the Outpatient Immunology and Allergy Hospital of the Faculty of Medicine, University of São Paulo and 93 healthy patients of School of Dentistry, University of São Paulo, and was conducted oral clinical examination, medical history and compilation of recent laboratory tests. Of all patients with hypogammaglobulinemia, 59 patients showed abnormalities of the mouth, with 21 patients exhibited caries, 21 enamel hypoplasia, 18 gingivitis, 8 periodontitis, 6 dry mouth, 5 geographic tongue and 2 recurrent aphthous ulcer. Twenty-seven patients complained of frequent recurrent aphthous ulcer. Of the 93 control group patients, 84 (90.3%) showed abnormalities, being the most frequent caries (66), gingivitis (31), periodontitis (44) and candidiasis (3). Eighteen patients complained of recurrent aphthous ulcers frequently. We conclude that patients with hypogammaglobulinemia, despite showing decreased blood immunoglobulins, and some patients had a decrease of cells in cellular immunity, we did not find a positive relationship between the incidence of caries and IgA, IgA and periodontal disease and periodontal disease and CD4.
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Déterminants de l'état de santé et de la qualité de vie des patients atteints de déficits immunitaires primitifs diagnostiqués au cours de leur enfance / Health status and quality of life of patients with primary immunodeficiencies diagnosed during childhoodBarlogis, Vincent 05 September 2017 (has links)
Justification de l’étude. Les déficits immunitaires primitifs (DIP) sont caractérisés par une grande hétérogénéité clinique, biologique, génétique et thérapeutique. Très peu de connaissances sont disponibles quant au devenir à long terme des patients en termes d’état de santé et de qualité de vie. Objectif : L'objectif principal de l’étude est de mettre en place un dispositif capable d’étudier les déterminants du devenir à long terme d’une cohorte de patients présentant un diagnostic de DIP diagnostiqué au cours de leur enfance. Résultats. Au 1er juin 2016, 1014 patients ont été inclus dans la cohorte sur les 1800 interrogés. La cohorte adulte montre que l’état de santé est marqué par la prévalence très élevée d’évènements de santé sévère ou très sévères (touchant 87% des adultes), avec un taux de cancer de 7.6%. Comparé aux normes françaises, tous les domaines de qualité de vie sont significativement altérés. Seuls les patients greffés présentent une qualité de vie meilleure par rapport aux patients non greffés. Nous montrons que la QoL est inversement proportionnelle à la survenue de complications sévères. L’étude pédiatrique fait le même constat, démontrant que c’est très tôt pendant l’enfance que surviennent les complications sévères dont l’impact sur leur qualité de vie est majeur. Conclusion : les patients atteints de DIP présentent un état de santé marqué par une fréquence très élevée d’évènements de santé de haut grade, et ceci très précocement dans l’enfance. La lourdeur de leur état de santé est le déterminant principal de la mauvaise qualité de vie des patients, justifiant d’une prise en charge spécialisée et multidisciplinaires dès le diagnostic posé. / Importance: Most children with primary immunodeficiencies (PID) now reach adulthood. Assessment of their long-term health status represents a major challenge. We aimed to gain insight into how PID affects patient health status and quality of life (QoL). Design: The French Reference Center for PIDs (CEREDIH) initiated a prospective multicenter cohort which enrolled participants who met all inclusion criteria: (1) patient with PID included in the CEREDIH registry, (2) clinical diagnosis before 18 years, (3) alive and living in France. Among 1810 patients eligible for inclusion (on 1/17/2016), 1047 were children, and 763 were adults. A severity score was assigned to each health condition: grade 1 (mild) to grade 4 (life-threatening/disabling). We report the health status of children by focusing on two endpoints: grade 4 conditions and grade 3 or 4 conditions. Results: In the adult study, only 12% of adults with PID had never experienced severe or life-threatening conditions, and 7.6% of patients had been diagnosed with cancer. Furthermore, adults reported significantly lower scores for all domains of QoL, and QoL was strongly associated with poor health conditions. In the pediatric study, the response rate was 62.5%. Of the 656 children participants, 83% experienced at least one grade 3 or 4 condition. Children with PID scored significantly lower for most QoL domains. QoL was strongly associated with heavy burden of health conditions. Conclusions: Taken together, these studies demonstrate that the deleterious health effects bore by patients with PID become heavy since childhood, emphasizing the need to establish multidisciplinary healthcare teams, from childhood.
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Deficiências concomitantes da proteína reguladora Fator H e do componente C9 do complemento. / Concomitant deficiences of complement factor H regulatory protein and C9 component.Dayseanne Araujo Falcão 28 June 2007 (has links)
O paciente, um menino brasileiro de família japonesa e pais consagüíneos, é portador de deficiência concomitante de C9 (C9D) e Fator (F) H. Detectamos níveis reduzidos de FH (16,8µg/mL), C3 e FB no seu soro. O Western Blot confirmou a ausência da proteína de 150 kDa (FH). Sua mãe também apresentou níveis reduzidos de FH (140,5µg/mL), C3 e FB, enquanto o pai e a irmã apresentaram níveis reduzidos de FH. C9 também estava reduzido no soro do paciente (5,6µg/mL). O seqüenciamento do cDNA de FH do paciente revelou a presença de uma substituição homozigota G453A, codificando uma His127Arg. Esta substituição é também homozigota na mãe e provavelmente altera a estrutura terciária do FH e/ou seu perfil de secreção, uma vez que o FH é produzido pelos fibroblastos do paciente. O seqüenciamento de fragmentos do DNA genômico de C9 do paciente revelou a ausência da mutação Arg95, principal causa de C9D entre japoneses. O paciente é portador de uma mutação missense que possivelmente impede a secreção de FH, contudo, não pudemos identificar mutações envolvidas na C9D do paciente. / Our proband, Brazilian from a family of Japanese descent and history of consanguinity, carries C9 (C9D) and FH deficiencies. He was referred with severe recurrent pneumonia. FH (16,8 µg/mL), C3 and FB were present in the patient at low levels. Western blot assays confirmed the complete absence of 150 kDa (FH). His mother also had FH (140,5 µg/mL), C3 and FB low levels, while his father and sister presented only FH low levels. C9 was present in low levels (5,6 µg/mL) and only a very faint ~70 kDa band (expected size) was detected. Sequencing of proband?s FH cDNA revealed a homozygous G453A substitution, encoding a His127Arg. This substitution is also homozygous in the mother and may alter FH protein tertiary structure and/or its secretion profile, as we detected FH production in patient?s fibroblast. Sequencing of proband?s C9 genomic DNA fragments revealed the absence of Arg95 mutation, main cause of C9D in other C9D Japanese patients. The proband carries a missense mutation that may impair the FH secretion, but we couldn?t identify mutations explaining its C9D.
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Estudo genetico-molecular da doença granulomatosa cronicaAgudelo Flórez, Piedad Matilde 08 April 2004 (has links)
Orientador: Antonio Condino Neto / Tese (doutorado) - Universidade Estadual de Campinas, Faculdade de Ciencias Medicas / Made available in DSpace on 2018-08-04T01:07:19Z (GMT). No. of bitstreams: 1
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Previous issue date: 2004 / Resumo: Doença Granulomatosa. Crônica (DOC) é uma imunodeficiência caracterizada por infecções recorrentes graves. Os defeitos moleculares que lavam a DGC são geralmente devidos a mau funcionamento, ausência o baixa expressão de um dos componentes do sistema NADPH oxidase. Este trabalho analisou o uso de RT-PCR para a triagem de defeitos moleculares responsáveis por DGC ligada ao X em 8 pacientes. RNA total foi preparado de linfócitos B transformados com vírus de Epstein-Barr e transcrição reversa com hexâmeros randomicos. O cDNA resultante foi amplificado por PCR com oligonucleotídeos específicos para 3 regiões exônicas abrangendo toda a extensão do gene. Com esta estratégia foi possível a detecção da expressão defeituosa de gp91-phox em 7 pacientes. Concluímos que a análise por meio de RT-PCR, um método alternativo menos complexo, rápido e econômico foi apropriado para detecção inicial de defeitos moleculares em 7 de 8 pacientes com DOC ligada ao X. Posteriormente investigamos em detalhe os defeitos genetico-moleculares de 7 crianças não relacionadas com DGC ligada ao X. Todos os pacientes foram procedentes do Chile e Brasil. Encontramos uma inserção c.1267_1268insA no paciente JY no exon 10 levando a uma mutação tipo "&ameshill:". Esta mutação é um novo registro na literatura. Detectamos duas substituições "nonsense", uma no paciente PT, c.95 G>A no exon 2 que leva a um códon de parada W28X e outra no paciente MF, c.229 C>T no exon 3 que leva a um códon de parada R73X. Em 4 casos, nos pacientes IC, Vin, RS, GO, diferentes erros de "splicing" foram encontrados. Dois pacientes apresentaram uma subtitução c.264 G> A ao final do exon 3. Os dois restantes apresentaram uma subtitução c.1326 + 1 G>A no intron 10 e outra subtitução c.1164 - 2 A>O no intron 9. Esta última mutação também é um novo registro na lit_ratura. As mutações identificadas na proteína gp91-phox confirmam um alto grau de heterogeneidade molecular como é relatado em outros grupos étnicos e a importância de investigar os defeitos moleculares em diferentes populações. Contrastando com esta heterogeneidade, a DGC associada com defeitos na proteína p47-phox, apresentam pouca variabilidade. Neste estudo, os pacientes analisados, dois irmãos, mostram uma deleção homozigota OT (L}.GT) no começo do exon 2. L Também é analisado o caso de um paciente com infecções recorrentes que inicaJmente recebeu o diagnóstico de deficiência de G6PD. Estudos moleculares mostraram que a deficiência de G6PD foi devida a uma mutação 202 G_A, variante Afi:icana. . O paciente também mostrou uma reduzida atividade da explosão respiratória como observado em DGC ligada ao X. A análise do gDNA mostrou uma subtitução 264 G_A na região do splicing do exon 3 da proteína gp91-phox. A seqüência do cDNA detectou uma deleção do exon 3, levando a uma mutante inestável ou não funcional da proteina gp91-phox e resultando no fenótipo de DGC ligada ao X. Propomos que ftente a um paciente com deficiência de G6PD com episódios de infecções graves considerem a possibilidade de um defeito na atividade fagocítica e uma eventual associação com DGC / Abstract: Chronic granulomatous disease (CGD) is a rare primary immunodeficiency characterized by ear1y onset recurrent severe infections. The molecular defects causing CGD are generally due to the absence, low expression or malfunctioning of one of the NADPH oxidase components. This work analyzed the potential use of reverse transcription (RT)PCR for screening molecular defects responsible for X-linked CGD in 8 Brazilian patients. Total RNA was prepared from EBV-transformed B-lymphocytes and reverse transcribed using random hexamers. The resultant cDNA was PCR-amplified by specific and overlapping pairs of primers regarding 3 exonic regions of gp91-phox gene. This strategy made possible the detection of defective gp91-phox expression in 7 patients. We conclude that RT -PCR analysis, a less complex, more economic and faster alternative method, was appropriate for screening molecular defects in 7 out 8 X-linked CGD patients. We further investigated the molecular genetic defects in 7 unrelated patients with X-linked CGD, from Chile and Brazil. We found an insertion c.1267_1268insA in exon 10 leading to a frameshift mutation. This mutation is a novel reporto we detected two single base-pair substitutions that lead to nonsense mutations. The first was a c.95 G>A substitution in the exon 2 which predicts a stop codon W28X and the second was a c.229 C> T substitution in the exon 3 which predicts a stop codon R73X. We also identified different splice site mutations in 4 cases. Two patients presented a c.264 G> A substitution at the end of exon 3. The remaining two patients presented either a c.1326 + 1 G>A substitution in intron 10 or a c.1164 - 2 A>G substitution in intron 9. This Iast mutation is also novel. The gp91-phox mutations identified in these patients show a high degree of molecular heterogeneity as reported in other ethnic groups and the importance to investigate molecular genetic defects in diferent populations. Contrasting with the heterogeneity of mutations observed in X-linked CGD, the disease associated with defect in p47-phox shows less variability. In this report, the patients with CGD, two sib1ings, show a homozygotous dinucleotide GT deletion (.6.GT) at the beginning of exon 2. We also reported a child with recurrent infections who initially received the diagnosis of G6PD deficiency. Molecular studies showed that the G6PD deficiency was due a 202 G-+A mutation, the A- variant common in African ethnic groups. The proband also exln'bited severely impaired respiratory burst activity, as observed in X-linked CGD. Sequence analysis of genomic DNA showed a 264 G-+A substitution at the 3' splice junction of gp91-phox exon 3. The cDNA sequence showed a deletion of gp91-phox exon 3, giving rise to an unstable or nonfunctional mutant gp91-phox and to the phenotype of Xlinked CGD. We propose that clinicians in face of a patient with G6PD deficiency under a severe infection episode consider the possibility of temporary or permanent impairment of the phagocytes microbicidal activity, and the eventual association of G6PD deficiencyand chronic granulomatous disease / Doutorado / Saude da Criança e do Adolescente / Doutor em Saude da Criança e do Adolescente
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Modulating hematopoietic progenitor cell engraftment and T cell differentiation : role of conditioning and route of administration / Modulation de la prise de greffe de progéniteurs hématopoiétiques et de la différenciation T : rôle du conditionnement et de la voie d'aministrationCochonneau, Stéphanie 26 October 2012 (has links)
Les déficits lymphocytaires T peuvent être corrigés par l'administration en intraveineuse (IV) de cellules souches hématopoiétiques (CSH) provenant d'un donneur. Dans un modèle d'immunodéficience lié à l'absence de la protéine kinase ZAP-70, notre équipe avait précédemment montré que l'injection intrathymique (IT) de CSH histocompatibles conduit à une reconstitution du compartiment T plus robuste et plus rapide que dans le cas où les CSH sont administrées par voie IV. Au cours de ma thèse, je me suis intéressée à l'approche IT dans un contexte non-histocompatible, où j'ai montré que l'injection de CSH semi-allogéniques directement dans le thymus permet le développement d'une thymopoièse à long-terme, même en absence de conditionnement. De plus, j'ai également montré la persistence de progéniteurs thymiques précoces (ETP) provenant du donneur dans le thymus des souris transplantées. De façon remarquable, ces ETP retiennent un potentiel de différenciation plus divers que ceux rencontrés dans le thymus d'une souris sauvage, et leur fréquence est significativement élévée après IT, ce dernier suggérant une disponibilité accrue des niches thymiques. De façon intéressante, j'ai également montré que les progéniteurs déficients en ZAP-70 pouvaient se différencier de façon importante vers le lignage CD8 lors d'une activation constante de la voie de signalisation Notch couplée à la présence d'interleukine 7 (IL-7). Après la greffe de CSH par voie IV de souris ZAP-70-/-, en absence de conditionnemt, j'ai également identifié l'accumulation d'une population de CSH présentant un phénotype particulier (Lin- Sca 1+ c-kit-), nommée LSAPT. Ces cellules LSAPT présentent un biais de différenciation vers le lignage T γδ ainsi qu'une production élevée d'IL-17, ce qui suggère que les fonctions effectrices d'une cellule T γδ sont dépendantes de leur origine progénitrices. L'ensemble de mes résultats apporte à la fois de nouveaux éléments concernant l'identification de progéniteurs T et démontrent de l'influence/coopération entre voies de signalisation et facteurs environnementaux dans la modulation de la différenciation T et de leur fonctions effectrices. / T cell deficiencies can be corrected by the intravenous (IV) injection of donor hematopoietic stem cells (HSCs). Using a murine model of ZAP-70-/- deficiency, our group previously showed that the intrathymic (IT) administration of histocompatible HSCs leads to a more robust and long-term thymopoiesis as compared to that achieved by the classical IV route. During my PhD, I found that the direct IT administration of semiallogeneic HSCs results in a sustained donor-derived thymopoiesis, overcoming histocompatibility barriers, even in the absence of conditioning. Furthermore, I found that donor-derived early thymic progenitors (ETPs) persist in the thymi of ZAP-70-/- transplanted mice, and present increased multi-lineage potential as compared to wild-type ETPs. Importantly, the frequency of donor-derived ETPs was augmented following IT transplantation, indicative of an increased progenitor niche. Interestingly, ZAP-70-deficient HSC could themselves be driven to a CD8 lineage fate in an environment where IL-7 potentiates continuous activation of the Notch pathway. Following IV transplantation of donor HSC into non-conditioned ZAP-70-/- mice, I determined that there is an accumulation of lineage-/Sca1+ donor progenitors lacking expression of the stem cell marker c-kit, termed LSAPT. These LSAPT show a biased differentiation towards the γδ T cell lineage with high IL-17-producing effector function, suggesting that progenitor origin regulates γδ T cell fate. The ensemble of my experiments provide new insights into the identity of T lineage progenitors and demonstrate how signaling pathways as well as environmental factors modulate T cell differentiation and effector function.
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Estudo de novos defeitos genético-moleculares em pacientes com diagnóstico clínico de imunodeficiência primária. / Study of new molecular genetic defects in patients with clinical diagnosis of primary immunodeficiency.Flores, Stefanie Klaver 10 August 2016 (has links)
As imunodeficiências primárias são um grupo heterogêneo de doenças hereditárias do sistema. Aqui nós descrevemos 4 famílias (2 Turcas e 2 Brasileiras), que apresentaram infecções recorrentes desde os primeiros dias de vida. Após uma análise clínica bem detalhada, combinamos as técnicas de sequenciamento de alta geração para identificar novos defeitos genéticos que levam ao fenótipo de IDP. Finalizamos com a identificação e caracterização de três IDP, sendo que duas inéditas. A primeira identificada (P1) foi causada por uma mutação bialélica no sítio de splice do gene PRKCD (c.1352+1G>A). A segunda (P2 e P3) foi causada por uma mutação bialélica no gene que codifica NIK (c. C1694G; p. Pro565Arg). A terceira (P4) foi causada uma mutação no gene IL7Rα (c.G353A). Finalizamos a análise da P5, mas nenhum dos genes candidatos foi confirmado. A análise genética e a identificação do defeito genético, permite que nossos pacientes possam ter uma melhor sobrevida, podendo realizar um tratamento correto e permite o aconselhamento genético na família. / Primary immunodeficiencies are a heterogeneous group of inherited diseases of the immune system. Here we describe 5 patients from 4 families (2 Turks and 2 Brazilian), all patients had recurrent infections since the firsts days of life. After a very detailed clinical analysis, we applied the Next Generation Sequencing to identify new genes that could be lead to PID phenotype. We finished with the identification and characterization of 3 PID, where 2 of them was new. The first identified (P1) was a biallelic mutation in the splice site of the gene PRKCD (c.1352 + 1G>A). The second (P2 and P3) was a biallelic mutation in the gene encoding NIK (MAP3K14; c.C1694G;. p.Pro565Arg). The third (P4) has a mutation in the gene IL7Rα (c.G353A). We finished the analysis of P5, but no candidate gene was confirmed to be the defect cause. Genetic analysis and identification of the genetic defect allows our patients may have a better survival and can perform a proper treatment and genetic counseling allows the family.
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Reconstitution de l’architecture thymique et de la différenciation des cellules T dans les immunodéficiences génétiques : développement de stratégies thérapeutiques ciblant directement le thymus / Reconstitution of thymus architecture and T cell differentiation in genetic immunodeficiencies : development of therapeutic strategies directly targeting the thymusPouzolles, Marie 14 September 2018 (has links)
Les cellules souches hématopoïétiques (CSH) assurent la génération de toutes les lignées sanguines. Leur différenciation en cellules T matures se déroule dans un microenvironnement spécialisé, le thymus, orchestrée par des interactions complexes entre cytokines, chimiokines et cellules stromales. Les mutations bloquant la différenciation des cellules T ont un impact sur l'architecture du thymus, soulignant l’importance des interactions entre cellules T en développement et cellules stromales thymiques.Les déficits immunitaires combinés sévères sont généralement traités, avec succès, par transplantation de CSH allogénique par voie intraveineuse. Cependant, des complications peuvent survenir notamment en cas de greffe non compatible. Pour pallier à cela, la thérapie génique a été développée mais son efficacité et son innocuité restent à améliorer. Dans ce but, notre groupe a développé une approche par correction génique des progéniteurs T directement in vivo, via un vecteur lentiviral. Bien qu’efficace, là encore, l’efficacité de traitement reste insuffisante voire extrêmement limitée chez les macaques.Lors de ma thèse, j'ai donc évalué le potentiel de différents sérotypes de vecteur viraux adéno-associés (AAV) pour la transduction des thymocytes. L'administration IT de plusieurs sérotypes de AAV2 engendre une transduction des thymocytes >10 fois plus élevée que celle des vecteurs lentiviraux. Le sérotype AAV2/8 induit la transduction des thymocytes la plus efficace et les cellules transduites représentent jusqu'à 1% des cellules T périphériques d’une souris immunocompétente. En utilisant des souris immunodéficientes ZAP-70-/- comme paradigme, j'ai découvert que l'injection IT de l’AAV2/8-ZAP-70 entraîne une transduction et différentiation lymphocytaire T rapide, associée à la génération d’une medulla thymique. En effet, des cellules épithéliales thymiques de la médulla (mTEC) exprimant le régulateur auto-immun AIRE sont détectées en <2 semaines. Bien que cette reconstitution soit transitoire, les mTECs AIRE+ diminuant 10 semaines post-injection, les cellules T périphériques corrigées persistent >40 semaines et présentent environ 1 copie du vecteur AAV/cellule. Ces cellules T effectrices peuvent sécréter des niveaux élevés de cytokines et un nombre important de cellules T régulatrices est également généré. Ainsi, une seule vague de thymopoïèse à partir de progéniteurs transduits par l’AAV-ZAP-70, permet une restauration, rapide et transitoire de l'architecture thymique mais, à long terme de cellules T périphériques fonctionnelles.Pour évaluer les diverses populations de TEC régissant le développement et la sélection des cellules T, j'ai collaboré avec les groupes de P Jay/J Abramson/I Amit pour établir une cartographie de novo du compartiment stromal thymique. Nos analyses ont mis en évidence quatre populations majeures de mTEC (I-IV) avec des fonctions distinctes. Notamment, les mTEC-IV constituent une population unique présentant des similarités moléculaires et morphologiques avec les cellules tuft intestinales. Comme nous avions précédemment identifié la sécrétion d'IL-25 par les cellules tufts comme un régulateur des interactions entre compartiment épithélial et hématopoïétique dans l'intestin, nous avons évalué ce potentiel dans le thymus. Ainsi, des souris déficientes en cellules tuft intestinales présentent également une déficience spécifique en mTEC-IV et une homéostasie perturbée de diverses populations exprimant l'IL-25R dans le thymus. Notre recherche a donc permis d'identifier une nouvelle population de TEC tuft avec un rôle critique dans la formation de la niche immunitaire du thymus.L’ensemble de mes résultats montrent le potentiel thérapeutique de stratégie intrathymique de thérapie génique pour des patients ayant besoin d’une reconstitution rapide en cellules T et fournissent de nouvelles perspectives sur les populations stromales thymique et leur rôle dans l’équilibre de la niche immunitaire. / Hematopoietic stem cells (HSC) ensure the generation of all blood lineages. Their differentiation to mature T lymphocytes occurs in the specialized microenvironment of the thymus, orchestrated by complex interactions between cytokines, chemokines, and stromal cells. Mutations resulting in a block in T cell differentiation impact on the architecture of the thymus, pointing to the critical crosstalk between developing T cells and thymic stromal components.Genetic severe combined immunodeficiencies (SCID) are generally treated by the intravenous transplantation of healthy allogeneic HSCs. Although this therapy is often successful, complications can occur, especially for patients receiving non-histocompatible HSC transplants. To circumvent these problems , significant efforts have gone into developing gene therapy strategies but adverse events indicate the necessity of exploring other avenues. Our group hypothesized that in situ gene correction of T lymphoid progenitors in the thymus itself may overcome some of the drawbacks of ex vivo gene therapy. While intrathymic (IT) lentiviral vector administration corrected immunodeficient thymocyte precursors in mice, thymus transduction was inefficient and efficacy in macaques was limited.During my PhD, I assessed the in vivo potential of adeno-associated vectors (AAV) to transduce thymocyte precursors. Intrathymic administration of several different scAAV2 serotypes resulted in a >10-fold higher transduction of thymocytes (3-5%) as compared to lentiviral vectors. scAAV2/8 promoted the highest level of gene transfer and strikingly, transduced cells represented up to 1% of peripheral T lymphocytes in immunocompetent mice. Using ZAP-70-/- immunodeficient mice as a paradigm, I found that IT injection of an AAV2/8-ZAP-70 vector resulted in a rapid transduction and T cell differentiation, correlating with a dramatic generation of the thymus medulla. Indeed, medullary thymic epithelial cells (mTEC) expressing the AIRE autoimmune regulator were detected within <2 weeks. While this reconstitution was transient––AIRE+ mTECs decreased by 10 weeks post gene transfer––gene-corrected peripheral T cells, harboring approximately 1 AAV genome/ cell, persisted for >40 weeks. Effector T cells had the potential to secrete high levels of cytokines and significant numbers of gene-corrected regulatory T cells were also generated. Thus, a single wave of thymopoiesis, from intrathymic AAV-ZAP-70-transduced progenitors, allows for a rapid but transient restoration of the thymic architecture and long-term peripheral T cell function.To better assess the diverse TEC populations that orchestrate T cell development and selection, I collaborated with the groups of P. Jay/J. Abramson/I. Amit to combine single cell analysis and in-vivo fate-mapping to de novo characterize the entire stromal compartment of the thymus. Our analyses highlighted four major medullary TEC (mTEC I-IV) populations with distinct lineage regulator function and specifically, we found that mTEC-IV constitutes a highly divergent TEC subset that bears strong molecular and morphological characteristics to intestinal tuft cells. As we previously identified tuft cell secretion of IL-25 as a regulator of the crosstalk between the epithelial and hematopoietic compartments in the gut, we assessed the potential immune-modulatory function of mTEC-IV. Notably, mice deficient in intestinal tuft cells exhibited a specific depletion of mTEC-IV and a perturbed homeostasis of various IL25-R-expressing populations in the thymus. Taken together, our data identify a new tuft TEC population critical for shaping the thymus immune niche.In conclusion, the data generated during my PhD advance the therapeutic potential of intrathymic-based vector strategies for the treatment of patients requiring a rapid T cell reconstitution and provide new insights into thymic stromal subsets that are critical for shaping the thymus immune niche.
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Estudo de novos defeitos genético-moleculares em pacientes com diagnóstico clínico de imunodeficiência primária. / Study of new molecular genetic defects in patients with clinical diagnosis of primary immunodeficiency.Stefanie Klaver Flores 10 August 2016 (has links)
As imunodeficiências primárias são um grupo heterogêneo de doenças hereditárias do sistema. Aqui nós descrevemos 4 famílias (2 Turcas e 2 Brasileiras), que apresentaram infecções recorrentes desde os primeiros dias de vida. Após uma análise clínica bem detalhada, combinamos as técnicas de sequenciamento de alta geração para identificar novos defeitos genéticos que levam ao fenótipo de IDP. Finalizamos com a identificação e caracterização de três IDP, sendo que duas inéditas. A primeira identificada (P1) foi causada por uma mutação bialélica no sítio de splice do gene PRKCD (c.1352+1G>A). A segunda (P2 e P3) foi causada por uma mutação bialélica no gene que codifica NIK (c. C1694G; p. Pro565Arg). A terceira (P4) foi causada uma mutação no gene IL7Rα (c.G353A). Finalizamos a análise da P5, mas nenhum dos genes candidatos foi confirmado. A análise genética e a identificação do defeito genético, permite que nossos pacientes possam ter uma melhor sobrevida, podendo realizar um tratamento correto e permite o aconselhamento genético na família. / Primary immunodeficiencies are a heterogeneous group of inherited diseases of the immune system. Here we describe 5 patients from 4 families (2 Turks and 2 Brazilian), all patients had recurrent infections since the firsts days of life. After a very detailed clinical analysis, we applied the Next Generation Sequencing to identify new genes that could be lead to PID phenotype. We finished with the identification and characterization of 3 PID, where 2 of them was new. The first identified (P1) was a biallelic mutation in the splice site of the gene PRKCD (c.1352 + 1G>A). The second (P2 and P3) was a biallelic mutation in the gene encoding NIK (MAP3K14; c.C1694G;. p.Pro565Arg). The third (P4) has a mutation in the gene IL7Rα (c.G353A). We finished the analysis of P5, but no candidate gene was confirmed to be the defect cause. Genetic analysis and identification of the genetic defect allows our patients may have a better survival and can perform a proper treatment and genetic counseling allows the family.
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