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Les cellules dendritiques plasmacytoides dans le sang de cordon et après greffe de sang de cordonCharrier, Emily 08 1900 (has links)
La greffe de sang de cordon est de plus en plus utilisée et a permis de traiter avec succès chez l’enfant des déficits immunitaires ainsi que des hémopathies malignes comme les leucémies. Malgré d’importants avantages tels que l’absence de risque pour le donneur ou la plus faible incidence de maladie du greffon contre l’hôte (GvHD), utiliser le sang de cordon comporte certains inconvénients. En effet, une reconstitution immunitaire retardée, des infections opportunistes en plus grand nombre et un risque de rechute sont des complications qui peuvent survenir et engendrer un risque pour le pronostic vital du patient. Par conséquent, de nouvelles stratégies d’immunothérapies doivent être envisagées.
Dans le cadre de ce travail, nous nous sommes particulièrement intéressés aux cellules dendritiques plasmacytoides (pDC) dont les fonctions sont importantes pour l’initiation des réponses immunitaires innée et adaptative et particulièrement pour leur capacité à activer les cellules NK. Afin d’élucider le rôle et l’impact de ces cellules dans les greffes de sang de cordon, le nombre et la fonction des pDC et des NK a été suivi longitudinalement chez des patients ayant subi une greffe de sang de cordon comparativement à des patients transplantés avec de la moelle osseuse. Nous avons ainsi démontré que les pDC et les NK apparaissent précocement suite à une greffe de sang de cordon et que ces cellules sont fonctionnelles. Ces résultats mettent donc en lumière que ces cellules pourraient être de bons outils pour l’établissement d’une immunothérapie après greffe de sang de cordon.
De plus, la caractérisation fonctionnelle des pDC du greffon de sang de cordon a permis de révéler une plus faible production d’IFN-α par les pDC, comparativement aux pDC de sang d’adulte. Cette différence pourrait jouer un rôle dans la plus faible incidence de GvHD après les greffes de sang de cordon. Dans le but de préciser les mécanismes moléculaires de régulation négative de la production d’IFN-α par les pDC de sang de cordon, nous avons étudié les protéines de la voie de signalisation TLR9-IRF7. L’expression similaire de l’ARN du TLR9, MyD88, IRAK1 et IRF7 contraste avec la plus faible expression des protéines correspondantes. De plus, l’expression des MicroARNs miR-146a et miR-155 est plus élevé dans les pDC de sang de cordon comparativement aux pDC de sang d’adultes. Ensemble, ces données pointent une régulation négative post-transcriptionnelle de la voie TLR9-IRF7 qui pourrait expliquer la plus faible production d’IFN-α des pDC du sang de cordon.
L’ensemble des ces travaux suggère que les pDC pourraient représenter une cible de choix dans le développement de nouvelles approches thérapeutiques dans les greffes de sang de cordon. / Umbilical cord blood transplantation has increasingly been used as a source of hematopoietic stem cells to successfully treat immunodeficiencies and malignant diseases such as leukemia in pediatric patients. Despite important advantages, namely lack of risk for the donor and low incidence of GvHD, use of cord blood is associated with several drawbacks. Specifically, delayed immune reconstitution, more opportunistic infections and a relative risk of relapse are complications that may occur and lead to a poor prognosis. Consequently, new immunotherapeutic strategies should be considered.
In this study, we were interested in plasmacytoid dendritic cells (pDC), whose functions are important for initiation of innate and adaptive immune responses and, in particular, for their ability to activate natural killer cells (NK). In order to elucidate the role and the impact of these cells in cord blood transplantation, pDC and NK numbers and function have been longitudinally followed in cord blood and bone marrow recipients. We showed that pDC and NK cells appeared early after umbilical cord blood transplantation and that these cells retained functional activity. Thus, these cells may constitute a good tool for immunotherapy in umbilical cord blood transplantation.
Moreover, the functional characterization of pDC in cord blood revealed a lower production of IFN-α by cord blood pDC, which may play a role in the lower incidence of GvHD after umbilical cord blood transplantations. In order to determine the molecular mechanism for the negative regulation of IFN-α production by cord blood pDC, we studied the expression of TLR9-IRF7 pathway. The stable expression of TLR9, MyD88, IRAK1 and IRF7 mRNA contrasts with the lower expression of corresponding proteins. Interestingly, expression of microRNA miR-146a and miR-155 is higher in cord blood pDC. Together, these results point to a post-transcriptionnal negative regulation of TLR9-IRF7 pathway which may explain the lower IFN-α production by cord blood pDC.
This work reinforces the idea that pDCs constitute a target of choice for developing new therapeutic approaches in cord blood transplantations.
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Protocolo para avaliação e terapia nutricional no transplante de células hematopoiéticas em pacientes do Hospital das Clínicas de Botucatu / Evaluation and nutritional therapy protocol for patients in hematopoietic stem cell transplantation program in Hospital das Clínicas de BotucatuCosta, Cesar Martins da 02 May 2018 (has links)
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Previous issue date: 2018-05-02 / O Transplante de Células Progenitoras Hematopoiéticas (TCPH) é um método terapêutico utilizado no tratamento de diversas doenças que envolvem o tecido linfo-hematopoiético, doenças autoimunes e condições não-malignas. As evidências apontam que o reconhecimento precoce de pacientes em grupos de risco nutricional no TCPH e a elaboração de um plano terapêutico para tal tem impacto positivo na redução da mortalidade. A monitorização diária das necessidades energéticas, proteicas e de nutrientes é um dos pontos cruciais da terapia, pois o paciente que é incapaz de suprir mais do que 60% das necessidades nutricionais diárias por via oral torna-se candidato a outras modalidades de terapia (enteral ou parenteral), a depender da viabilidade do trato gastrointestinal, das contra-indicações relativas a cada método (plaquetopenia na introdução de sonda nasoenteral, por exemplo) e das complicações associadas aos procedimentos (aumento das taxas de infecção de corrente sanguínea na nutrição parenteral). Se o paciente atingir mais do que 60% das necessidades nutricionais por via oral e mantiver esse aporte por pelo menos 3 dias, o suporte por nutrição enteral ou parenteral pode ser descontinuado. A literatura científica ainda não elucidou todos os questionamentos quanto à melhor abordagem nutricional em pacientes submetidos a TCPH, podendo-se observar grande variação entre as condutas orientadas pelas diretrizes internacionais mais recentes e o que se adota como prática clínica diária, chamando atenção para a necessidade da elaboração de protocolos nutricionais que diminuam essas divergências. Objetivos: elaboração de um manual de avaliação do risco nutricional e de implementação de terapia nutricional para pacientes que serão submetidos ao Transplante de Células Progenitoras Hematopoiéticas no Hospital das Clínicas de Botucatu, facilitando a tomada de decisões de acordo com as evidências científicas mais recentes e contribuindo para minimizar as divergências de condutas através de um protocolo nutricional hospitalar. Casuística e Métodos: o manual foi elaborado por meio de uma revisão narrativa da literatura científica, utilizando-se de artigos e diretrizes relevantes contidos nas bases de dados Pubmed, Lilacs e Scielo, assim como de livros textos e de consensos desde o ano 2000 até 2017. Para a busca, os termos utilizados foram “nutrition assessment", "nutrition therapy", "nutrition risk", “undernutrition”, "malnutrition", “obesity”, "chemotherapy", “blood 8 marrow transplantation”, “haematopoietic stem cell transplantation”, “body composition”, “phase angle”. Resultados: há escassez de estudos específicos relacionados a terapia nutricional e a TCPH. A busca resultou na utilização de 20 trabalhos científicos que embasam a produção desta dissertação. Considerando a estrutura e a dinâmica do Hospital das Clínicas de Botucatu, a padronização de condutas deste Manual levou à elaboração de um protocolo em forma de fluxograma que abrange a avaliação do Risco Nutricional e de aplicação da Terapia Nutricional em pacientes submetidos ao TCPH neste serviço de saúde. Conclusão: o protocolo de avaliação de Risco e de aplicação de Terapia Nutricional, redigido em forma de fluxograma, facilita a aplicabilidade do conteúdo do Manual para os profissionais que dele se utilizarão, simplifica a classificação dos grupos de risco nutricional, disponibiliza elaboração rápida de condutas e evita divergências de prescrição quanto à melhor Terapia Nutricional em pacientes submetidos ao TCPH. / Hematopoietic Stem Cell Transplantation (HSCT) is a therapeutic method used for treatment of various diseases involving lymphohematopoietic tissue, autoimmune diseases and non-malignant conditions. Evidence indicates that the early recognition of nutritional risk in HSCT patients and the elaboration of a therapeutic plan for them has a positive impact in reducing mortality. Monitoring daily needs of energy, protein and nutrient is one of the crucial points of therapy, because individuals who are unable to supply more than 60% of the daily nutritional needs orally become candidates for other modalities of therapy (enteral or parenteral), depending on the viability of the gastrointestinal tract, contraindications for each method (thrombocytopenia in the introduction of nasoenteral probe, for example) and complications associated with procedures (increased bloodstream infection rates in parenteral nutrition) . If the patient reaches more than 60% of nutritional needs orally and maintains this intake for at least 3 days, enteral or parenteral nutrition support may be discontinued. The scientific literature has not yet elucidated all the questions regarding the best nutritional approach in patients undergoing HSCT and a great variation between the conducts guided by the most recent international guidelines and what is adopted as daily clinical practice can be observed, drawing attention to the need for nutritional protocols that could reduce these divergences. Objectives: elaboration of a manual of nutritional therapy and nutritional risk assessment for patients in the Hematopoietic Progenitor Cell Transplantation program at the Hospital das Clínicas de Botucatu, facilitating decision-making according to the latest scientific evidence and contributing to minimize differences of conduct guided by a hospital nutritional protocol. Materials and Methods: the manual is a narrative review of the scientific literature, using relevant articles and guidelines contained in the Pubmed, Lilacs and Scielo databases, as well as textbooks and consensus books from year 2000 to 2017. The terms used for the research were “nutrition assessment”, “nutrition therapy”, “nutrition risk”, “undernutrition”, “malnutrition”, “obesity”, “chemotherapy”, “blood marrow transplantation”, “haematopoietic stem cell transplantation","Body composition","phase angle". Results: there are few specific studies related to nutritional therapy and HSCT. The search resulted in the use of 20 scientific papers that support the production of this dissertation. Considering the structure and dynamics of Hospital das Clínicas de Botucatu, 10 the standardization of conducts in this Manual led to the elaboration of a protocol in the form of flowchart that includes the evaluation of Nutritional Risk and Nutritional Therapy in patients undergoing HSCT. Conclusion: the risk assessment and nutrition therapy application protocols, built in the form of a flowchart, facilitate the applicability of the manual contents, simplify the classification of nutritional risk groups, provide rapid pipeline elaboration and avoid divergences of prescription regarding the best nutritional therapy in patients undergoing HSCT.
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Protocolo para avaliação e terapia nutricional no transplante de células hematopoiéticas em pacientes do Hospital das Clínicas de BotucatuCosta, Cesar Martins da January 2018 (has links)
Orientador: Paula Schmidt Azevedo Gaiolla / Resumo: O Transplante de Células Progenitoras Hematopoiéticas (TCPH) é um método terapêutico utilizado no tratamento de diversas doenças que envolvem o tecido linfo-hematopoiético, doenças autoimunes e condições não-malignas. As evidências apontam que o reconhecimento precoce de pacientes em grupos de risco nutricional no TCPH e a elaboração de um plano terapêutico para tal tem impacto positivo na redução da mortalidade. A monitorização diária das necessidades energéticas, proteicas e de nutrientes é um dos pontos cruciais da terapia, pois o paciente que é incapaz de suprir mais do que 60% das necessidades nutricionais diárias por via oral torna-se candidato a outras modalidades de terapia (enteral ou parenteral), a depender da viabilidade do trato gastrointestinal, das contra-indicações relativas a cada método (plaquetopenia na introdução de sonda nasoenteral, por exemplo) e das complicações associadas aos procedimentos (aumento das taxas de infecção de corrente sanguínea na nutrição parenteral). Se o paciente atingir mais do que 60% das necessidades nutricionais por via oral e mantiver esse aporte por pelo menos 3 dias, o suporte por nutrição enteral ou parenteral pode ser descontinuado. A literatura científica ainda não elucidou todos os questionamentos quanto à melhor abordagem nutricional em pacientes submetidos a TCPH, podendo-se observar grande variação entre as condutas orientadas pelas diretrizes internacionais mais recentes e o que se adota como prática clínica diária, cham... (Resumo completo, clicar acesso eletrônico abaixo) / Abstract: Hematopoietic Stem Cell Transplantation (HSCT) is a therapeutic method used for treatment of various diseases involving lymphohematopoietic tissue, autoimmune diseases and non-malignant conditions. Evidence indicates that the early recognition of nutritional risk in HSCT patients and the elaboration of a therapeutic plan for them has a positive impact in reducing mortality. Monitoring daily needs of energy, protein and nutrient is one of the crucial points of therapy, because individuals who are unable to supply more than 60% of the daily nutritional needs orally become candidates for other modalities of therapy (enteral or parenteral), depending on the viability of the gastrointestinal tract, contraindications for each method (thrombocytopenia in the introduction of nasoenteral probe, for example) and complications associated with procedures (increased bloodstream infection rates in parenteral nutrition) . If the patient reaches more than 60% of nutritional needs orally and maintains this intake for at least 3 days, enteral or parenteral nutrition support may be discontinued. The scientific literature has not yet elucidated all the questions regarding the best nutritional approach in patients undergoing HSCT and a great variation between the conducts guided by the most recent international guidelines and what is adopted as daily clinical practice can be observed, drawing attention to the need for nutritional protocols that could reduce these divergences. Objectives: elabora... (Complete abstract click electronic access below) / Mestre
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Análise de polimorfismos dos genes HFE, fator V de Leiden, protrombina, glutationa-S transferase, metilenotetrahidrofolato e o risco de doença veno-oclusiva hepática em pacientes submetidos a transplante alogênico de células tronco hematopoiéticas: Estudo clínico observacional / Inglês: Analysis genetic polymorphisms of HFE, prothrombin, factor V Leiden, methylenetetrahydrofolate reductase, glutathione S-transferase in hepatic veno-occlusive disease after hematopoietic stem cell transplantation: a observe clinical studyResende Junior, José Dias [UNIFESP] 29 October 2010 (has links) (PDF)
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Publico-018.pdf: 1910669 bytes, checksum: a40b61267560276f1db47642341c6e56 (MD5) / Introdução: Polimorfismos genéticos estão associados com um aumento do risco de tromboembolismo venoso (TEV) e outras doenças cardiovasculares. Estudos prévios sugerem que a doença venooclusiva hepática (DVOH), que se desenvolve intra transplante de medula óssea pode ser atribuída à polimorfismos gênicos. Objetivos: Avaliar a correlação entre polimorfismos genéticos e o risco de doença venooclusiva hepática no transplante de medula óssea e a associação com a presença de variáveis como o uso de vancomicina, drogas citotóxicas usadas no regime de condicionamento, presença de disfução hepática anterior ao transplante, presença de infecção por citomegalovírus, e grupos de doenças avaliáveis. Pacientes e métodos: Este estudo caracteriza-se por um estudo clinico observacional multicêntrico. Foram avaliados 120 pacientes, submetidos a transplante alogênico de medula óssea. Cada paciente foi avaliado propectivamente para DVOH, confirmado pelo critério de Seattle modificado, idade variando de 2 a 65 anos. Fatores de risco para DVOH severo foram analisados usando modelos estatisticos de avaliação. Detectamos simultaneamente através de PCR seguido de digestão e detecção através de eletroforese em gel de agarose, mutação do HFE C282Y, H63D, S65C; MTHFR C677T; Fator V de Leiden, Protrombina 20210A e glutationa S-tranferase. Resultados: Neste estudo observacional de pessoas, submetidas a transplante de medula óssea alogênico, a presença de disfução hepática pré transplante foi um fator de risco significante para DVOH. Nós tambem observamos uma associação entre a presença de mutação HFE S65C e disfunção hepática. Conclusões: Em resumo, nossos dados sugerem que disfunção hepatica observada pré transplante de medula óssea é um fator de risco estatisticamente significante para DVOH e que a presença da mutação do HFE S65C apresenta uma tendência ao desenvolvimento de dano hepático. Contudo, não evidenciamos associação dos polimorfismos estudados com DVOH. / TEDE
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Viral Abrogation of Stem Cell Transplantation Tolerance Causes Graft Rejection and Host Death by Different Mechanisms: A DissertationForman, Daron 22 May 2002 (has links)
Tolerance-based stem cell transplantation using sub-lethal conditioning is being considered for the treatment of human disease, but safety and efficacy remain to be established. In order to study these two issues, we first established that mouse bone marrow recipients treated with sub-lethal irradiation plus transient blockade of the CD40-CD154 costimulatory pathway develop permanent hematopoietic chimerism across allogeneic barriers. Our conditioning regimen of 6 Gy irradiation, a short course of anti-CD154 mAb and 25 million fully allogeneic BALB/c bone marrow cells consistently produced long-term, stable, and multilineage chimerism in C57BL/6 recipients. Furthermore, chimeric mice displayed donor-specific transplantation tolerance, as BALB/c skin allografts were permanently accepted while third-party CBA/JCr skin allografts were promptly rejected. We next determined both the safety and efficacy of this protocol by infecting chimeric mice with lymphocytic choriomeningitis virus (LCMV) either at the time of transplantation or at several time points afterwards. Infection with LCMV at the time of transplantation prevented engraftment of allogeneic, but not syngeneic, bone marrow in similarly treated mice. Surprisingly, infected allograft recipients also failed to clear the virus and died. Post-mortem study revealed hypoplastic bone marrow and spleens. Hypoplasia and death in these mice required the combination of 6 Gy irradiation, LCMV infection on the day of transplantation, and an allogeneic bone marrow transplant but did not require the presence of anti-CDl54 mAb. Allochimeric mice infected with LCMV 15 days after transplantation were able to survive and maintain their bone marrow graft, indicating that the deleterious effects of LCMV infection on host and graft survival are confined to a narrow window of time during the tolerization and transplantation process. The final section of this thesis studied the mechanisms of graft rejection and death in sublethally irradiated recipients of allogeneic bone marrow and infection with LCMV at the time of bone marrow transplantation. Infection of interferon-α/β receptor knockout mice at the time of transplantation prevented the engraftment of allogeneic bone marrow, but the mice survived. Therefore, IFN-αβ is involved in the development of marrow hypoplasia and death, whereas a second mechanism is involved in blocking the development of chimerism in these mice. Through the use of depleting mAb's and knockout mice we demonstrate that three types of recipients survived and became chimeric after being given sublethal irradiation, anti-CD154 mAb, an allogeneic bone marrow transplant and a day 0 LCMV infection: mice depleted of CD8+ T cells, CD8 knockout mice, and TCR-αβ knockout mice. Our data indicate that the mediator of bone marrow allograft destruction in LCMV-infected mice treated with costimulatory blockade is a radioresistant CD8+ NK1.1- TCRαβ+ T cell. We conclude that a non-cytopathic viral infection at the time of transplantation can prevent engraftment of allogeneic bone marrow and result in the death of sub-lethally irradiated mice treated with costimulation blockade. The abrogation of allogeneic bone marrow engraftment is mediated by a population of CD8+ NK1.1- TCRαβ+ T cells and the mediator of hypoplasia and death is viral induction of IFN-αβ.
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Avaliação da função tímica em pacientes com diabetes mellitus tipo 1 submetidos ao transplante autólogo de células-tronco hematopoéticas / Evaluation of thymic function in type 1 diabetes mellitus patients following autologous hematopoietic stem cell transplantation.Júlia Teixeira Cottas de Azevedo 19 August 2013 (has links)
O diabetes mellitus tipo 1 (DM-1) é uma doença autoimune órgão-específica caracterizada pela destruição seletiva das células pancreáticas produtoras de insulina. A imunossupressão em altas doses seguida do transplante autólogo de células-tronco hematopoéticas (TACTH) constitui uma alternativa terapêutica recente e promissora para o DM-1 recém-diagnosticado, impedindo a progressão da destruição das células pancreáticas produtoras de insulina e induzindo independência insulínica por um período prolongado na maioria dos pacientes. O princípio dessa terapia baseia-se na eliminação das células autorreativas pela imunossupressão intensa e na reconstituição de um sistema imunológico novo e tolerante após o transplante. Com o objetivo de avaliar a função do timo e sua contribuição na geração do repertório de células T nos pacientes com DM-1 após o TACTH, nesse trabalho foram avaliados os níveis de T cell receptor excision circles (TRECs) em células T do sangue periférico e a diversidade do repertório de células T dos pacientes com DM-1 (n=23) antes e em diversos períodos após o transplante. A quantificação absoluta dos níveis de TRECs (número de moléculas de TRECs/100g de DNA) foi realizada pela técnica de PCR em tempo real e a avaliação do repertório de células T foi realizada pela técnica de TCRBV CDR3 Spectratyping. Dentre os vinte e três pacientes, vinte alcançaram a independência insulínica por períodos variáveis de tempo e três não responderam ao tratamento. Não foi observada a restrição do repertório de células T nos pacientes com DM-1 no período pré-transplante, ou seja, quando recém-diagnosticados. Foram identificadas cinco famílias V (7, 18, 19, 20 e 22) em expansão clonal nos pacientes com DM-1. As famílias V 7, 18, 19, 20 apresentaram-se em expansão clonal antes do transplante e se mantiveram com frequência elevada após o transplante, enquanto a família V 22 apresentou aumento da frequência somente nos períodos mais tardios após o transplante. Nos primeiros meses após o transplante, houve redução do número de moléculas de TRECs e restrição do repertório de células T. Contudo, um ano após o transplante, o número de moléculas de TRECs atingiram valores normais e o repertório de células T apresentou-se com ampla diversidade. Nossos resultados mostraram que o TACTH foi capaz de induzir mudanças na composição do repertório de células T dos pacientes com DM-1 após a terapia de IAD/TACTH, evidenciadas por alterações qualitativas e quantitativas dos picos de CDR3 do TCR, sugerindo a reconstituição de um repertório de células T diverso até dois anos pós-transplante. Embora tenha ocorrido reativação da função tímica após o transplante, evidenciada pelo aumento dos níveis de TRECs de um ano e meio a cinco anos pós-transplante, a diversidade do repertório das células T diminuiu a partir de dois anos e meio pós-transplante, sugerindo uma reconstituição tímica de novo de células T naive que expressam preferencialmente algumas cadeias V. Estas evidências imunológicas poderiam explicar a melhora clínica (independência insulínica) temporária observada na maioria dos pacientes após a terapia de IAD/TACTH. / Type 1 diabetes mellitus (T1D) is an organ-specific autoimmune disease characterized by insulin-producing pancreatic cell destruction. High-dose immunosuppression followed by autologous hematopoietic stem cell transplantation (AHSCT) is a recent and promising therapeutic approach for treatment of T1D, preventing the progress of destruction of pancreatic cells and inducing insulin independence for a prolonged period in most patients. The rationale of the AHSCT is based on the elimination of autoreactive cells by the intense immunosuppression and on the reconstitution of a new and tolerant immune system after transplantation. Aiming at assessing the thymic role in the production of new T cell repertoire in T1D patients after AHSCT, in this study was evaluated the levels of T cell receptor excision circles (TRECs) in T cells of peripheral blood as well as the clonality and diversity of T cell repertoire in T1D patients (n=23) before and several periods after transplantation. The absolute quantification of TRECs levels (number of molecules of TRECs/100ng of DNA) was performed by real-time PCR and the analysis of T cell repertoire was performed by TCRBV CDR3 Spectratyping. Among the twenty-three patients, twenty achieved insulin independence for variable periods and three did not respond to the treatment. The T cell repertoire in T1D patients was not restricted in pre-transplantation, i.e., when newly diagnosed. It was identified five V families (7, 18, 19, 20 e 22) in the clonal expansion in T1D patients. The V families 7, 18, 19, 20 were in clonal expansion before transplantation and maintained with high frequency after transplantation, whereas the V 22 family increased its frequency only in the later periods after transplantation. It was observed that the numbers of molecules of TRECs decreased and the T cell repertoire was restricted in the early months after transplantation. However, the levels of TRECs were normalized and the T cell repertoire showed diversity one year after transplantation. Our results indicate that AHSCT was able to induce changes in the composition of the T cell repertoire of patients after AHSCT, evidenced by qualitative and quantitative changes in the composition of T-cell receptor -chain CDR3 peaks, suggesting the reconstitution of diverse T cell repertoire up to two years after transplantation. Although there was reactivation of thymic function after transplantation, as evidenced by increased levels of TRECs from one and a half year to five years after transplantation, the diversity of the T cells repertoire decreased from two and a half years after transplantation, suggesting a reconstruction of new naive T cells that preferentially express some V chains. These immunological evidences could explain the temporary clinical improvement (insulin independence) observed in most patients after IAD / AHSCT therapy.
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Medidas utilizadas na prevenção de infecções em transplante de células-tronco hematopoéticas: evidências para a prática / Infection prevention measures used in hematopoietic stem cell transplantation: evidences for practiceLivia Maria Garbin 30 June 2010 (has links)
O transplante de células-tronco hematopoéticas (TCTH) consiste em um procedimento complexo e relacionado à ocorrência de diversas complicações, dentre elas os processos infecciosos decorrentes do longo período de imunossupressão vivenciado após a instituição do regime de condicionamento. Inúmeras medidas têm sido empregadas visando à prevenção e controle de infecções, porém, observam-se divergências em relação à utilização das mesmas; sendo que o emprego da prática baseada em evidências possibilita ao profissional tomar decisões em relação à sua prática fundamentadas em resultados de pesquisas científicas atuais. Esta revisão integrativa da literatura teve como objetivo identificar e avaliar as evidências disponíveis na literatura e publicadas nos últimos 20 anos em relação ao uso de três medidas de prevenção de infecção em pacientes submetidos ao TCTH durante o período de internação: uso de filtros de ar de alta eficiência, isolamento protetor e máscaras. Para a seleção dos artigos foram utilizadas as bases de dados LILACS, PUBMED, CINAHL, EMBASE e a Biblioteca Cochrane. A amostra foi composta por 15 estudos, sendo que apenas um apresentou nível de evidência forte (nível I), dois apresentaram nível de evidência moderado (nível IV e V) e doze consistiram em estudos com evidências fracas (nível VI e VII). Dez estudos abordaram a utilização dos filtros HEPA, sendo recomendado seu emprego para pacientes submetidos ao transplante alogênico durante o período de neutropenia. A necessidade de seu uso para pacientes submetidos ao transplante autólogo ainda é controversa. Nove trabalhos abordaram o uso do isolamento protetor e, embora alguns autores relatem que o emprego do mesmo parece apresentar benefícios quando não se dispõe de filtros HEPA, a utilização desta medida já não é mais indicada tanto pelos Centers for Disease Control and Prevention (CDC) quanto pela maioria dos estudos analisados. Em relação à utilização de máscaras por pacientes, profissionais de saúde ou visitantes dentro das unidades de internação para TCTH, não foram encontrados estudos com evidências fortes que justifiquem o seu uso. No entanto, recomenda-se que sejam seguidas as diretrizes dos CDC quanto ao uso de respiradores especiais (como as máscaras N95) pelos pacientes imunocomprometidos submetidos ao TCTH ao deixar a unidade de transplante provida de filtro HEPA quando próximo a ela houver áreas de construção/reforma ou atividades geradoras de poeira. Embora os dados evidenciados auxiliem na tomada de decisão para a implementação da assistência de enfermagem a estes pacientes, verificou-se a necessidade de realização de estudos com nível de evidência forte que comprovem ou refutem a efetividade destas medidas. / Hematopoietic stem cell transplantation (HSCT) is a complex procedure related to the occurrence of different complications, including infectious processes deriving from the long period of immunosuppression experienced after the establishment of the conditioning regimen. Countless measures have been used for infection prevention and control, but divergences are observed with regard to their use; evidence-based practice allows professionals to make decisions for practice based on current scientific research results. This integrative literature review aimed to identify and assess evidence available in literature and published in the last 20 years about the use of three infection prevention measures in patients submitted to HSCT during hospitalization: use of high-efficiency air filters, protective isolation and masks. LILACS, PUBMED, CINAHL, EMBASE and the Cochrane Library were used to select the articles. The sample comprised 15 studies, only one of which presented strong evidence (level I), while two presented moderate evidence (levels IV and V) and twelve were studies with weak evidence (levels VI and VII). Ten studies discussed the use of HEPA filters, recommended for patients submitted to allogeneic transplantation during the neutropenia period. It remains controversial whether these filters need to be used for patients submitted to autologous transplant. Nine studies addressed the use of protective isolation and, although some authors report that using this measure can be beneficial when HEPA filters are unavailable, neither the Centers for Disease Control and Prevention (CDC) nor by most of the studies under analysis indicate it any longer. With regard to the use of masks by patients, health professionals or visitors inside HSCT hospitalization units, no studies with strong evidence were found that justify its use. However, it is recommended that CDC recommendations be followed regarding the use of special respirators (like N95 masks) by immunocompromised patients submitted to HSCT when they leave the transplantation unit with a HEPA filter in case of nearby construction/reform areas or activities that generate dust. Although the evidenced data support decision making with a view to nursing care delivery to these patients, research with strong evidence is needed to prove or reject the efficacy of these measures.
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Modulation de l’effet des lymphocytes T régulateurs par la voie TNFα/TNFR2 : une nouvelle immunothérapie en allogreffe de cellules souches hématopoïétiques / Modulation of regulatory T cells function through the TNFα/TNFR2 pathway : a new immune therapy for allogeneic hematopoietic stem cell transplantationLeclerc, Mathieu 21 June 2017 (has links)
Les lymphocytes T régulateurs (Treg) jouent un rôle majeur dans la modulation de l’alloréactivité après allogreffe de cellules souches hématopoïétiques et permettent notamment de contrôler la réaction du greffon contre l’hôte (GVH) dans des modèles expérimentaux. Le potentiel thérapeutique des Treg est donc très important dans ce domaine, mais aussi dans l’auto-immunité ou en cancérologie. Cependant, de nombreuses barrières rendent difficile l’élaboration de stratégies thérapeutiques reposant sur le transfert adoptif de Treg chez l’homme et une meilleure compréhension des facteurs et mécanismes contrôlant la prolifération et les capacités suppressives de ces cellules permettrait de les cibler directement et si possible spécifiquement in vivo.Dans ce travail, après avoir élaboré un nouveau système d’évaluation clinique de la GVH chez la souris et démontré sa simplicité, sa reproductibilité et sa performance, nous avons pu montrer que l’action suppressive des Treg dans la GVH dépendait de l’interaction entre le TNFα produit par les lymphocytes T conventionnels (Tconv) du donneur et le récepteur TNFR2 exprimé par les Treg. En effet, en bloquant cette interaction de 3 façons différentes, à savoir par un anticorps monoclonal bloquant anti-TNFR2, ou en utilisant soit des Treg n’exprimant pas TNFR2 soit des Tconv ne produisant pas de TNFα, nous avons à chaque fois montré que l’effet protecteur des Treg était aboli en l’absence du signal TNF. Le récepteur TNFR2 étant exprimé préférentiellement par les Treg par rapport aux Tconv, nos résultats ouvrent la voie au ciblage des Treg in vivo via TNFR2, soit pour activer ce récepteur par un agoniste et donc stimuler les Treg afin de contrôler la GVH, soit à l’inverse pour bloquer l’axe TNFα/TNFR2 par un antagoniste et ainsi inhiber les Treg, ce qui permettrait alors de lever un frein à l’alloréactivité dans les situations où l’on cherche à la stimuler pour renforcer l’effet anti-tumoral, comme par exemple dans le cas des rechutes post-allogreffe. / Regulatory T cells (Tregs) are key players involved in the modulation of alloreactivity after hematopoietic stem cell transplantation. Indeed, Tregs can prevent graft-versus-host disease (GVHD) in experimental models. Therefore, the therapeutic potential of these cells in GVHD is substantial, as it is in other fields like auto-immunity or oncology. However, many obstacles still make the application of cellular therapy strategies based on the adoptive transfer of Tregs in humans quite complicated. A better understanding of factors and mechanisms that control the proliferation and suppressive capacities of Tregs could allow for a direct and specific targeting of these cells in vivo.In this work, after designing a new clinical grading system for murine GVHD and demonstrating its ease of use, reproducibility and performance, we have shown that the suppressive action of Tregs in GVHD depends on the interaction between TNFα produced by donor conventional T cells (Tconvs) and TNFR2 expressed by Tregs. Using 3 different ways to block this interaction, i.e. with an anti-TNFR2 blocking monoclonal antibody, or Tregs that do not express TNFR2 or donor Tconvs that cannot produce TNFα, we were able to show in each situation that blocking TNF signaling resulted in a loss of protection by Tregs. TNFR2 being highly expressed by Tregs as compared with Tconvs, our results pave the way for in vivo targeting of Tregs through TNFR2, either to activate this receptor with an agonist and therefore stimulate Tregs to control GVHD, or to block the TNFα/TNFR2 axis with an antagonist and in this case inhibit Tregs, which could boost alloreactivity, as expected in some particular settings like post-transplant relapse.
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Natural Killer Cells for Therapy of LeukemiaSuck, Garnet, Linn, Yeh Ching, Tonn, Torsten 05 August 2020 (has links)
Clinical application of natural killer (NK) cells against leukemia is an area of intense investigation. In human leukocyte antigen-mismatched allogeneic hematopoietic stem cell transplantations (HSCT), alloreactive NK cells exert powerful anti-leukemic activity in preventing relapse in the absence of graft-versus-host disease, particularly in acute myeloid leukemia patients. Adoptive transfer of donor NK cells post-HSCT or in non-transplant scenarios may be superior to the currently widely used unmanipulated donor lymphocyte infusion. This concept could be further improved through transfusion of activated NK cells. Significant progress has been made in good manufacturing practice (GMP)-compliant large-scale production of stimulated effectors. However, inherent limitations remain. These include differing yields and compositions of the end-product due to donor variability and inefficient means for cryopreservation. Moreover, the impact of the various novel activation strategies on NK cell biology and in vivo behavior are barely understood. In contrast, reproduction of the thirdparty NK-92 drug from a cryostored GMP-compliant master cell bank is straightforward and efficient. Safety for the application of this highly cytotoxic cell line was demonstrated in first clinical trials. This novel ‘off-theshelf’ product could become a treatment option for a broad patient population. For specific tumor targeting chimeric-antigen-receptor-engineered NK-92 cells have been designed.
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Treating GM1 Gangliosidosis With Ex Vivo Hematopoietic Stem Cell Gene Therapy Without Using Total Body Irradiation: A Masters ThesisWhalen, Michael 31 August 2011 (has links)
GM1 gangliosidosis is an autosomal recessive lysosomal storage disease, caused by a deficiency in the enzyme β-galactosidase. The disease affects the CNS, liver, kidney, heart and skeletal system, leading to severe neurodegeneration and death. We propose to treat this disorder using ex vivo hematopoietic stem cell therapy. The effectiveness of this therapy requires the recruitment of transduced donor cells to the CNS. This is only found to occur after mice are conditioned with total body irradiation, due to the increase in CNS cytokine production and blood brain barrier permeability that occurs. As the use of total body irradiation in pediatric patients has been linked to future developmental problems, this myeloablation approach is often avoided in younger patients in favor of a conditioning regimen using the chemotherapy drugs, busulfan and cyclophosphamide. Whether donor cells can enter the CNS when a busulfan and cyclophosphamide conditioning regimen is used has not been determined. In this study we plan to quantify the cytokine and blood-brain barrier permeability increases necessary for donor cells to be recruited to the CNS after total body irradiation. We will then investigate whether busulfan and cyclophosphamide conditioning and/or the chronic neuroinflammation present in GM1 mice can produce similar conditions and facilitate the recruitment of donor hematopoietic stem cells to the CNS. Finally we will assess whether ex vivo hematopoietic stem cell gene therapy is still an effective therapy when busulfan and cyclophosphamide are used for myeloablative conditioning.
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