Global ETD Search

91	Therapeutic immunomodulation of allergic lung disease using regulatory dendritic cells in a mouse model of asthma Nayyar, Aarti 24 February 2009 (has links) We report herein that IL-10-treated dendritic cells (DC) can be used effectively to reverse established severe asthma-like disease in a mouse model. Our lab had shown previously that allergen-presenting splenic CD8¦Á+ DCs could ¡Ö50% reduce airway hyper responsiveness (AHR), eosinophilia, and Th2 responses in asthma-phenotype mice, but only marginally reduce IgE/IgG1 levels. We now show that bone marrow-derived DCs that have been differentiated in the presence of IL-10 (DCIL-10) are effective in reversing the asthma phenotype. Co-culture of DCIL-10 with T memory (TM) cells from asthma-phenotype mice was associated with lack of Th2 responses, and this was partially reversed by IL-2. Immunostimulatory DC activated these Th2 cells. <i>In vivo</i>, delivery of allergen-pulsed DCIL-10, either into the airway or intraperitoneally abrogated AHR from weeks 3-10 post-treatment, and ameliorated lung eosinophilia and Th2 (IL-4, -5, -9, & -13, IgE) responses, as well as circulating allergen-specific IgE responses for at least 32 weeks following treatment. Repeated OVADCIL-10 treatments kept AHR normalized for 8 weeks as well as Th2 responses significantly low. In vivo, delivery of anti-IL-10R, but not anti-TGF-¦Â from day 12-21 after treatment had moderate effects on DCIL-10-driven tolerance, but 1-methyl tryptophan (inhibitor of indoleamine-2,3-dioxygenase) treatment had significant effects on Th2 responses. The mechanisms mediating tolerance in vivo are likely complex, but we speculate that infectious tolerance sustains this regulatory activity during the 32-week period in which we have observed tolerance to be in place. Immunomodulation Th2 responses Airway Hyperresponsiveness Asthma Dendritic cells regulatory T cells Interleukin-10
92	Prenatal Stress, Depression, and Herpes Viral Titers Hsu, Pao-Chu 01 January 2013 (has links) Recent studies suggest that some cases of prenatal depression may be associated with reactivation of latent infections of the herpesvirus family. The possible relationships among stress, prenatal depression, and herpes viral reactivation in pregnancy are understudied and the molecular pathways such as the neuroimmune biogenic amine pathway are unidentified. Chronic stress shifts the T helper-1 cell (Th1) cytokine profile to a Th2 profile, which favors virus induced pathogenesis and survival. Pregnancy is also associated with a similar Th2 dominance. In non-pregnant individuals, exposure to psychological or physical stress may be associated with latent herpes viral reactivation and could result in behavioral deficits and depression. Normally, type-1 cytokines such as Interferon-gamma (IFN -gamma) and inflammatory cytokines such as tumor necrosis factor-alpha (TNF-alpha) induce indoleamine-2, 3-dioxygenase (IDO) activation which inhibits herpes virus replication and reactivation, decreases tryptophan production, and alters phenylalanine /tyrosine metabolism. Thus it is possible that prenatal depression may occur from tryptophan stealing through the IDO pathway which results in decreased serotonin as well as increased risk for latent herpes viral reactivation. The purpose of this study is to analyze the relationships among stress, herpes viral titers, depression, and metabolites of IDO activation, which involves tryptophan and guanosine-triphosphate-cyclohydrolase-1(GTP-CH1) pathways. This study builds on Influence of Lactation on Postpartum Stress and Immunity (Grant number: R01-NR05000) which investigated perinatal immune, endocrine, and inflammatory changes in pregnancy and the postpartum. A secondary data analysis was conducted on baseline data from women collected at 16 to 25 gestational weeks. This data set included some herpes viral titers, and additional ones were measured in stored plasma samples. The aim of this study is to examine relationships among stress, herpes viral reactivation, depression, and the IDO activation pathway. The results of this study provide information about the possible role of further relationships of prenatal stress, latent herpes viral reactivation, and depression mechanisms. The results will be important in health promotion and disease prevention during pregnancy. CMV HSV-2 IDO Phenylalanine Th1/Th2 Immunity Tryptophan Biological Psychology Immunology and Infectious Disease Nursing Virology
93	Th1 και Th2 τύπου κυτταροκίνες σε αυτοάνοσα νοσήματα Χατζαντώνη, Κοκώνα Π. 25 June 2007 (has links) Η παρούσα διατριβή είχε ως στόχο τη μελέτη των Th1 και Th2 τύπου κυτταροκινών σε αυτοάνοσες νόσους και τη διερεύνηση του τρόπου με τον οποίο η έκφρασή τους επηρεάζεται από παράγοντες όπως πεπτιδικά ανάλογα της βασικής πρωτείνης της μυελίνης και ανοσοτροποποιητικοί παράγοντες όπως το μόριο της λεπτίνης. Η μελέτη αυτών των παραγόντων εστιάστηκε στη νόσο της Σκλήρυνσης Κατά Πλάκας, επειδή πρόκειται για οργανοειδικό CD4+ Τ κυτταρομεσολαβούμενο αυτοάνοσο νόσημα με χαρακτηριστικό Th1 κυτταροκινικό προφίλ. Αυτά τα χαρακτηριστικά, σε συνδυασμό με το γεγονός ότι διαθέτει το καλύτερα μελετημένο αντίστοιχο ζωικό μοντέλο, την Επαγόμενη Αλλεργική Εγκεφαλομυελίτιδα, καθιστούν τη νόσο αυτή ένα ιδανικό πειραματικό σύστημα για την επίτευξη του στόχου της παρούσας εργασίας. / - Κυτταροκίνες Th1 Κυτταροκίνες Th2 Αυτοάνοσα νοσήματα Τ κύτταρα B κύτταρα 616.978 Autoimmune diseases
94	Mécanismes responsables de la protection des souris NOD contre le diabète de type 1 par les cellules dendritiques conditionnées à la TSLP Dogbe, Akuvi Mawulom January 2012 (has links) Le diabète de type 1 (DT1) est une maladie auto-immune qui résulte en la destruction des cellules (ß des îlots de Langerhans par les cellules du système immunitaire. Des travaux précédents de notre laboratoire ont identifié la cytokine "Thymic Stromal Lymphopoietin" (TSLP) comme étant un stimulus tolérogénique pour les cellules dendritiques (DCs) chez le modèle murin du DT1, la souris "Non Obese Diabeiic" (NOD). Les DCs conditionnées à la TSLP (TSLP-DCs) présentent un phénotype semi-mature, sont capables d’induire une réponse Th2 ainsi qu’une conversion et une expansion des lymphocytes T régulateurs (Tregs) in vitro et protègent les souris NOD contre le DT1. Ces observations nous ont amené à investiguer les mécanismes qui entraînent cette protection contre le DT1. Les travaux décrits dans ce mémoire montrent que les TSLP-DCs injectées chez les souris NOD migrent vers la rate, de manière privilégiée. Ces observations nous ont amené à étudier l’influence des TSLP-DCs sur la réponse Th1/Th2 au niveau de la rate. Nous avons observé que les splénocytes CD4[indice supérieur +] et CD8[indice supérieur +] de souris injectées avec des TSLP-DCs exprimaient moins d’IFN? par rapport au souris témoins (splénocytes des souris injectées avec des LPS-DCs). Ces résultats suggèrent une diminution de la réponse Th1 chez ces splénocytes. Par contre, les résultats obtenus avec l’IL-10 ne nous ont pas permis de conclure quant à l’influence des TSLP-DCs sur la réponse Th2. Cependant, nous avons confirmé la capacité des TSLP-DCs à induire la conversion des lymphocytes T CD4[indice supérieur +]CD25[indice supérieur -] en Tregs CD4[indice supérieur +]CD25[indice supérieur +]Foxp3[indice supérieur +]. Nous avons aussi montré que ces Tregs partiellement convertis inhibent la prolifération de lymphocytes T 8.3-CD8[indice supérieur +] diabétogènes, et empêchent la production d’IFN?. Les Tregs convertis en présence de TSLP-DCs ou de LPS-DCs ont également été injectés à des souris 8.3-NOD.RAG2[indice supérieur -/-]. Les résultats ont révélé que seuls les Tregs différenciés en présence de TSLP-DCs ont la capacité d’empêcher le développement du DT1. Nos travaux suggèrent que la diminution de la réponse Th1 et l’induction d’une population efficiente de lymphocytes Tregs font partie des mécanismes utilisés par les TSLP-DCs pour protéger les souris NOD contre le DT1. Réponse Th1/Th2 Tregs Souris NOD Cellules dendritiques TSLP Diabète de type 1
95	Cytokines and immune balance in preeclampsia : a survey of some immunological variables and methods in the study of preeclampsia / Jonsson, Yvonne, January 2005 (has links) (PDF) Diss. (sammanfattning) Linköping : Linköpings universitet, 2005. / Härtill 4 uppsatser.
96	LPS induced T[subscript]H2 (Interleukin-4) cytokine production in macrophages and its regulation Mukherjee, Sumanta. January 2008 (has links) Dissertation (Ph.D.)--University of Toledo, 2008. / "In partial fulfillment of the requirements for the degree of Doctor of Philosophy in Biomedical Sciences." Title from title page of PDF document. Bibliography: p. 161-180.
97	Cannabinoids induce immunoglobulin class switching to IgE in B lymphocytes / Agudelo, Marisela. January 2009 (has links) Dissertation (Ph.D.)--University of South Florida, 2009. / Includes vita. Includes bibliographical references. Also available online.
98	Níveis de vitamina d e perfil de citocinas em pacientes com lúpus eritematoso sistêmico Schneider, Laiana January 2014 (has links) OBJETIVO: Avaliar a expressão dos perfis de citocinas Th1, Th2 e Th17 em pacientes com LES e verificar possíveis associações com os níveis séricos de vitamina D. MÉTODOS: Estudo transversal com inclusão de 172 pacientes acompanhados no ambulatório de reumatologia do Hospital de Clínicas de Porto Alegre. Os níveis de vitamina D foram medidos por quimiluminescência. Níveis séricos <20 ng/ml foram considerados como deficiência de vitamina D e níveis ≥20 ng/ml foram considerados normais. As citocinas foram medidas no soro após o descongelamento das amostras em uma única ocasião, usando Kit CBA (cytometric beads array) Th1/Th2/Th17. RESULTADOS: Cento e sessenta e um (94%) pacientes eram mulheres e 128 (74,4%) foram classificados como euro-descendentes. A idade média foi de 40,5±13,8 anos e a idade média no momento do diagnóstico foi de 31,5±13,4 anos. Na entrada do estudo, os pacientes tiveram mediana (intervalo interquartil) de atividade da doença (SLEDAI- systemic lupus erythematosus disease activity index) de 2 (1-4) e cronicidade (SLICC damage index- systemic lupus international collaborating clinics) de 0 (0-1). O nível médio de vitamina D foi de 25,4±11,04 ng/ml. Cinquenta e nove (34,3%) pacientes apresentavam deficiência de vitamina D e 113 (65,7%) tinham níveis considerados normais. Nenhuma associação e correlação estatisticamente significativa foram encontradas. Os níveis de INF-α e SLEDAI mostraram uma correlação positiva fraca (rs=0,22, p=0,04). Análise de regressão linear foi realizada para controlar possíveis fatores de confusão. CONCLUSÃO: A deficiência de vitamina D é prevalente em pacientes com LES, entretanto, não foram encontradas correlações e associações entre níveis de vitamina D e perfil de citocinas. Confirmamos a correlação existente entre o IFN-α e SLEDAI, conforme a literatura. Efeito in vitro de vitamina D no perfil de citocinas não foi reproduzido no presente estudo. Estudos longitudinais podem ajudar a esclarecer a influência da vitamina D na fisiopatogenia do LES. / OBJECTIVES: To evaluate the expression of Th1, Th2 and Th17 cytokine profiles in SLE patients and verify possible associations with serum vitamin D levels. METHODS: Cross-sectional study with 172 SLE patients, followed at the outpatient clinic of rheumatology at Hospital de Clínicas de Porto Alegre were included. The levels of vitamin D were measured by chemiluminescence. Serum levels <20 ng/ml were considered as vitamin D deficiency. Normal vitamin D levels were defined as ≥20ng/ml. Cytokines were measured in serum after thawing the samples on a single occasion, using Kit CBA (cytometric beads array) Th1/Th2/Th17. RESULTS: One hundred sixty one (94%) patients were women and 128 (74.4%) were classified as European derived. The mean age of patients was 40.5±13.8 years and the mean age at diagnosis was 31.5±13.4 years. At the time of study entry, patients had median (IQR) of active disease (SLEDAI- systemic lupus erythematosus disease activity index) of 2 (1-4) and chronicity (SLICC damage index- systemic lupus international collaborating clinics) of 0 (0-1). Mean vitamin D levels were 25.4±11.04 ng/ml. Fifty-nine (34.3%) patients had vitamin D deficiency and 113 (65.7%) had normal levels. No association and statistically significant correlations was found. The levels of INF-α and SLEDAI showed a weak positive correlation (rs=0.22, p=0.04). Linear regression analysis was performed to control for possible confounding factors. CONCLUSION:Vitamin D deficiency is prevalent in patients with SLE, however, no statistically significant correlations and associations between vitamin D levels and cytokine profile were found. We confirm the correlation between IFN-α and SLEDAI, according to the literature. In vitro effect of vitamin D on the cytokine profile was not reproduced in this study. Longitudinal studies may help clarify the influence of vitamin D in the pathogenesis of SLE. Vitamina D Citocinas Lupus eritematoso cutâneo Systemic lupus erythematosus Vitamin D Cytokines Th1 Th2 Th17
99	Níveis de vitamina d e perfil de citocinas em pacientes com lúpus eritematoso sistêmico Schneider, Laiana January 2014 (has links) OBJETIVO: Avaliar a expressão dos perfis de citocinas Th1, Th2 e Th17 em pacientes com LES e verificar possíveis associações com os níveis séricos de vitamina D. MÉTODOS: Estudo transversal com inclusão de 172 pacientes acompanhados no ambulatório de reumatologia do Hospital de Clínicas de Porto Alegre. Os níveis de vitamina D foram medidos por quimiluminescência. Níveis séricos <20 ng/ml foram considerados como deficiência de vitamina D e níveis ≥20 ng/ml foram considerados normais. As citocinas foram medidas no soro após o descongelamento das amostras em uma única ocasião, usando Kit CBA (cytometric beads array) Th1/Th2/Th17. RESULTADOS: Cento e sessenta e um (94%) pacientes eram mulheres e 128 (74,4%) foram classificados como euro-descendentes. A idade média foi de 40,5±13,8 anos e a idade média no momento do diagnóstico foi de 31,5±13,4 anos. Na entrada do estudo, os pacientes tiveram mediana (intervalo interquartil) de atividade da doença (SLEDAI- systemic lupus erythematosus disease activity index) de 2 (1-4) e cronicidade (SLICC damage index- systemic lupus international collaborating clinics) de 0 (0-1). O nível médio de vitamina D foi de 25,4±11,04 ng/ml. Cinquenta e nove (34,3%) pacientes apresentavam deficiência de vitamina D e 113 (65,7%) tinham níveis considerados normais. Nenhuma associação e correlação estatisticamente significativa foram encontradas. Os níveis de INF-α e SLEDAI mostraram uma correlação positiva fraca (rs=0,22, p=0,04). Análise de regressão linear foi realizada para controlar possíveis fatores de confusão. CONCLUSÃO: A deficiência de vitamina D é prevalente em pacientes com LES, entretanto, não foram encontradas correlações e associações entre níveis de vitamina D e perfil de citocinas. Confirmamos a correlação existente entre o IFN-α e SLEDAI, conforme a literatura. Efeito in vitro de vitamina D no perfil de citocinas não foi reproduzido no presente estudo. Estudos longitudinais podem ajudar a esclarecer a influência da vitamina D na fisiopatogenia do LES. / OBJECTIVES: To evaluate the expression of Th1, Th2 and Th17 cytokine profiles in SLE patients and verify possible associations with serum vitamin D levels. METHODS: Cross-sectional study with 172 SLE patients, followed at the outpatient clinic of rheumatology at Hospital de Clínicas de Porto Alegre were included. The levels of vitamin D were measured by chemiluminescence. Serum levels <20 ng/ml were considered as vitamin D deficiency. Normal vitamin D levels were defined as ≥20ng/ml. Cytokines were measured in serum after thawing the samples on a single occasion, using Kit CBA (cytometric beads array) Th1/Th2/Th17. RESULTS: One hundred sixty one (94%) patients were women and 128 (74.4%) were classified as European derived. The mean age of patients was 40.5±13.8 years and the mean age at diagnosis was 31.5±13.4 years. At the time of study entry, patients had median (IQR) of active disease (SLEDAI- systemic lupus erythematosus disease activity index) of 2 (1-4) and chronicity (SLICC damage index- systemic lupus international collaborating clinics) of 0 (0-1). Mean vitamin D levels were 25.4±11.04 ng/ml. Fifty-nine (34.3%) patients had vitamin D deficiency and 113 (65.7%) had normal levels. No association and statistically significant correlations was found. The levels of INF-α and SLEDAI showed a weak positive correlation (rs=0.22, p=0.04). Linear regression analysis was performed to control for possible confounding factors. CONCLUSION:Vitamin D deficiency is prevalent in patients with SLE, however, no statistically significant correlations and associations between vitamin D levels and cytokine profile were found. We confirm the correlation between IFN-α and SLEDAI, according to the literature. In vitro effect of vitamin D on the cytokine profile was not reproduced in this study. Longitudinal studies may help clarify the influence of vitamin D in the pathogenesis of SLE. Vitamina D Citocinas Lupus eritematoso cutâneo Systemic lupus erythematosus Vitamin D Cytokines Th1 Th2 Th17
100	Imunoglobulina e e eosin?filos em crian?as de ?rea tropical, infectadas por ascaris lumbricoides Silva, Edna Marques de Ara?jo 20 August 2013 (has links) Made available in DSpace on 2014-12-17T14:13:46Z (GMT). No. of bitstreams: 1 EdnaMAS_TESE.pdf: 813256 bytes, checksum: 6c2788ba74c72a29680a0f392ee49282 (MD5) Previous issue date: 2013-08-20 / Universidade Federal do Rio Grande do Norte / Este trabalho objetivou estudar a imunoglobulina E total e espec?fica para A. lumbricoides e eosin?filos em crian?as de ?rea end?mica, a fim de avaliar a resposta imune do tipo Th2 e relacionar os dados obtidos com a idade, sexo e intensidade da infec??o numa popula??o formada por 205 crian?as com faixa et?ria de 1 a 10 anos, de ambos os sexos e baixo n?vel socioecon?mico. Foram analisadas amostras fecais das crian?as, pelos m?todos de Blagg e Cols. e Kato-katz, determinadas as dosagens s?ricas de IgE total, IgE espec?fica para A. lumbricoides, pelo m?todo ImmunoCAP e realizada a contagem relativa de eosin?filos no sangue perif?rico. Os resultados revelaram uma ocorr?ncia de 182 (88,8 %) para enteroparasitas, 168 (81,9%) para helmintos intestinais e 140 (68,3%) para A. lumbricoides. A mediana dos n?veis s?ricos de IgE total e espec?fica e o n?mero de eosin?filos se apresentaram acima dos valores de refer?ncia padr?o (mediana 480 kU/L, 0,74 kU/L e 8 %). Ocorreu uma diferen?a significante nos n?veis de IgE total, IgE espec?fica e no n?mero de eosin?filos entre as crian?as parasitadas por A. lumbricoides e as n?o parasitadas (p = 0,02; <0,01; < 0,03), no entanto, estes, n?o apresentaram diferen?a significativa com a idade e sexos das crian?as e intensidade da infec??o.Houve uma correla??o positiva entre os n?veis de IgE total e IgE espec?fica (r = 0,55). Conclu?mos, portanto, que a infec??o por enteroparasitas, em especial para o A. lumbricoides, induziu uma resposta imune do tipo Th2 com produ??o de IgE total e espec?fica e eosin?filos nas crian?as infectadas CNPQ::CIENCIAS DA SAUDE

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