Global ETD Search

21	Etude des dysfonctions lymphocitaires T dans le syndrome néphrotique idiopathique / Investigating T cells dysfunctions in minimal-change nephrotic syndrom Vachin, Pauline 19 January 2018 (has links) La pathogénie du syndrome néphrotique idiopathique est inconnue, mais de nombreux arguments clinques et expérimentaux favorisent l’hypothèse d’une pathogénie dys-immunitaire à expression immunologique et rénale, au cours de laquelle on observerait une altération des lymphocytes T. Cependant, le mécanisme exact reste encore mal connu. Récemment, le Rituximab, un anticorps dirigé contre l’antigène CD20, a montré une efficacité à induire une rémission à moyen et long terme suggérant l’implication d’une dysfonction des lymphocytes B et/ou un défaut de coopération T-B. Notre laboratoire a isolé un nouveau gène C-MIP dont l’expression est induite dans certaines sous-populations lymphocytaires T et B, ainsi que dans les podocytes de patients atteints de SNI en phase de poussée mais quasiment indétectable chez les sujets sains.Dans ces travaux, ancillaires au PHRC NEPHRUTIX, nous avons étudié les perturbations lymphocytaires T, avant, au moment de la rechute et en période de rémission au cours de syndrome néphrotique à lésions glomérulaires minimes et l’effet du traitement par le Rituximab. Dans cette étude, nous avons mis en évidence que la rechute était associée à un effondrement des lymphocytes T régulateurs, une baisse profonde de l’interleukine-2 ainsi qu’à une surexpression significative de C-MIP, précédant la survenue de la rechute. Ces modifications se restaurent en rémission. Enfin, la rémission obtenue dans le bras Rituximab, entraîne une diminution des lymphocytes T folliculaires (Tfh), des iNKT et des cellules double-négatives DN-TCR Vα24, suggérant que le SNLGM implique un défaut des réponses immunitaires innées et adaptatives, qui peut être stabilisé par un traitement par Rituximab.Afin d’étudier le rôle de C-MIP, nous avons généré des souris transgéniques sur-exprimant ce gène dans les lymphocytes T matures périphériques. Cette surexpression est à l’origine d’un phénotype lymphocytaire altéré marqué par une accumulation de lymphocytes T naïfs, un effondrement des cytokines activatrices de type Th1 et Th2 et une accumulation des formes inactives des Src kinases. Ces résultats suggèrent que C-MIP, en inhibant les Src kinases, est un régulateur négatif de l’activation T impliqué dans la signalisation proximale et pourrait être impliqué dans l’hypo-réactivité lymphocytaire T observée chez les patients atteints de SNLGM actif. / The pathogenesis of minimal-change nephrotic syndrom (MCNS) is unknown, but, supported by many clinical and experimental arguments, it was suggested that MCNS is a dys-immune disorder with immunogical and renal expression, during which T-cell alteration would be observed. However, the exact mechanism remains unknown. Recently, Rituximab, a B-cell depleting agent, is effctive in inducing mid- and long-term remission suggesting involvement of B-cell dysfunction and/or lack of T-B cooperation. Our laboratory identified a new gene: C-MIP. We have shown that C-MIP abundance is increased in some T and B lymphocyte subpopulations, as well as in podocytes of MCNS patients during relapse phase but undetectable in healthy subjects.In this work, ancillary to the NEPHRUTIX PHRC, we studied T-cell disturbances before and during the relapse or during the remission time in MCNS and the effect of Rituximab therapy. In this study, we found that relapses were associated with significant decrease in regulatory T cell and interleukin-2 expression, while C-MIP abundance was significantly increased. These changes are restored during remission time. Finally, remission after Rituximab therapy leads to a decrease in follicular T cells (Tfh), iNKT and double-negative (CD4- CD8-) T cells expressing the invariant Vα24 chain, suggesting that MCNS involves a disorder of innate and adaptative immune response, which can be stabilized by Rituximab treatment.In order to study the C-MIP role, we generated transgenic mice overexpressing this gene in the peripheral mature T-cells. This overexpression leads to an altered lymphocyte phenotype with an accumulation of naive T lymphocytes, a significant decrease of Th1 and Th2 activating cytokines and accumulation of inactive Src kinases. These results suggest that, by inhibiting Src kinases, C-MIP is a negative regulator of activation T involved in proximal signalling and may be responsable of the lymphocyte T hypo-reactivity observed in patients with active MCNS. C-Mip Rituximab Signalisation proximale Lymphocyte T C-Mip Minimal Change Nephrotic Syndrom Rituximab Proximal signalling T lymphocyte 610
22	Defining clinically relevant subgroups of follicular lymphoma cases according to the functional status of the CDKN2A gene Alhejaily, Abdulmohsen 13 March 2013 (has links) Follicular lymphoma (FL) is the second most common non-Hodgkin lymphoma (NHL). FL is clinically designated as an indolent disease with a long median survival of 8-10 years. However, the clinical and biological behavior of FL shows considerable variability, with some patients showing aggressive disease progression and very short survival. Because defects in the regulation of apoptotic cell death are fundamental in FL pathogenesis, we hypothesized that deregulated expression of components of the pRb signaling pathway may promote cell proliferation, thereby complementing antecedent anti-apoptotic mutations and producing more aggressive disease. In the present study we undertook an immunohistochemical (IHC) evaluation of expression of key cell-cycle regulatory proteins in diagnostic biopsies from 127 cases of FL using formalin-fixed, paraffin-embedded tissues (FFPE) in tissue microarray (TMA) sections immunostained for p53, pRb, p16INK4A and cyclin D3. Data analysis revealed that increased abundance of p53 or p16INK4A is associated with reduced overall survival (OS) (p=0.005 and p=0.014 respectively), and with conventional pathological markers of tumour aggressiveness including high histologic grade. Encouraged by this remarkable finding of a counterintuitive association between p16INK4A expression and clinical outcome, we analyzed CDKN2A gene deletion and methylation, as these are the most frequent mechanisms of the CDKN2A gene inactivation in NHL including FL. We determined the deletion and methylation status of CDKN2A in 105 FL cases. Laser-capture microdissection was used to enrich the samples for lymphoma cells. CDKN2A was deleted in 9 cases and methylated in 22 cases. The 29 cases (28%) with CDKN2A deletion or methylation had decreased overall survival (OS) (p=0.046) in all cases and in cases treated with rituximab (p<0.001). Our findings indicate that deleterious alterations of CDKN2A are relatively prevalent in FL at diagnosis and can predict poor clinical outcome. In summary, our data reveal novel insights into the pathogenesis of FL and suggest a relationship between increased p16INK4A expression and CDKN2A deletion or methylation and unfavorable clinical outcome in FL. We hope that the work presented herein will provide a useful prognostic tool for predicting the prognosis and choosing optimal treatment approaches to help patients suffering from FL. / Thesis (Ph.D, Pathology & Molecular Medicine) -- Queen's University, 2013-03-12 23:49:44.541 Biomarkers Personalized medicine Follicular lymphoma Cell cycle Rituximab FLIPI CD20 NHL Prognostic CDKN2A
23	Implication de l'association CD20/CD40 dans la mort cellulaire induite via le CD20 Al-Zoobi, Loubna 06 1900 (has links) CD20 est une phosphoprotéine transmembranaire exprimée spécifiquement à la surface des lymphocytes B. Malgré les nombreuses études qui ont montré son implication dans le flux calcique, son rôle physiologique est assez mal connu. Cependant, des études récentes ont démontré que CD20 peut jouer un rôle important dans la mort cellulaire. D’ailleurs, le rituximab, un anticorps monoclonal chimérique dirigé contre CD20 humain, a montré son efficacité dans le traitement de nombreuses maladies auto-immunes. Cet anticorps est capable d’induire une profonde déplétion des lymphocytes B, qui va également interférer avec la coopération T et la sécrétion de cytokines. En plus, l’engagement du CD20 à la surface des cellules induit la mort cellulaire, alors que la partie cytoplasmique de cette molécule ne possède pas un motif de mort. Donc, il est possible que cette réponse soit médiée par des molécules qui semblent être associées au CD20 comme CD40. En effet, CD40, une glycoprotéine transmembranaire de type I, est un composant majeur du système immunitaire, dont l’engagement pourrait moduler la fonction cellulaire et même conduire à la mort rapide des cellules B. Le travail présenté dans ce mémoire porte sur l’étude de la mort cellulaire induite par un anti-CD20, le rituximab, ainsi que l’étude du rôle de l’association CD20/CD40 dans la mort cellulaire médiée par cet anticorps. Nos résultats montrent que la mort cellulaire induite par le rituximab varie en fonction du type cellulaire et du niveau d’expression du CD20, et que la présence du CD40 à la surface des cellules augmente l’activité de la mort cellulaire induite par le rituximab. En plus, CD20 et CD40 sont associés à la surface cellulaire, et la partie cytoplasmique n’est pas impliquée dans cette association mais semble être importante dans la mort cellulaire induite via CD20. / CD20 is a transmembrane phosphoprotein specifically expressed at the surface of B cells. Despite the many studies that have shown its involvement in calcium flux, its physiological role is poorly understood. However, recent studies have shown that CD20 can play an important role in cell death. Moreover, rituximab, a chimeric monoclonal antibody directed against human CD20, has shown efficacy in the treatment of many autoimmune diseases. Indeed, this antibody is able to induce a profound depletion of B cells and interfere in T cooperation and secretion of cytokines. In addition, the engagement of CD20 at the cell surface induces cell death, while the cytoplasmic portion of this molecule has no death domain. So, it is possible that this response is mediated by molecules that could be associated with CD20, like CD40. In fact, CD40, a type I transmembrane glycoprotein, is a major component of the immune system. The engagement of CD40 can modulate cellular function and may even lead to rapid B cell death. The work presented in this thesis will focus on the study of cell death induced by an anti-CD20, rituximab, and on the role of the association of CD40 with CD20 at the cell surface in susceptibility to cell death mediated by this antibody. Our results show that cell death induced by rituximab depends on cell type and on the levels of expression of CD20, and that the presence of CD40 at the cell surface increases cell death induced by rituximab. In addition, CD20 and CD40 are associated at the cell surface, and the cytoplasmic portion is not involved in this association but seems to be important in induction of cell death by CD20. CD20 CD40 rituximab mort cellulaire association cell death
24	Células natural killer em uma coorte de pacientes com artrite reumatóide tratados com rituximabe Garcia, Mariana Pires January 2013 (has links) OBJETIVOS: Avaliar o perfil e o número absoluto e percentual de células NK verdadeiras (CD56+CD16+CD3-) e de células NK e NKT (CD56+) no sangue periférico de uma coorte de pacientes com artrite reumatóide (AR) antes e durante o tratamento com rituximabe (RTX). MÉTODOS: Foram analisados dez pacientes do grupo controle (doadores de sangue) e dez pacientes com AR que receberam duas infusões de RTX 1g separadas por intervalo de 14 dias. As análises imunofenotípicas para avaliação do perfil e quantificação de células NK foram realizadas pré e após a infusão ou até a recaída clínica. Pacientes respondedores e não respondedores foram classificados de acordo com os critérios do Colégio Americano de Reumatologia (ACR) em 6 meses. RESULTADOS: A quantidade de células NK verdadeiras não demonstrou variação significativa pré e após o tratamento com RTX. Contudo, houve aumento percentual de células CD56+ entre o primeiro e o segundo mês após a infusão com RTX. Além disso, os pacientes respondedores apresentaram uma tendência de aumento do número absoluto de células NK verdadeiras após dois meses de tratamento. Já em relação ao grupo controle, observou-se um aumento significativo do número de células NK basais nos pacientes com AR (p<0,05). CONCLUSÕES: Foi identificada uma tendência de aumento nos valores absolutos de células NK verdadeiras entre os pacientes respondedores no segundo mês após a infusão com RTX. Não foi identificada uma variação significativa no perfil e quantidade de células NK nos pacientes com AR pré e após o tratamento com RTX. Contudo, foi observado que os pacientes com AR possuem uma quantidade maior de células NK do que os controles, sugerindo um possível envolvimento destas células na AR. / OBJECTIVES: To assess the profile as well as the absolute number and percentage of true NK cells (CD56+CD16+CD3-), and NK and NKT cells (CD56+) in the peripheral blood of a cohort of patients with rheumatoid arthritis (RA) before and during rituximab (RTX) therapy. METHODS: Ten control patients (blood donors) and ten patients with RA were assessed. The latter group received two intravenous infusions of 1g RTX, separated by a 14 day interval. Immunophenotypic analyses of NK cells were conducted before and after infusion, or until clinical relapse. After six months, respondents and nonrespondents were reassessed according to American Rheumatology Criteria (ARC). RESULTS: The number of true NK cells did not significantly change after treatment with RTX. However, an increase in the percentage of CD56+ cells was observed between the first and second month after RTX infusion. Respondents also displayed a tendency toward an increased number of true NK cells after two months of treatment. At baseline, the number of NK cells was also found to be significantly higher in patients with RA than in control individuals (p<0.05). CONCLUSIONS: Respondents displayed a tendency toward an increase in the absolute number of true NK cells in the second month after RTX infusion. No significant changes in the profile and frequency of NK cells were found between preand post-RTX treatment assessments of patients with RA. However, it was found that patients with RA have a higher number of NK cells than control partcipants, suggesting a possible role of these cells in RA. Artrite reumatóide Células matadoras naturais Cells natural killer Rituximab Rheumatoid arthritis
25	Comparaison des mécanismes de cytotoxicité des anticorps monoclonaux anti-CD20 Rituximab et GA101 dans les cellules fraiches de la Leucémie Lymphoïde Chronique Reslan, Lina 23 December 2010 (has links) (PDF) CD20 est une cible thérapeutique validée pour l'immunothérapie des néoplasmes lymphoïdesdes cellules B, incluant la Leucémie Lymphoïde Chronique (LLC). Nous avons comparé les effets de rituximab et de GA101 (nouvel anticorps anti-CD20) contre les cellules LLC fraiches in vitro. Le marquage avec Annexine V a démontré une induction de l'apoptose après l'exposition au rituximab et GA101.Contrairement au rituximab, GA101 induisait une réduction du potentiel transmembranaire mitochondrial, uneffet qui peut être partiellement inhibé par la cyclosporine A et qui est partiellement caspase-dépendant. GA101induisait aussi la production des espèces d'oxygènes réactives. L'analyse du niveau d'expression des protéinespro- et anti-apoptotiques après exposition aux anticorps a démontré une forte hétérogénéité entre les échantillons.Bax subissait une activation de conformation et une translocation mitochondriale suite à l'exposition aux anticorps d'une manière caspase-indépendante. GA101, mais pas rituximab, induisait le clivage des caspase-8, -9et -3. En transfectant les cellules LLC avec un siRNA ciblant Bcl-xL utilisant la sonoporation, nous avons trouvéque la réduction du niveau d'expression de Bcl-xL est associée à une augmentation de la sensibilité aux anticorps. Nos résultats suggèrent que les voies de signalisation apoptotiques diffèrent entre rituximab et GA101avec une implication de la voie mitochondriale avec le GA101. L'inhibition de Bcl-xL peut constituer une façon pour sensibiliser les cellules LLC aux effets apoptotiques des anticorps anti-CD20. Leucémie Lymphoïde Chronique Rituximab GA101 Apoptose Sonoporation
26	Implication de l'association CD20/CD40 dans la mort cellulaire induite via le CD20 Al-Zoobi, Loubna 06 1900 (has links) CD20 est une phosphoprotéine transmembranaire exprimée spécifiquement à la surface des lymphocytes B. Malgré les nombreuses études qui ont montré son implication dans le flux calcique, son rôle physiologique est assez mal connu. Cependant, des études récentes ont démontré que CD20 peut jouer un rôle important dans la mort cellulaire. D’ailleurs, le rituximab, un anticorps monoclonal chimérique dirigé contre CD20 humain, a montré son efficacité dans le traitement de nombreuses maladies auto-immunes. Cet anticorps est capable d’induire une profonde déplétion des lymphocytes B, qui va également interférer avec la coopération T et la sécrétion de cytokines. En plus, l’engagement du CD20 à la surface des cellules induit la mort cellulaire, alors que la partie cytoplasmique de cette molécule ne possède pas un motif de mort. Donc, il est possible que cette réponse soit médiée par des molécules qui semblent être associées au CD20 comme CD40. En effet, CD40, une glycoprotéine transmembranaire de type I, est un composant majeur du système immunitaire, dont l’engagement pourrait moduler la fonction cellulaire et même conduire à la mort rapide des cellules B. Le travail présenté dans ce mémoire porte sur l’étude de la mort cellulaire induite par un anti-CD20, le rituximab, ainsi que l’étude du rôle de l’association CD20/CD40 dans la mort cellulaire médiée par cet anticorps. Nos résultats montrent que la mort cellulaire induite par le rituximab varie en fonction du type cellulaire et du niveau d’expression du CD20, et que la présence du CD40 à la surface des cellules augmente l’activité de la mort cellulaire induite par le rituximab. En plus, CD20 et CD40 sont associés à la surface cellulaire, et la partie cytoplasmique n’est pas impliquée dans cette association mais semble être importante dans la mort cellulaire induite via CD20. / CD20 is a transmembrane phosphoprotein specifically expressed at the surface of B cells. Despite the many studies that have shown its involvement in calcium flux, its physiological role is poorly understood. However, recent studies have shown that CD20 can play an important role in cell death. Moreover, rituximab, a chimeric monoclonal antibody directed against human CD20, has shown efficacy in the treatment of many autoimmune diseases. Indeed, this antibody is able to induce a profound depletion of B cells and interfere in T cooperation and secretion of cytokines. In addition, the engagement of CD20 at the cell surface induces cell death, while the cytoplasmic portion of this molecule has no death domain. So, it is possible that this response is mediated by molecules that could be associated with CD20, like CD40. In fact, CD40, a type I transmembrane glycoprotein, is a major component of the immune system. The engagement of CD40 can modulate cellular function and may even lead to rapid B cell death. The work presented in this thesis will focus on the study of cell death induced by an anti-CD20, rituximab, and on the role of the association of CD40 with CD20 at the cell surface in susceptibility to cell death mediated by this antibody. Our results show that cell death induced by rituximab depends on cell type and on the levels of expression of CD20, and that the presence of CD40 at the cell surface increases cell death induced by rituximab. In addition, CD20 and CD40 are associated at the cell surface, and the cytoplasmic portion is not involved in this association but seems to be important in induction of cell death by CD20. CD20 CD40 rituximab mort cellulaire association cell death
27	Células natural killer em uma coorte de pacientes com artrite reumatóide tratados com rituximabe Garcia, Mariana Pires January 2013 (has links) OBJETIVOS: Avaliar o perfil e o número absoluto e percentual de células NK verdadeiras (CD56+CD16+CD3-) e de células NK e NKT (CD56+) no sangue periférico de uma coorte de pacientes com artrite reumatóide (AR) antes e durante o tratamento com rituximabe (RTX). MÉTODOS: Foram analisados dez pacientes do grupo controle (doadores de sangue) e dez pacientes com AR que receberam duas infusões de RTX 1g separadas por intervalo de 14 dias. As análises imunofenotípicas para avaliação do perfil e quantificação de células NK foram realizadas pré e após a infusão ou até a recaída clínica. Pacientes respondedores e não respondedores foram classificados de acordo com os critérios do Colégio Americano de Reumatologia (ACR) em 6 meses. RESULTADOS: A quantidade de células NK verdadeiras não demonstrou variação significativa pré e após o tratamento com RTX. Contudo, houve aumento percentual de células CD56+ entre o primeiro e o segundo mês após a infusão com RTX. Além disso, os pacientes respondedores apresentaram uma tendência de aumento do número absoluto de células NK verdadeiras após dois meses de tratamento. Já em relação ao grupo controle, observou-se um aumento significativo do número de células NK basais nos pacientes com AR (p<0,05). CONCLUSÕES: Foi identificada uma tendência de aumento nos valores absolutos de células NK verdadeiras entre os pacientes respondedores no segundo mês após a infusão com RTX. Não foi identificada uma variação significativa no perfil e quantidade de células NK nos pacientes com AR pré e após o tratamento com RTX. Contudo, foi observado que os pacientes com AR possuem uma quantidade maior de células NK do que os controles, sugerindo um possível envolvimento destas células na AR. / OBJECTIVES: To assess the profile as well as the absolute number and percentage of true NK cells (CD56+CD16+CD3-), and NK and NKT cells (CD56+) in the peripheral blood of a cohort of patients with rheumatoid arthritis (RA) before and during rituximab (RTX) therapy. METHODS: Ten control patients (blood donors) and ten patients with RA were assessed. The latter group received two intravenous infusions of 1g RTX, separated by a 14 day interval. Immunophenotypic analyses of NK cells were conducted before and after infusion, or until clinical relapse. After six months, respondents and nonrespondents were reassessed according to American Rheumatology Criteria (ARC). RESULTS: The number of true NK cells did not significantly change after treatment with RTX. However, an increase in the percentage of CD56+ cells was observed between the first and second month after RTX infusion. Respondents also displayed a tendency toward an increased number of true NK cells after two months of treatment. At baseline, the number of NK cells was also found to be significantly higher in patients with RA than in control individuals (p<0.05). CONCLUSIONS: Respondents displayed a tendency toward an increase in the absolute number of true NK cells in the second month after RTX infusion. No significant changes in the profile and frequency of NK cells were found between preand post-RTX treatment assessments of patients with RA. However, it was found that patients with RA have a higher number of NK cells than control partcipants, suggesting a possible role of these cells in RA. Artrite reumatóide Células matadoras naturais Cells natural killer Rituximab Rheumatoid arthritis
28	Rituximab som tilläggsbehandling till fludarabin och cyklofosfamid vid kronisk lymfatisk leukemi Fredén, Caroline January 2016 (has links) Kronisk lymfatisk leukemi (KLL) är en hematologisk malignitet som framför allt drabbar äldre personer. KLL går inte att bota men kan behandlas så att sjukdomen går i remission. Patienterna börjar behandlas när sjukdomssymtom förekommer. Det finns flera olika behandlingsalternativ. Vilken behandling som används beror bl.a. på patientens ålder och olika prognostiska faktorer. Syftet med arbetet var att utvärdera effekterna av rituximab som tillägg till fludarabin och cyklofosfamid (R-FC) vid behandling av KLL samt om behandlingen är kostnadseffektiv. Arbetet bestod av en litteraturstudie där fem vetenskapliga studier som hittats via sökningar i databasen PubMed valts ut för att besvara syftet. Av de utvalda studierna var det två randomiserade kliniska studier, två kohortstudier och en hälsoekonomisk studie. Resultaten från studierna visade att tilläggsbehandling med rituximab gav bättre behandlingseffekter både hos obehandlade patienter och hos patienter som behandlats tidigare. Den progressionsfria överlevnaden (PFS) blev signifikant längre med R-FC behandling. Även den totala överlevnaden blev längre och fler patienter uppnådde komplett remission. Studie 3 visade att minimal residual disease (MRD) nivån sänktes mer och hos fler av patienterna som fick R-FC. Låg MRD nivå gav också längre PFS. Studie 4 visade att patienter som hade ett högt uttryck av protein tyrosin kinas 2 (PTK2) genen och behandlades med R-FC hade längre PFS än de som fick FC. Den hälsoekonomiska studien visade att R-FC behandling höjde antalet kvalitetsjusterade levnadsår (QALY) med 1,127, kostnadseffektivitetskvoten (ICER) blev €17979 per QALY och behandlingen var kostnadseffektiv i Tyskland. Tillägg med rituximab gav signifikant bättre behandlingseffekter och är ett bra behandlingsalternativ framför allt hos de lite yngre patienterna som inte är så sjuka, som är jämförbara med patientpopulationen som deltog i studierna, medan det bl.a. beror på betalningsviljan per QALY om R-FC behandling är kostnadseffektiv även i Sverige. Kronisk lymfatisk leukemi KLL rituximab cyklofosfamid fludarabin Pharmaceutical Sciences Farmaceutiska vetenskaper
29	Behandlingseffekt av rituximab jämfört med infliximab vid reumatoid artrit Peterson, Cecilia January 2013 (has links) The aim of this study was to compare the effect between the drugs rituximab and infliximab in rheumatoid arthritis (RA). RA is an autoimmune disease that affects the peripheral joints and is associated with exacerbations. Various immune reactions in the body cause inflammation of the joints which further results in cartilage and bone damage. The diagnosis is made by the classification system "The 2010 American College of Rheumatology (ACR) / European league against rheumatism (EULAR) classification criteria for rheumatoid arthritis", which is an update of the older system called "The 1987 American College of Rheumatology classification criteria for RA". Approximately 0.5-1% of the population is developing the disease, but it varies slightly between different parts of the world. The disease is 2-3 times more common in women and the median age of onset is 60 years. Methotrexate is the first line drug for treatment of RA, but in more severe disease, monoclonal antibodies such as infliximab and rituximab are used. Infliximab and rituximab are only used for combination therapy with methotrexate. Infliximab is a tumor necrosis factor (TNF) α inhibitor, while rituximab inhibits B cells. The method for this work was study of literature. The Pubmed database was used and the following terms were used as keywords: "Rheumathoid Arthritis", "Rheumatoid Arthritis rituximab" and "Rheumatoid Arthritis infliximab." A total of 6 studies were elected, 3 for each drug. When evaluating the results it should be kept in mind that the study approaches vary. The study endpoints were ACR 20, ACR 50, ACR 70 and disease activity score (DAS) 28. Based on these measurements there were no significant difference between the drugs. ACR 20 for infliximab was reached by 50 %, 62.4 % and 59.4 % of the patients, respectively in three different studies. ACR 20 for rituximab was reached by 50.6 %, 51 % and 73 % of the patients in three different studies. The DAS 28 reduction for infliximab was 2.6 and 2.3, while the same numbers for rituximab were 1.6, 1.9 and 2.6. In conclusion, both rituximab and infliximab are good treatment options for severe RA. Because of the small difference between the drugs in the results, other aspects become more important. For example, costs and safety profile should be further investigated. RA reumatoid artrit rituximab infliximab biologiska läkemedel Pharmaceutical Sciences Farmaceutiska vetenskaper
30	Pharmacoépidémiologie de la thrombopénie immunologique en France : suivi de cohorte issue du Système national d'information inter-régimes de l'Assurance maladie et création d'un registre clinique / Pharmacoepidemiology of immune thrombocytopenia in France : follow-up of a cohort built in the French national health insurance database and creation of a clinical registry Moulis, Guillaume 05 January 2016 (has links) La thrombopénie immunologique (TI) est une maladie auto-immune rare. Son épidémiologie est mal connue. Le traitement de la TI aiguë repose sur les corticoïdes et les immunoglobulines. Passée la phase aiguë, plusieurs traitements sont possibles, dont la splénectomie, le rituximab et les agonistes du récepteur à la thrombopoiétine. L'exposition aux traitements de la TI en vie réelle n'a jamais été évaluée, et leur risque infectieux jamais comparé. Des vaccinations sont recommandées avant le rituximab et la splénectomie, mais la couverture vaccinale n'est pas connue. Nous avons constitué deux matériels complémentaires : 1) la cohorte French Adult Immune Thrombocytopenia : a pHarmacoepidemiological study (FAITH) est la cohorte des patients adultes incidents ayant une TI primaire traités de façon persistante (plus de 3 mois), bâtie dans le Système National d'Information Inter-régimes de l'Assurance Maladie (SNIIRAM) au niveau national ; 2) le registre Cytopénie Auto-immune : Registre Midi-PyrénéEN (CARMEN) est une étude observationnelle en vie réelle suivant les patients incidents de TI dans la région Midi-Pyrénées. Grâce à ces deux cohortes, nous avons décrit l'épidémiologie de la TI incidente en France, l'exposition aux traitements et la couverture vaccinale chez l'adulte, et évalué le risque infectieux des traitements et l'effet protecteur des vaccins. / Immune thrombocytopenia (ITP) is a rare autoimmune bleeding disorder. ITP epidemiology is not well known. ITP treatment is based on glucocorticoids, and intravenous polyvalent immunoglobulin in case of severe bleeding. ITP becomes persistent (lasting more than 3 months) or chronic (more than 12 months) in about 70% of adults. In that case, non-corticosteroid treatments are suggested, mostly splenectomy, rituximab and thrombopoietin receptor agonists. The use of these treatments have never been assessed in the real life practice as well as their effectiveness and safety, particularly as regards the risk of infection. Vaccinations are recommended before splenectomy or rituximab. However, the vaccination rates and their effectiveness has not been assessed. We build two complementary materials: 1) the French Adult Immune Thrombocytopenia: a pHarmacoepidemiological study (FAITH) is the cohort of all incident primary ITP adults persistently treated (more than 3 months), built in the French health Insurance system database (Système national d'information inter-régimes de l'Assurance Maladie, SNIIRAM) at the national level; 2) the Cytopénie Auto-immune : Registre Midi-PyrénéEN (CARMEN) registry that includes and follows all incident ITP adults in the French Midi-Pyrénées region. Thanks to these two cohorts, we could assess the epidemiology of incident ITP in France; describe the exposure ITP treatments; assess the vaccination coverage in rituximab treated and splenectomized patients in France; and assess the risk of infection according to ITP treatments and the protective effect of the vaccines in this population. Thrombopénie immunologique Pharmacoépidémiologie Epidémiologie Rituximab Splénectomie Infection Vaccin

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