Global ETD Search

71	Identificação de marcadores moleculares para células T reguladoras humanas com perfil CD4+CD25+ por phage display / Peptide phage display for the identification of novel molecular markers on human thymic regulatory CD4+CD25+ T cells Mundin, Georgia Sabio Porto 29 February 2008 (has links) Há dados na literatura indicando que as células que saem do timo com o fenótipo CD4+CD25+ são desenvolvidas continuamente como uma linhagem independente e possuem um papel importante no processo de regulação da resposta imune. Essas células são chamadas células T reguladoras naturais. Várias questões sobre estas células permanecem em aberto, como por exemplo, como elas são geradas, o que é determinante na sua atividade reguladora e que marcadores específicos podem ser usados para identificá-las? Dentro deste contexto, o nosso objetivo neste trabalho foi identificar no timo e em timócitos CD4+/CD25+ humanos, novas moléculas potencialmente importantes no desenvolvimento e/ou na atividade supressora das células T reguladoras naturais. Para este objetivo, utilizamos a abordagem de phage display, com uma biblioteca de fagos de peptídeos, e timos humanos obtidos de pacientes portadores de cardiopatias congênitas, submetidos a cirurgias cardíacas realizadas no InCor. A busca dessas moléculas foi feita, separadamente, em 3 tipos de material biológico: timócitos totais, fragmento do tecido tímico e timócitos CD4+/CD25+. Antes da incubação da biblioteca de fagos com os timócitos totais e timócitos CD4+/CD25+ (separação em FACS), foi realizada uma etapa de preclearing, incubando-se a biblioteca de fagos com um pool de células mononucleares de sangue periférico (PBMC) ou timócitos CD4+/CD25-, respectivamente. Os fagos não ligantes, recuperados desta etapa, foram então incubados com as células de interesse. Para o tecido tímico não foi feita etapa de pre-clearing. Os fagos obtidos com os diferentes materiais biológicos foram recuperados em cultura de bactérias e usados em ciclos posteriores de seleção. Após três ciclos de seleção, os fagos foram seqüenciados e identificados quanto à expressão de peptídeos ligantes para timócitos totais, timo e timócitos CD4+/CD25+, e analisados em bancos de dados no BLAST. Os fagos selecionados para validação um ligante de tecido tímico: M2C e um ligante de timócitos CD4+/CD25+: R2A fazem similaridade a duas proteínas associadas ao metabolismo da Vitamina D3, molécula envolvida em imunorregulação e indução de tolerância, em diversos modelos experimentais. Porém, não há dados na literatura a respeito do seu papel em células T reg naturais. Na validação molecular desses fagos, apesar de certa variabilidade entre os diferentes ensaios, verificamos, por ELISA, que os fagos se ligam preferencialmente a 1,25 diidroxivitamina D3, forma ativa da Vitamina D3. Entretanto, nos ensaios de validação funcional, a influência da vitamina D na diferenciação dessas células não foi confirmada de forma consistente, uma vez que só tivemos aumento no número de células CD4+/CD25+, em cultura com Vitamina D, em poucos experimentos. As moléculas identificadas no presente estudo podem ter implicações relevantes no processo de diferenciação e na atividade de células T CD4+CD25+ reguladoras e serão mais investigadas na continuidade deste trabalho. / There are consistent data in literature indicating that thymic CD4+CD25+ cells play an important role in immune regulation and are continuously developed as an independent lineage in the thymus. These cells are known as natural regulatory T cells. Several questions about these cells remain unanswered, such as how they are generated, what is determinant in their regulatory function and which specific molecular markers can be used to identify them. Taking this into consideration, our aim was to identify new potentially important molecules in the development and/or supressive function of natural regulatory T cells, both in the thymus and in CD4+CD25+ thymocytes. For this, the phage display technique was employed, with a peptide phage library and thymic specimens obtained from children who underwent corrective cardiac surgery at the Heart Institute (InCor), in São Paulo. The search for these molecules was separately performed in 3 types of biological material: thymic tissue, thymocytes and CD4+CD25+ thymic cells. In the first stage, the phage peptide-library was incubated with a pool of PBMC (peripheral blood mononuclear cells). After the incubation, phages bound to PBMC were discarded (pre-clearing). In the second stage, unbound phages were incubated with either total thymocytes or CD4+CD25+ thymic cells. The pre-clearing stage was not perfomed in the thymic tissue. The phages obtained with after incubation with the different biological materials were recovered in E. coli culture and used in additional cycles of selection. After three rounds of selection, the recovered phages from the total thymocytes, from thymic tissue and thymocytes CD4+CD25+ were sequenced and their ligands identified. Among the phages selected for validation one ligand of thymic tissue: M2C and one ligand of CD4+CD25+ thymocytes: R2A present similarity to two proteins associated to the metabolism of Vitamin D3, a molecule involved in imunoregulation and toelrance induction in several experimental models. However, there are no data in the literature concerning the possible role of this moelcule in natural regulatory T cells. In the molecular validation of theses phages, although some variability between the diffeterent assays we have verified by ELISA, that the phages present preferential binding to the 1,25 dhydroxyvitamin D3, the active form of Vitamin D3. However, in the functional validation assays, the influence of the Vitamin D3 in the differentiation of these cells could not be consistently confirmed since we could observe an increase in the number of CD4+CD25+ cells cultured with vitamin D in only a few experiments. The ligand-receptor molecules we have defined in this study may have relevant implications in the development of CD4+CD25+ regulatory T cells in the thymus Biblioteca de peptídeos Biological markers Calcitriol receptors Imunoregulation Imunorregulação Linfócitos T reguladores Marcadores biológicos Peptide library Receptores de calcitiol Regulatory T lymphocytes Thymus gland Timo Vitamin D3 Vitamina D3
72	Interaction of the Hedgehog and vitamin D receptor signaling pathways in Patched associated cancers Linder, Benedikt 07 May 2015 (has links) No description available. 570 hedgehog patched smoothened vitamin d calcitriol gli gli1 gli2 gli3 cancer oncology mouse models basal cell carcinoma vdr vitamin d receptor Biologie (PPN619462639)
73	Enzymatic Regulation of Steroidogenesis and Nuclear Receptor Activation : Special Focus on Vitamin D and Sex Hormones Lundqvist, Johan January 2011 (has links) Enzyme-catalyzed reactions are important to regulate steroidogenesis and nuclear receptor activation. The present investigation examines the role of steroid metabolism catalyzed by CYP7B1 for regulation of hormone receptor activation and the effects of vitamin D on enzymatic regulation of steroidogenesis. The study reports data indicating that CYP7B1 can regulate estrogenic signaling by converting estrogens into inactive or less active metabolites. Similar results were obtained for CYP7B1-mediated metabolism of some androgen receptor ligands, indicating that CYP7B1 can be involved also in the regulation of androgenic signaling. CYP7B1 substrates and metabolites were found to exert androgenic effects in a cell line-specific manner. Furthermore, cell line differences were observed in the expression pattern for androgen receptor comodulators. This thesis reports that 1α,25-dihydroxyvitamin D3 alters the gene expression and enzyme activity of CYP21A2 and CYP17A1 leading to suppressed production of aldosterone, dehydroepiandrosterone and androstenedione in adrenocortical cells. These are novel findings on vitamin D action. A mechanism is reported for the vitamin D-mediated regulation of the CYP21A2 gene. Data indicate that vitamin D receptor interacting repressor (VDIR) and Williams syndrome transcription factor (WSTF) are key comodulators in this novel vitamin D receptor (VDR)-mediated mechanism. Furthermore, the results indicate that altered expression levels of VDIR and WSTF can shift the suppressing effect of vitamin D to a stimulatory effect. Also, epigenetic components were found to be involved in the effects of vitamin D on CYP21A2 transcriptional rate. In addition, a functional vitamin D response element was identified in the CYP21A2 promoter. This study also reports that 1α,25-dihydroxyvitamin D3 affects sex hormone production in a tissue-specific way. Gene expression and enzyme activity of aromatase were found to be downregulated in cells derived from breast, but not in cells derived from prostate and adrenal cortex. The production of estradiol and dihydrotestosterone was altered in a tissue-selective manner following vitamin D treatment. These findings are of importance for the discussion on vitamin D as a potential anti-breast cancer agent. adrenal steroidogenesis CYP7B1 vitamin D calcitriol enzymatic regulation transcriptional regulation CYP21A2 aromatase sex hormone estrogen androgen nuclear receptor Pharmaceutical biochemistry Farmaceutisk biokemi
74	Identificação de marcadores moleculares para células T reguladoras humanas com perfil CD4+CD25+ por phage display / Peptide phage display for the identification of novel molecular markers on human thymic regulatory CD4+CD25+ T cells Georgia Sabio Porto Mundin 29 February 2008 (has links) Há dados na literatura indicando que as células que saem do timo com o fenótipo CD4+CD25+ são desenvolvidas continuamente como uma linhagem independente e possuem um papel importante no processo de regulação da resposta imune. Essas células são chamadas células T reguladoras naturais. Várias questões sobre estas células permanecem em aberto, como por exemplo, como elas são geradas, o que é determinante na sua atividade reguladora e que marcadores específicos podem ser usados para identificá-las? Dentro deste contexto, o nosso objetivo neste trabalho foi identificar no timo e em timócitos CD4+/CD25+ humanos, novas moléculas potencialmente importantes no desenvolvimento e/ou na atividade supressora das células T reguladoras naturais. Para este objetivo, utilizamos a abordagem de phage display, com uma biblioteca de fagos de peptídeos, e timos humanos obtidos de pacientes portadores de cardiopatias congênitas, submetidos a cirurgias cardíacas realizadas no InCor. A busca dessas moléculas foi feita, separadamente, em 3 tipos de material biológico: timócitos totais, fragmento do tecido tímico e timócitos CD4+/CD25+. Antes da incubação da biblioteca de fagos com os timócitos totais e timócitos CD4+/CD25+ (separação em FACS), foi realizada uma etapa de preclearing, incubando-se a biblioteca de fagos com um pool de células mononucleares de sangue periférico (PBMC) ou timócitos CD4+/CD25-, respectivamente. Os fagos não ligantes, recuperados desta etapa, foram então incubados com as células de interesse. Para o tecido tímico não foi feita etapa de pre-clearing. Os fagos obtidos com os diferentes materiais biológicos foram recuperados em cultura de bactérias e usados em ciclos posteriores de seleção. Após três ciclos de seleção, os fagos foram seqüenciados e identificados quanto à expressão de peptídeos ligantes para timócitos totais, timo e timócitos CD4+/CD25+, e analisados em bancos de dados no BLAST. Os fagos selecionados para validação um ligante de tecido tímico: M2C e um ligante de timócitos CD4+/CD25+: R2A fazem similaridade a duas proteínas associadas ao metabolismo da Vitamina D3, molécula envolvida em imunorregulação e indução de tolerância, em diversos modelos experimentais. Porém, não há dados na literatura a respeito do seu papel em células T reg naturais. Na validação molecular desses fagos, apesar de certa variabilidade entre os diferentes ensaios, verificamos, por ELISA, que os fagos se ligam preferencialmente a 1,25 diidroxivitamina D3, forma ativa da Vitamina D3. Entretanto, nos ensaios de validação funcional, a influência da vitamina D na diferenciação dessas células não foi confirmada de forma consistente, uma vez que só tivemos aumento no número de células CD4+/CD25+, em cultura com Vitamina D, em poucos experimentos. As moléculas identificadas no presente estudo podem ter implicações relevantes no processo de diferenciação e na atividade de células T CD4+CD25+ reguladoras e serão mais investigadas na continuidade deste trabalho. / There are consistent data in literature indicating that thymic CD4+CD25+ cells play an important role in immune regulation and are continuously developed as an independent lineage in the thymus. These cells are known as natural regulatory T cells. Several questions about these cells remain unanswered, such as how they are generated, what is determinant in their regulatory function and which specific molecular markers can be used to identify them. Taking this into consideration, our aim was to identify new potentially important molecules in the development and/or supressive function of natural regulatory T cells, both in the thymus and in CD4+CD25+ thymocytes. For this, the phage display technique was employed, with a peptide phage library and thymic specimens obtained from children who underwent corrective cardiac surgery at the Heart Institute (InCor), in São Paulo. The search for these molecules was separately performed in 3 types of biological material: thymic tissue, thymocytes and CD4+CD25+ thymic cells. In the first stage, the phage peptide-library was incubated with a pool of PBMC (peripheral blood mononuclear cells). After the incubation, phages bound to PBMC were discarded (pre-clearing). In the second stage, unbound phages were incubated with either total thymocytes or CD4+CD25+ thymic cells. The pre-clearing stage was not perfomed in the thymic tissue. The phages obtained with after incubation with the different biological materials were recovered in E. coli culture and used in additional cycles of selection. After three rounds of selection, the recovered phages from the total thymocytes, from thymic tissue and thymocytes CD4+CD25+ were sequenced and their ligands identified. Among the phages selected for validation one ligand of thymic tissue: M2C and one ligand of CD4+CD25+ thymocytes: R2A present similarity to two proteins associated to the metabolism of Vitamin D3, a molecule involved in imunoregulation and toelrance induction in several experimental models. However, there are no data in the literature concerning the possible role of this moelcule in natural regulatory T cells. In the molecular validation of theses phages, although some variability between the diffeterent assays we have verified by ELISA, that the phages present preferential binding to the 1,25 dhydroxyvitamin D3, the active form of Vitamin D3. However, in the functional validation assays, the influence of the Vitamin D3 in the differentiation of these cells could not be consistently confirmed since we could observe an increase in the number of CD4+CD25+ cells cultured with vitamin D in only a few experiments. The ligand-receptor molecules we have defined in this study may have relevant implications in the development of CD4+CD25+ regulatory T cells in the thymus Biblioteca de peptídeos Imunorregulação Linfócitos T reguladores Marcadores biológicos Receptores de calcitiol Timo Vitamina D3 Biological markers Calcitriol receptors Imunoregulation Peptide library Regulatory T lymphocytes Thymus gland Vitamin D3
75	Vitamin D Clinical Relevance in the Recovery From Traumatic Brain Injury Among the Military Population Colón, Yuisa M. 01 January 2016 (has links) Background: Traumatic brain injury (TBI) still remains a difficult disorder to treat. TBI has been associated to chronic neuroinflammation and a high risk for neurodegenerative disorders. Since 2001 between ten to twenty percent of all deployed military members have suffered a combat-related TBI. Nearly twenty to thirty percent of those will experience chronic cognitive, behavioral and somatic symptoms after suffering a TBI. Methods: The objective of this review is to evaluate current literature examining vitamin D as a neurosteroid with protective properties and its clinical relevance after traumatic brain injury. Vitamin D is known to participate in neurobiological processes and genomic regulation in the brain. Clinical and laboratory findings support that vitamin D modulates the immune responses to trauma, diminishes oxidative and toxic damage, and inhibiting activation and progression of the neuroinflammation. Inadequate levels of vitamin D have been identified as a common risk factor for many neurological disorders and have been linked to poorer recovery. Results: This review found compelling evidence to support that the pathology of TBI is closely associated with neuroprotective mechanisms of vitamin D. Low vitamin D levels are common among US active duty military and veterans. The findings strongly suggest that optimizing vitamin D prior to injury could improve the recovery for military members after experiencing a TBI. Vitamin D ameliorates brain damage by modulating neuroinflammation, improving cell survival and down-regulating mechanisms involved in the progression of cell damage following a TBI. However, further studies are needed to evaluate the effects of vitamin D optimization in TBI outcomes. vitamin D calcitriol 25OHD3 low vitamin D neuroprotection traumatic brain injury TBI Behavioral Neurobiology Cognitive Neuroscience Medicine and Health Military and Veterans Studies Molecular and Cellular Neuroscience Neurology Neurosciences Trauma
76	Hiperparatireoidismo secundário: fatores prognósticos de recidiva atribuída ao implante após paratireoidectomia total e auto-implante\" / Secondary hyperparathyroidism : prognostic factors of graft-dependent recurrence after total parathyroidectomy and parathyroid autotransplantation Arap, Sérgio Samir 27 October 2005 (has links) Nos casos de hiperparatireoidismo secundário onde não é possível o tratamento clínico, é indicada a paratireoidectomia. No Serviço de Cirurgia de Cabeça e Pescoço do Hospital das Clínicas da Faculdade de Medicina da Universidade de São Paulo, o tipo de cirurgia utilizada é a paratireoidectomia total com auto-implante de paratireóide em membro superior. Nesses casos, ao contrário da paratireoidectomia total, pode haver recidiva do hiperparatireoidismo no sítio do implante, com sintomas sistêmicos e com necessidade de intervenção para retirada do tecido hiperplásico. Já na paratireoidectomia total, há hipoparatireoidismo definitivo e risco de doença óssea adinâmica. O presente estudo tem como escopo avaliar os pacientes submetidos a paratireoidectomia com implante e esclarecer se há fatores clínicos e de imunohistoquímica que possam indicar antes da cirurgia algum risco de recidiva no implante / When clinical treatment of secondary hyperparathyroidism fails, parathyroidectomy is mandatory. Total parathyroidectomy and immediate parathyroid autotransplantation in the forearm is the treatment of choice at Head and Neck Surgery of Hospital das Clínicas of University of São Paulo Medical School. In this cases, recurrent hyperparathyroidism may be caused by hyperplastic graft tissue. Without autotransplantation, adinamic bone disease may occur. The present study seek to evaluate patients submitted to total parathyroidectomy and autotransplantation and try to clarify clinical or immunohistochemical calcium-sensing/analysis Glândulas paratireóides/fisiopatologia Glândulas paratireóides/transplante Hyperparathyroidism secondary/surgery Parathyroid glands/physiopathology Parathyroid glands/transplantation Parathyroidectomy/adverse effects Paratireoidectomia/efeitos adversos Receptores de calcitriol/análise Receptors Receptors calcitriol/analysis Receptors parathyroid hormone/analysis Recidiva/prevenção & controle Recurrence/prevention & control
77	1alpha,25-Dihydroxy-VitaminD3 hemmt das Wachstum von Patched-assoziierten Rhabdomyosarkomen und Basaliomen / 1alpha,25-Dihydroxy-VitaminD3 inhibits the growth of Patched-associated rhadomyosarkomas and basal cell carcinomas Lammering, Iris Berenice 02 November 2011 (has links) No description available. 610 Medizin, Gesundheit MED 301 MED 424 Medicine Hedgehog/Patched-Signalweg VitaminD-Rezeptor-Siganlweg 1á 25(OH)2D3 Calcitriol Antitumor Therapie Basalzellkarzinome Rhabdomyosarkome Hedgehog/Patched-signaling 1á 25(OH)2D3 vitamin-D-receptor-signalin calcitriol antitumor therapy basal cell carcinoma rhabdomyosarkoma 44.30 44.48 44.81
78	Hiperparatireoidismo secundário: fatores prognósticos de recidiva atribuída ao implante após paratireoidectomia total e auto-implante\" / Secondary hyperparathyroidism : prognostic factors of graft-dependent recurrence after total parathyroidectomy and parathyroid autotransplantation Sérgio Samir Arap 27 October 2005 (has links) Nos casos de hiperparatireoidismo secundário onde não é possível o tratamento clínico, é indicada a paratireoidectomia. No Serviço de Cirurgia de Cabeça e Pescoço do Hospital das Clínicas da Faculdade de Medicina da Universidade de São Paulo, o tipo de cirurgia utilizada é a paratireoidectomia total com auto-implante de paratireóide em membro superior. Nesses casos, ao contrário da paratireoidectomia total, pode haver recidiva do hiperparatireoidismo no sítio do implante, com sintomas sistêmicos e com necessidade de intervenção para retirada do tecido hiperplásico. Já na paratireoidectomia total, há hipoparatireoidismo definitivo e risco de doença óssea adinâmica. O presente estudo tem como escopo avaliar os pacientes submetidos a paratireoidectomia com implante e esclarecer se há fatores clínicos e de imunohistoquímica que possam indicar antes da cirurgia algum risco de recidiva no implante / When clinical treatment of secondary hyperparathyroidism fails, parathyroidectomy is mandatory. Total parathyroidectomy and immediate parathyroid autotransplantation in the forearm is the treatment of choice at Head and Neck Surgery of Hospital das Clínicas of University of São Paulo Medical School. In this cases, recurrent hyperparathyroidism may be caused by hyperplastic graft tissue. Without autotransplantation, adinamic bone disease may occur. The present study seek to evaluate patients submitted to total parathyroidectomy and autotransplantation and try to clarify clinical or immunohistochemical Glândulas paratireóides/fisiopatologia Glândulas paratireóides/transplante Paratireoidectomia/efeitos adversos Receptores de calcitriol/análise Recidiva/prevenção & controle calcium-sensing/analysis Hyperparathyroidism secondary/surgery Parathyroid glands/physiopathology Parathyroid glands/transplantation Parathyroidectomy/adverse effects Receptors Receptors calcitriol/analysis Receptors parathyroid hormone/analysis Recurrence/prevention & control
79	Fibroblast growth factor-23 and Klotho in bone/mineral and parathyroid disorders Krajisnik, Tijana January 2009 (has links) Fibroblast growth factor-23 (FGF23) is a novel, bone-produced hormone that regulates renal phosphate (Pi) reabsorption and calcitriol metabolism. Disorders of mineral and bone metabolism, such as autosomal dominant hypophosphatemic rickets (ADHR) and hyperostosis-hyperphosphatemia syndrome (HHS), witness the importance of well-balanced serum levels of FGF23. Patients with chronic kidney disease (CKD) are highly morbid due to Pi retention/hyperphosphatemia and calcitriol deficiency, which lead to elevated serum levels of parathyroid hormone (PTH) and secondary hyperparathyroidism (sHPT). As a response to hyperphosphatemia, CKD patients have also remarkably high serum FGF23 levels, which are associated with cardiovascular risk factors and increased mortality in CKD. The overall aim of this dissertation was to discern a possible role of FGF23 in parathyroid biology. Our in vitro experiments on isolated bovine parathyroid cells demonstrate that FGF23 directly and dose-dependently suppresses the PTH production and secretion, while increasing the expression of the 25-hydroxyvitamin D3-activating enzyme 1α-hydroxylase. We investigated possible expressional changes in the FGF23 receptor co-factor Klotho in hyperparathyroid disorders and found that Klotho expression is decreased or absent and inversely correlated to serum calcium (Ca) in adenomas of primary HPT (pHPT). In the hyperplastic parathyroid glands of sHPT, Klotho expression declines in parallel with the kidney function and correlates with the glomerular filtration rate. Moreover, Klotho expression is suppressed by Ca and FGF23, increased by calcitriol, but unaffected by Pi and PTH in vitro. Finally, we identified a novel missense mutation in the gene encoding GALNT3, which is normally involved in the post-translational glycosylation of FGF23, as the cause of aberrant FGF23 processing in a patient with HHS. In summary, we provide evidence for a novel bone/parathyroid axis in which FGF23 functions as a direct, negative regulator of the PTH production. High extracellular Ca is a major determinant of the Klotho expression in pHPT, whereas the Klotho levels in sHPT may be attributed to a combination of the high FGF23 and Ca, and low calcitriol levels associated with CKD. Hence, the decreased Klotho expression in sHPT could explain the concomitantly high FGF23 and PTH levels, as well as the failure of FGF23 to prevent or mitigate the development of sHPT in CKD. calcitriol chronic kidney disease CKD chronic renal failure fibroblast growth factor 23 fibroblast growth factor-23 FGF23 FGF-23 GalNac-T3 GALNT3 GFR hyperostosis-hyperphosphatemia syndrome HHS Klotho parathyroid hormone PTH hyperparathyroidism pHPT sHPT uremic vitamin D3 Endocrinology Endokrinologi
80	Vitamin D in Normal Breast Tissue Correlates to Early Breast Carcinogenesis Lan, Shang-Lun January 2016 (has links) No description available. Biomedical Research Biostatistics Endocrinology Epidemiology Molecular Biology Oncology Womens Studies breast cancer breast vitamin D 25OHD Calcifediol 1,25OH2D Calcitriol reduction mammoplasty breast risk factor pre-carcinogenesis metabolomics metabolomic profiling HMEC cyclic AMP UHPLC-QTOF-MS

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