Global ETD Search

141	Étude de substances bioactives issues de la flore amazonienne : analyse de préparations phytothérapeutiques à base de Quassia amara L (simaroubacae) et Psidium acutangulum DC (Myrtaceae) utilisées en Guyane française pour une indication antipaludique : identification et analyse métabolomique d'huiles essentielles à activité antifongique Houël, Emeline 01 July 2011 (has links) L’objectif du travail effectué était la recherche de nouvelles substances actives d’origine végétale, présentant soit une activité antiplasmodiale soit une activité antifongique. Cette étude a été menée suivant deux stratégies différentes: l’étude de remèdes traditionnels antipaludiques identifiés suite à des enquêtes ethnopharmacologiques, et la mise en évidence des propriétés antifongiques d’huiles essentielles grâce à une stratégie bioinspirée. La première partie du travail a permis de mettre en évidence le rôle d’un quassinoïde connu, la simalikalactone D, dans l’activité antipaludique d’une tisane de jeunes feuilles fraîches de Quassia amara L. (Simaroubaceae). Dans le cas de la décoction de rameaux de Psidium acutangulum DC. (Myrtaceae), c’est cette fois un mélange de flavonoïdes glycosylés qui est responsable de l’activité du remède. Dans le cadre de la recherche de nouvelles substances antifongiques, le criblage effectué a permis d’identifier de nombreuses huiles essentielles présentant des activités intéressantes, validant ainsi la démarche bioinspirée retenue dans ce cas. L’huile essentielle d’Otacanthus azureus (Linden) Ronse a en particulier démontré une activité remarquable, à la fois seule et en combinaison avec des antifongiques azolés. Enfin, l’étude métabolomique de la composition des huiles essentielles a permis de mettre au point un outil pouvant orienter la sélection des huiles en fonction des données obtenues en GC/MS dans l’optique de la recherche de nouvelles substances antifongiques. Ce travail démontre donc la validité des stratégies retenues – ethnopharmacologie et bioinspiration – dans la recherche de nouvelles substances bioactives. / The aim of this work was to search for new bioactive compounds, displaying either antiplasmodial or antifungal activity. Two strategies were developed here: the evaluation of traditional remedies identified as antimalarial through ethnopharmacological studies, and the search for antifungal essential oils, the criterium being here a bioinspired approach. Our work led to the discovery that the antimalarial activity of Quassia amara L. (Simaroubaceae) fresh young leaves was due to the presence of a known quassinoid, simalikalactone D. In the case of Psidium acutangulum DC. (Myrtaceae), a flavonol glycosides mixture explained the activity observed for the decoction. The search for antifungal essential oils from the Amazonian flora led to the identification of several interesting species, thus validating our bioinspired strategy. The essential oil of Otacanthus azureus (Linden) Ronse was among the most active ones, either alone or in combination with azole drugs. Eventually, a metabolomic study of the GC/MS composition of these oils allowed us to develop a statistical tool which could help to select interesting antifungal products. This work thus demonstrates the major interest of the two strategies – ethnopharmacology and bioinspiration – for the search of new bioactive compounds. Chimie des substances personnelles Paludisme Mycoses Dermatophytes Levures Remèdes traditionnels Métabolomique Plasmodium falciparum Quassia amara L. Psidium actutangulum DC. Otacanthus azureus (Linden) Ronse Natural substances chemistry Malaria Mycoses Dermatophytes Yeasts Traditional remedies Metabolomics Plasmodium falciparum Quassia amara L. Psidium actutangulum DC. Otacanthus azureus (Linden) Ronse 547 572
142	Asiatic Cholera in Kentucky 1832 to 1873 Baird, Nancy 01 May 1972 (has links) Asiatic cholera has been called the scourge of the nineteenth century, for it caused the untimely death of millions throughout the world. During its four visits to the United States, unknown thousands of Kentuckians fell victims to the disease. In attempting to prevent the dreaded scourge, Kentuckians became more conscious of the need for cleaner cities, pure water and adequate sewage disposal. Modern waterworks facilities, sewage treatment and disposal facilities have provided the means by which the United States has conquered this scourge of the nineteenth century, for with these facilities cholera is the easiest of all communicable diseases to prevent. But, as with the eradication of any disease, constant vigilance and continued use of modern scientific knowledge are necessary to prevent its return. The disease is presently ravaging India and the Far East, and with modern jet travel it could bypass quarantine stations and enter the United States undetected. The “seeds” of the pestilence could be sown across the nation within a few hours. The only safeguard is modern sanitation facilities, for no permanent inoculation or miraculous cure has been developed. Today many rural areas of Kentucky and other states use wells and old cisterns that are, or could easily become, contaminated by human fecal matter. A fifth visit from cholera should not be necessary to correct the ignorance and complacent attitudes concerning inadequate sanitation facilities that exist in these areas of the nation. This study attempts to show the horrors of cholera’s four visits to Kentucky, and how the fear of the disease stimulated interest in public health. Western Kentucky University Epidemics Diseases Arts and Humanities Bacterial Infections and Mycoses Diseases History Medicine and Health Sciences Public History Social and Behavioral Sciences Social History United States History
143	Efeito da depleção in vivo de leucócitos PMN em camundongos resistentes e susceptíveis à Paracoccidioidomicose pulmonar / Effect of in vivo depletion of PMN leukocytes in mice resistant to and susceptible to pulmonary Paracoccidioidomycosis Pina, Adriana 05 April 2002 (has links) Estudos em nosso laboratório caracterizaram camundongos B10.A como susceptíveis e camundongos A/J como resistentes à infecção pulmonar pelo P. brasiliensis. Para investigar o papel das células PMN na paracoccidioidomicose (PCM) pulmonar, camundongos B10.A e A/J foram depletados destas células através da inoculação in vivo por via intraperitoneal (i.p.) do anticorpo monoclonal anti-células PMN e infectados pela via intratraqueal (i.t.) com um milhão de leveduras viáveis. Camundongos-controle receberam doses equivalentes de IgG normal de rato. A depleção de granulócitos diminuiu o tempo de sobrevida dos animais B10.A, mas não dos animais A/J. Quando comparados com os animais não depletados, camundongos resistentes apresentaram aumento da carga fúngica no pulmão somente no dia 7 pós-infecção. Ao contrário, camundongos susceptíveis depletados de PMN apresentaram números mais elevados de células leveduriformes no pulmão, fígado e baço nos dias 7, 15, 30 e 120 pós-infecção, com relação aos seus grupos-controle tratados com IgG. A depleção dos granulócitos, entretanto, não alterou as reações de hipersensibilidade do tipo tardio (HTT) desenvolvidas por ambas as linhagens de animais. Considerando a resposta imune humoral, a depleção de células PMN levou à maior produção de anticorpos específicos em animais B10.A (Ig Total, IgG1, IgA e IgG3) e em animais A/J (Ig Total, IgG2a, IgG2b e IgG3). A depleção também alterou o padrão de citocinas pulmonares. Nos animais B10.A-tratados foram encontradas concentrações mais elevadas de IL-12 aos 15 dias e de IL-4 aos 120 dias pós-infecção, em comparação aos animais controle. Níveis de IL-12 significativamente mais altos foram detectados no grupo de animais A/J-depletados aos 7 e 120 dias e o IFN-γ foi detectado em níveis mais elevados em todo o curso da doença. Então, a depleção de PMN induz níveis mais altos de anticorpos e um ambiente mais pró-inflamatório no local da infecção. De acordo com esses dados, pudemos verificar que os neutrófilos são células importantes na defesa do hospedeiro à infecção pelo P.brasiliensis. Entretanto, o efeito protetor desta população celular depende do patrimônio genético do hospedeiro e é mais marcante na linhagem susceptível de camundongos. Neste trabalho também investigamos o efeito da depleção in vivo de leucócitos PMN na imunidade adquirida e protetora desenvolvida pela pré-imunização de animais B10.A. Assim, os camundongos foram previamente imunizados pela via s.c., depletados ou não de células PMN e desafiados i.t. com 1 milhão de células leveduriformes. Não foram detectadas diferenças significativas na contagem de fungos viáveis do pulmão, fígado e baço, entre os grupos imunizados tratados ou não com o AcM anti-PMN. A depleção não alterou a produção de anticorpos específicos, porém aumentou significativamente a síntese de IL-3, bem como a reatividade de HTT. Portanto, nossos resultados mostraram que, diferentemente da imunidade natural, os leucócitos PMN não exercem um papel protetor na fase adquirida da resposta imune à infecção com o P.brasiliensis. / Previous studies in our laboratory defined susceptible (B10.A) and resistant (A/J) mice to pulmonary P.brasiliensis infection. To investigate the role of PMN cells in pulmonary PCM, resistant and susceptible mice were depleted in vivo of these cells by intraperitoneal (i.p.) injection of a granulocyte-depleting monoclonal antibody and infected intratracheally (i.t) with one million yeast cells. Control mice received equivalent doses of normal rat IgG. PMN depletion decreased survival times of B10.A, but not of A/J infected mice. When compared with the non-depleted counterparts, resistant mice presented increased fungal loads in the lung only at day 7 after infection. On the contrary, PMN-depleted susceptible mice presented higher number of yeast cells in the lung, liver and spleen at days 7, 15, 30 and 120 after infection than their IgG-treated controls. PMN cells depletion, however, did not alter the DTH reaction developed by both mouse strains. Regarding humoral immune response, PMN cells depletion caused increased production of specific antibodies in B10.A (Total Ig, IgG1, IgA and IgG3) and A/J (Total Ig, IgG2a, IgG2b and IgG3) mice. Levels of pulmonary cytokines were also altered after PMN depletion. B10.A-treated mice presented increased levels of IL-12 and IL-4 at days 15 and 120 post-infection, respective/y. In A/J-depleted mice, augmented levels of IL-12 were detected at days 7 and 120 after infection; IFN-γ, however, was produced in higher levels during whole course of infection. Thus, PMN depletion induces higher levels of specific antibodies and enhanced pro-inflammatory milieu at the site of infection. As a whole, our data on PMN depletion at the onset of infection showed that neutrophils are important cells in host defense to P.brasiliensis infection. However, the effect of PMN depletion depends on the genetic background of the host and has a more pronounced effect in the susceptible strain of mice. We have also assessed the effect of in vivo depletion of the leukocytes on the acquired phase of immunity developed by B10.A mice previously immunized by the subcutaneous (s.c.) route were depleted or not of PMN cells and challenged i.t. with one million yeast cells. No differences were detected in the CFU counts in the lung, liver and spleen between untreated and PMN depleted vaccinated mice. PMN depletion also did not alter the production of specific antibodies but enhanced IL-3 synthesis as well as DTH reactivity. In conclusion, our results showed that, differently from natural immunity, PMN cells do not play a protective role in the acquired phase of immune response to P.brasiliensis infection. Bacterial infections and mycoses Camundongos Clinical immunology Fungi Fungo Hematologia Hematology Immunity Imunidade Imunologia clínica Infecções bacterianas e micoses Mice Paracoccidioidomicose Paracoccidioidomycosis Polimorfonuclear neutrófilo Polymorphonuclear neutrophil
144	Infecções fúngicas invasivas em pacientes com lúpus eritematoso sistêmico juvenil / Invasive fungal infections in juvenile systemic lupus erythematosus patients Silva, Marco Felipe Castro da 31 August 2015 (has links) Introdução: As infecções são importantes causas de morbidade e mortalidade em pacientes com lúpus eritematoso sistêmico juvenil (LESJ). No entanto, estudos avaliando somente infecções fúngicas invasivas (IFI) em pacientes com LESJ são restritos a relatos de casos ou série de casos, sem qualquer avaliação sistemática dos possíveis fatores de risco ou desfechos associados. A escassez de dados referentes às IFI em pacientes com LESJ e seu impacto sobre as características da doença em uma grande população levou ao desenvolvimento deste estudo multicêntrico. Objetivos: Estudar a prevalência, fatores de risco e mortalidade de IFI em pacientes com LESJ. Método: Um estudo de coorte multicêntrico retrospectivo foi realizado com 852 pacientes com LESJ de 10 Serviços de Reumatologia Pediátrica do Estado de São Paulo. Uma reunião foi realizada e todos os pesquisadores foram treinados para o preenchimento do banco de dados. As IFI foram diagnosticadas de acordo com as definições revisadas pelo grupo de consenso EORTC/MSG (comprovadas, prováveis ou possíveis). Foram coletados dados acerca de dados demográficos, características clínico-laboratoriais, atividade da doença (SLEDAI-2K), dano cumulativo (SLICC/ACR-DI) e tratamento, além de características e complicações das IFI. Resultados: IFI foram diagnosticadas em 33/852 (3,9%) pacientes com LESJ. IFI comprovadas foram diagnosticadas em 22 pacientes, IFI prováveis em 5 e IFI possíveis em 6. Os tipos de IFI encontradas foram: candidíase em 20 pacientes, aspergilose em 9, criptococose em 2, histoplasmose disseminada em um e paracoccidioidomicose em um. A mediana de duração da doença foi menor (1,0 vs. 4,7 anos, p < 0,0001), com maiores escores de SLEDAI-2K atual [19,5 (0-44) vs. 2 (0-45), p < 0,0001] e dose atual de prednisona [50 (10-60) vs. 10 (2-90) mg/dia, p < 0,0001] em pacientes com IFI em comparação com os pacientes sem IFI. A frequência de óbito foi maior no grupo com IFI (51% vs. 6%, p < 0,0001). A análise de regressão logística revelou que SLEDAI-2K atual (OR=1,108, IC 95%=1,057- 1,163, p < 0,0001), dose atual de prednisona (OR=1,046, IC 95%=1,021-1,071; p < 0,0001) e duração da doença (OR=0,984, IC 95%=0,969-0,998, p=0,030) foram fatores de risco independentes para IFI (R2 Nagelkerke 0,425). Conclusão: Este foi o primeiro estudo que caracterizou IFI em pacientes com LESJ. Identificou-se que a atividade da doença e uso de glicocorticoides foram os principais fatores de risco para estas infecções potencialmente graves, principalmente nos primeiros anos de curso da doença e com uma elevada taxa mortalidade / Introduction: Infections are an important cause of morbidity and mortality in childhoodonset systemic lupus erythematosus (cSLE) patients. However, studies evaluating solely invasive fungal infections (IFI) in cSLE patients are restricted to case reports or case series without any systematic evaluation of the possible associated risk factors and outcome in pediatric lupus population. The scarcity of data regarding IFI in cSLE patients and its impact on disease characteristics in a large population led to the development of this multicenter study. Objective: To study the prevalence, risk factors and mortality of IFI in cSLE patients. Methods: A retrospective multicenter cohort study was performed in 852 cSLE patients from 10 Pediatric Rheumatology services. An investigator meeting was held and all participants received database training. IFI were diagnosed according to EORTC/MSG Consensus Group criteria (proven, probable and possible). Demographic data, clinical, laboratorial, disease activity (SLEDAI-2K), cumulative damage (SLICC/ACR-DI) and treatment were collected. IFI were characterized and its outcome were also evaluated. Results: IFI were observed in 33/852 (3.9%) cSLE patients. Proven IFI was diagnosed in 22 cSLE patients, probable IFI in 5 and possible IFI in 6. Types of IFI were: 20 candidiasis, 9 aspergillosis, 2 cryptococcosis, one disseminated histoplasmosis and one paracoccidioidomycosis. The median of disease duration was lower (1.0 vs. 4.7 years, p < 0.0001), with a higher current SLEDAI-2K [19.5 (0-44) vs. 2 (0-45), p < 0.0001] and current prednisone dose [50 (10-60) vs. 10 (2-90) mg/day, p < 0.0001] in patients with IFI compared to those without IFI. The frequency of death was higher in the former group (51% vs. 6%, p < 0.0001). Logistic regression analysis revealed that current SLEDAI-2K (OR=1.108; 95%CI=1.057-1.163; p < 0.0001), prednisone current dose (OR=1.046; 95%CI=1.021-1.071; p < 0.0001) and disease duration (OR=0.984; 95%CI=0.969-0.998; p=0.03) were independent risk factors for IFI (R2 Nagelkerke 0.425). Conclusion: This was the first study that characterized IFI in cSLE patients. We identified that disease activity and glucocorticoid use were the main risk factors for these life-threatening infections, mainly in the first years of disease course and with a high rate of fatal outcome Aspergillosis Aspergilose Candidíase Candidiasis Child Clinical trial Cohort studies Criança Criptococose Cryptococcosis Ensaio clínico Estudos de coortes Glicocorticoides Glucocorticoids Histoplasmose Histoplasmosis, Paracoccidioidomycosis Infecção Infection Lúpus eritematoso sistêmico Micoses Mycoses Paracoccidioidomicose Prednisona Prednisone Systemic lupus erythematosus
145	Efeito da depleção in vivo de leucócitos PMN em camundongos resistentes e susceptíveis à Paracoccidioidomicose pulmonar / Effect of in vivo depletion of PMN leukocytes in mice resistant to and susceptible to pulmonary Paracoccidioidomycosis Adriana Pina 05 April 2002 (has links) Estudos em nosso laboratório caracterizaram camundongos B10.A como susceptíveis e camundongos A/J como resistentes à infecção pulmonar pelo P. brasiliensis. Para investigar o papel das células PMN na paracoccidioidomicose (PCM) pulmonar, camundongos B10.A e A/J foram depletados destas células através da inoculação in vivo por via intraperitoneal (i.p.) do anticorpo monoclonal anti-células PMN e infectados pela via intratraqueal (i.t.) com um milhão de leveduras viáveis. Camundongos-controle receberam doses equivalentes de IgG normal de rato. A depleção de granulócitos diminuiu o tempo de sobrevida dos animais B10.A, mas não dos animais A/J. Quando comparados com os animais não depletados, camundongos resistentes apresentaram aumento da carga fúngica no pulmão somente no dia 7 pós-infecção. Ao contrário, camundongos susceptíveis depletados de PMN apresentaram números mais elevados de células leveduriformes no pulmão, fígado e baço nos dias 7, 15, 30 e 120 pós-infecção, com relação aos seus grupos-controle tratados com IgG. A depleção dos granulócitos, entretanto, não alterou as reações de hipersensibilidade do tipo tardio (HTT) desenvolvidas por ambas as linhagens de animais. Considerando a resposta imune humoral, a depleção de células PMN levou à maior produção de anticorpos específicos em animais B10.A (Ig Total, IgG1, IgA e IgG3) e em animais A/J (Ig Total, IgG2a, IgG2b e IgG3). A depleção também alterou o padrão de citocinas pulmonares. Nos animais B10.A-tratados foram encontradas concentrações mais elevadas de IL-12 aos 15 dias e de IL-4 aos 120 dias pós-infecção, em comparação aos animais controle. Níveis de IL-12 significativamente mais altos foram detectados no grupo de animais A/J-depletados aos 7 e 120 dias e o IFN-γ foi detectado em níveis mais elevados em todo o curso da doença. Então, a depleção de PMN induz níveis mais altos de anticorpos e um ambiente mais pró-inflamatório no local da infecção. De acordo com esses dados, pudemos verificar que os neutrófilos são células importantes na defesa do hospedeiro à infecção pelo P.brasiliensis. Entretanto, o efeito protetor desta população celular depende do patrimônio genético do hospedeiro e é mais marcante na linhagem susceptível de camundongos. Neste trabalho também investigamos o efeito da depleção in vivo de leucócitos PMN na imunidade adquirida e protetora desenvolvida pela pré-imunização de animais B10.A. Assim, os camundongos foram previamente imunizados pela via s.c., depletados ou não de células PMN e desafiados i.t. com 1 milhão de células leveduriformes. Não foram detectadas diferenças significativas na contagem de fungos viáveis do pulmão, fígado e baço, entre os grupos imunizados tratados ou não com o AcM anti-PMN. A depleção não alterou a produção de anticorpos específicos, porém aumentou significativamente a síntese de IL-3, bem como a reatividade de HTT. Portanto, nossos resultados mostraram que, diferentemente da imunidade natural, os leucócitos PMN não exercem um papel protetor na fase adquirida da resposta imune à infecção com o P.brasiliensis. / Previous studies in our laboratory defined susceptible (B10.A) and resistant (A/J) mice to pulmonary P.brasiliensis infection. To investigate the role of PMN cells in pulmonary PCM, resistant and susceptible mice were depleted in vivo of these cells by intraperitoneal (i.p.) injection of a granulocyte-depleting monoclonal antibody and infected intratracheally (i.t) with one million yeast cells. Control mice received equivalent doses of normal rat IgG. PMN depletion decreased survival times of B10.A, but not of A/J infected mice. When compared with the non-depleted counterparts, resistant mice presented increased fungal loads in the lung only at day 7 after infection. On the contrary, PMN-depleted susceptible mice presented higher number of yeast cells in the lung, liver and spleen at days 7, 15, 30 and 120 after infection than their IgG-treated controls. PMN cells depletion, however, did not alter the DTH reaction developed by both mouse strains. Regarding humoral immune response, PMN cells depletion caused increased production of specific antibodies in B10.A (Total Ig, IgG1, IgA and IgG3) and A/J (Total Ig, IgG2a, IgG2b and IgG3) mice. Levels of pulmonary cytokines were also altered after PMN depletion. B10.A-treated mice presented increased levels of IL-12 and IL-4 at days 15 and 120 post-infection, respective/y. In A/J-depleted mice, augmented levels of IL-12 were detected at days 7 and 120 after infection; IFN-γ, however, was produced in higher levels during whole course of infection. Thus, PMN depletion induces higher levels of specific antibodies and enhanced pro-inflammatory milieu at the site of infection. As a whole, our data on PMN depletion at the onset of infection showed that neutrophils are important cells in host defense to P.brasiliensis infection. However, the effect of PMN depletion depends on the genetic background of the host and has a more pronounced effect in the susceptible strain of mice. We have also assessed the effect of in vivo depletion of the leukocytes on the acquired phase of immunity developed by B10.A mice previously immunized by the subcutaneous (s.c.) route were depleted or not of PMN cells and challenged i.t. with one million yeast cells. No differences were detected in the CFU counts in the lung, liver and spleen between untreated and PMN depleted vaccinated mice. PMN depletion also did not alter the production of specific antibodies but enhanced IL-3 synthesis as well as DTH reactivity. In conclusion, our results showed that, differently from natural immunity, PMN cells do not play a protective role in the acquired phase of immune response to P.brasiliensis infection. Camundongos Fungo Hematologia Imunidade Imunologia clínica Infecções bacterianas e micoses Paracoccidioidomicose Polimorfonuclear neutrófilo Bacterial infections and mycoses Clinical immunology Fungi Hematology Immunity Mice Paracoccidioidomycosis Polymorphonuclear neutrophil
146	Infecções fúngicas invasivas em pacientes com lúpus eritematoso sistêmico juvenil / Invasive fungal infections in juvenile systemic lupus erythematosus patients Marco Felipe Castro da Silva 31 August 2015 (has links) Introdução: As infecções são importantes causas de morbidade e mortalidade em pacientes com lúpus eritematoso sistêmico juvenil (LESJ). No entanto, estudos avaliando somente infecções fúngicas invasivas (IFI) em pacientes com LESJ são restritos a relatos de casos ou série de casos, sem qualquer avaliação sistemática dos possíveis fatores de risco ou desfechos associados. A escassez de dados referentes às IFI em pacientes com LESJ e seu impacto sobre as características da doença em uma grande população levou ao desenvolvimento deste estudo multicêntrico. Objetivos: Estudar a prevalência, fatores de risco e mortalidade de IFI em pacientes com LESJ. Método: Um estudo de coorte multicêntrico retrospectivo foi realizado com 852 pacientes com LESJ de 10 Serviços de Reumatologia Pediátrica do Estado de São Paulo. Uma reunião foi realizada e todos os pesquisadores foram treinados para o preenchimento do banco de dados. As IFI foram diagnosticadas de acordo com as definições revisadas pelo grupo de consenso EORTC/MSG (comprovadas, prováveis ou possíveis). Foram coletados dados acerca de dados demográficos, características clínico-laboratoriais, atividade da doença (SLEDAI-2K), dano cumulativo (SLICC/ACR-DI) e tratamento, além de características e complicações das IFI. Resultados: IFI foram diagnosticadas em 33/852 (3,9%) pacientes com LESJ. IFI comprovadas foram diagnosticadas em 22 pacientes, IFI prováveis em 5 e IFI possíveis em 6. Os tipos de IFI encontradas foram: candidíase em 20 pacientes, aspergilose em 9, criptococose em 2, histoplasmose disseminada em um e paracoccidioidomicose em um. A mediana de duração da doença foi menor (1,0 vs. 4,7 anos, p < 0,0001), com maiores escores de SLEDAI-2K atual [19,5 (0-44) vs. 2 (0-45), p < 0,0001] e dose atual de prednisona [50 (10-60) vs. 10 (2-90) mg/dia, p < 0,0001] em pacientes com IFI em comparação com os pacientes sem IFI. A frequência de óbito foi maior no grupo com IFI (51% vs. 6%, p < 0,0001). A análise de regressão logística revelou que SLEDAI-2K atual (OR=1,108, IC 95%=1,057- 1,163, p < 0,0001), dose atual de prednisona (OR=1,046, IC 95%=1,021-1,071; p < 0,0001) e duração da doença (OR=0,984, IC 95%=0,969-0,998, p=0,030) foram fatores de risco independentes para IFI (R2 Nagelkerke 0,425). Conclusão: Este foi o primeiro estudo que caracterizou IFI em pacientes com LESJ. Identificou-se que a atividade da doença e uso de glicocorticoides foram os principais fatores de risco para estas infecções potencialmente graves, principalmente nos primeiros anos de curso da doença e com uma elevada taxa mortalidade / Introduction: Infections are an important cause of morbidity and mortality in childhoodonset systemic lupus erythematosus (cSLE) patients. However, studies evaluating solely invasive fungal infections (IFI) in cSLE patients are restricted to case reports or case series without any systematic evaluation of the possible associated risk factors and outcome in pediatric lupus population. The scarcity of data regarding IFI in cSLE patients and its impact on disease characteristics in a large population led to the development of this multicenter study. Objective: To study the prevalence, risk factors and mortality of IFI in cSLE patients. Methods: A retrospective multicenter cohort study was performed in 852 cSLE patients from 10 Pediatric Rheumatology services. An investigator meeting was held and all participants received database training. IFI were diagnosed according to EORTC/MSG Consensus Group criteria (proven, probable and possible). Demographic data, clinical, laboratorial, disease activity (SLEDAI-2K), cumulative damage (SLICC/ACR-DI) and treatment were collected. IFI were characterized and its outcome were also evaluated. Results: IFI were observed in 33/852 (3.9%) cSLE patients. Proven IFI was diagnosed in 22 cSLE patients, probable IFI in 5 and possible IFI in 6. Types of IFI were: 20 candidiasis, 9 aspergillosis, 2 cryptococcosis, one disseminated histoplasmosis and one paracoccidioidomycosis. The median of disease duration was lower (1.0 vs. 4.7 years, p < 0.0001), with a higher current SLEDAI-2K [19.5 (0-44) vs. 2 (0-45), p < 0.0001] and current prednisone dose [50 (10-60) vs. 10 (2-90) mg/day, p < 0.0001] in patients with IFI compared to those without IFI. The frequency of death was higher in the former group (51% vs. 6%, p < 0.0001). Logistic regression analysis revealed that current SLEDAI-2K (OR=1.108; 95%CI=1.057-1.163; p < 0.0001), prednisone current dose (OR=1.046; 95%CI=1.021-1.071; p < 0.0001) and disease duration (OR=0.984; 95%CI=0.969-0.998; p=0.03) were independent risk factors for IFI (R2 Nagelkerke 0.425). Conclusion: This was the first study that characterized IFI in cSLE patients. We identified that disease activity and glucocorticoid use were the main risk factors for these life-threatening infections, mainly in the first years of disease course and with a high rate of fatal outcome Aspergilose Candidíase Criança Criptococose Ensaio clínico Estudos de coortes Glicocorticoides Histoplasmose Infecção Lúpus eritematoso sistêmico Micoses Paracoccidioidomicose Prednisona Aspergillosis Candidiasis Child Clinical trial Cohort studies Cryptococcosis Glucocorticoids Histoplasmosis, Paracoccidioidomycosis Infection Mycoses Prednisone Systemic lupus erythematosus
147	ChAT Expression in Chlamydia muridarum-infected Female Murine Genital Tract Sartain, Hallie 01 May 2017 (has links) Chlamydia trachomatis is the most prevalent agent of bacterial sexually transmitted infections in the world. However, a profuse number of cases are unreported, as the infection is often asymptomatic. Sequelae such as pelvic inflammatory disease, an increased risk of cervical cancer, premature birth, and perinatal infections in pregnant women can occur. Inflammation occurs in the body in response to infection or injury. Although inflammation can lead to some unwanted secondary effects, such as pain, it serves to return the body to homeostasis by restoring injured tissues and eliminating pathogens. One recently identified connection between the central nervous system and the immune system that regulates inflammation is the cholinergic anti-inflammatory pathway (CAP). In the CAP, pathogen-associated molecular patterns stimulate the vagus nerve to activate the pathway, which ultimately results in acetylcholine (ACh) release, which down regulates inflammation. We hypothesized that genital chlamydial infection would increase the expression of choline acetyltransferase (ChAT), the enzyme that synthesizes ACh, in the female murine genital tract, therefore down regulating inflammation and promoting chlamydial infection. Transgenic female mice carrying a ChAT-promoter driven GFP reporter gene were vaginally infected with C. muridarum. Mice were sacrificed on days 3, 9, 15, and 21 post infection; cervical, uterine horn, and ovarian tissues were removed and embedded in paraffin. Small sections of each tissue were cut and mounted onto slides. The tissue sections were then stained for the expression of ChAT using immunohistochemical techniques. Finally, tissue sections were viewed under a microscope for positive staining and the data was analyzed. The results indicated that there is a significant increase in the number of cells that express ChAT in genital tract of chlamydia-infected mice versus non-infected mice. cholinergic acetylcholine anti-inflammatory pathway chlamydia Bacteria Bacterial Infections and Mycoses Enzymes and Coenzymes Infectious Disease Medical Microbiology Obstetrics and Gynecology Pathology Urogenital System
148	Epidemiologie und Empfindlichkeit von Pilzisolaten gegenüber sechs Antimykotika aus primär sterilen Materialien in Deutschland / Epidemiology and susceptibility of fungal isolates to six antifungals from primarily sterile sites in Germany Kunz, Luisa 20 August 2012 (has links) No description available. 610 Medizin, Gesundheit MED 333 Medicine Candida Empfindlichkeit Resistenz Etest Mikrodilution Hefen Caspofungin Fluconazol Itraconazol Voriconazol Amphotericin B 5-Fluorcytosin Epidemiologie NRZSM Mykose candida susceptibility resistance Etest microdilution yeasts caspofungin fluconazole itraconazole voriconazole amphotericin B flucytosine epidemiology NRZSM mycoses 44
149	ETUDE DE SUBSTANCES BIOACTIVES ISSUES DE LA FLORE AMAZONIENNE Analyse de préparations phytothérapeutiques à base de Quassia amara L. (Simaroubaceae) et de Psidium acutangulum DC. (Myrtaceae) utilisées en Guyane française pour une indication antipaludique. Identification et analyse métabolomique d'huiles essentielles à activité antifongique. Houël, Emeline 01 July 2011 (has links) (PDF) L'objectif du travail effectué était la recherche de nouvelles substances actives d'origine végétale, présentant soit une activité antiplasmodiale soit une activité antifongique. Cette étude a été menée suivant deux stratégies différentes: l'étude de remèdes traditionnels antipaludiques identifiés suite à des enquêtes ethnopharmacologiques, et la mise en évidence des propriétés antifongiques d'huiles essentielles grâce à une stratégie bioinspirée. La première partie du travail a permis de mettre en évidence le rôle d'un quassinoïde connu, la simalikalactone D, dans l'activité antipaludique d'une tisane de jeunes feuilles fraîches de Quassia amara L. (Simaroubaceae). Dans le cas de la décoction de rameaux de Psidium acutangulum DC. (Myrtaceae), c'est cette fois un mélange de flavonoïdes glycosylés qui est responsable de l'activité du remède. Dans le cadre de la recherche de nouvelles substances antifongiques, le criblage effectué a permis d'identifier de nombreuses huiles essentielles présentant des activités intéressantes, validant ainsi la démarche bioinspirée retenue dans ce cas. L'huile essentielle d'Otacanthus azureus (Linden) Ronse a en particulier démontré une activité remarquable, à la fois seule et en combinaison avec des antifongiques azolés. Enfin, l'étude métabolomique de la composition des huiles essentielles a permis de mettre au point un outil pouvant orienter la sélection des huiles en fonction des données obtenues en GC/MS dans l'optique de la recherche de nouvelles substances antifongiques. Ce travail démontre donc la validité des stratégies retenues - ethnopharmacologie et bioinspiration - dans la recherche de nouvelles substances bioactives. [CHIM:THER] Chimie/Chimie thérapeutique Chimie des substances naturelles paludisme mycoses dermatophytes levures remèdes traditionnels métabolomique Plasmodium falciparum Quassia amara L Psidium actutangulum DC Otacanthus azureus (Linden) Ronse
150	Maternally Derived Anti-Dengue Antibodies and Risk of DHF in Infants: A Case-Control Study Hatch, Steven 01 August 2010 (has links) This study proposes to directly test the hypothesis that antibody-dependent enhancement (ADE) is the critical factor in the development of dengue hemorrhagic fever (DHF) in infants. DHF occurs in two distinct clinical settings: a) in children and adults with secondary DENV infection, and b) in infants with primary DENV infection born to mothers with prior DENV infection. The ADE hypothesis proposes that pre-existing serotype-cross-reactive non-neutralizing anti-DENV antibodies bind the heterotypic DENV during secondary infection and enhance its uptake into immune cells, leading to increased viral load and DHF. This model suggests that DHF in DENV-infected infants is caused by the enhancing effect of waning maternal anti-DENV antibodies, thus causing a “physiologic secondary infection” during an infant’s primary infection and thereby increasing the infant’s risk for DHF. The effect of maternal immunity on DHF in infants has been studied exclusively in Southeast Asia. However, the maternal DENV seroprevalence approaches 100% in this part of the world. As a consequence, the ADE model of infant DHF cannot truly be tested in Southeast Asia, because all infants possess anti-DENV antibody at birth. In the Western Hemisphere, by contrast, women may have experienced either a single DENV infection, more than one DENV infection, or no DENV infection at all. The ability to include DENV-seronegative mothers as controls allows for the ADE hypothesis to be directly tested in a clinical study. To our knowledge, no such study has been previously conducted. This thesis presents a case-control study designed to evaluate the influence of positive maternal dengue seroprevalence on the risk of DHF in infants. As the MSCI program provides instruction in study design, this thesis does not present findings. The clinical trial described herein began in May 2010 and enrollment is expected to continue through May 2012 (see Table 4). Dengue Dengue Hemorrhagic Fever Seroepidemiologic Studies Infectious Disease Transmission Vertical Infant Bacterial Infections and Mycoses Environmental Public Health Immunology and Infectious Disease Infectious Disease Investigative Techniques Life Sciences Maternal and Child Health Medicine and Health Sciences Virus Diseases

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