Global ETD Search

441	Vitamin D and TNF-alpha Effects on Adipogenesis and Inflammation in Human Adipocytes Gray, Brianna 01 January 2011 (has links) (PDF) Obesity accounts for $168 billion in annual medical expenses and increases the risk of cardiovascular disease, cancer, and type-2 diabetes, three diseases responsible for over 50% of deaths in the United States. It is well established that the pattern of adiposity is an important factor in the relationship with disease risk and that visceral adiposity, which favors hypertrophy (characterized by enlarged cells) is more dangerous than subcutaneous adiposity, which tends to be hyperplastic (characterized by an increase in cell number). Hypertrophy is associated with inflammation and insulin resistance, and hyperplasia (adipogenesis, i.e., the formation of new adipocytes), is associated with improved insulin sensitivity. Tumor necrosis factor-alpha (TNF-alpha) is a potent pro-inflammatory cytokine that activates a nuclear factor-kappa B (NFKB) intracellular pathway that is an important mediator of obesity-associated insulin resistance and increased risk of type-2 diabetes. Interestingly, obesity has been positively associated with both low vitamin D status and elevated levels of TNF-alpha. Our studies focused on examining the influence of the active vitamin D hormone, 1,25-dihydroxyvitamin D, and TNF-alpha on adipogenesis and inflammation in human primary adipocytes and determining whether the balance of these two factors influences the extent to which adipocytes accumulate lipid or express pro-inflammatory cytokines. We found no effect of 1,25-dihydroxyvitamin D on adipogenesis or pro-adipogenic gene expression despite a clear upregulation of a vitamin D responsive gene, 24-hydroxylase, in response to treatment with 1,25-dihydroxyvitamin D. TNF-alpha clearly inhibited adipogenesis and expression of PPAR-gamma and C/EBP-alpha and enhanced expression of the pro-inflammatory cytokines IL-6 and MCP-1, but not IL-8. There was a trend towards a dose-dependent downregulation of MCP-1 by 1,25-dihydroxyvitamin D in three individuals; however, this effect was not statistically significant. While we found no interaction between TNF-alpha and 1,25-dihydroxyvitamin D on adipogenesis, there is a potential anti-inflammatory action of 1,25-dihydroxyvitamin D in human primary adipocytes. Future studies into this potential are warranted in light of the growing obesity epidemic and the interest in finding nutritionally modifiable treatment or prevention strategies to mitigate the negative consequences of obesity. obesity inflammation vitamin D TNF-alpha adipocyte cytokine Cell Biology Endocrinology Laboratory and Basic Science Research Nutritional and Metabolic Diseases Other Public Health
442	PRMT5-CATALYZED ARGININE METHYLATION OF NF-kappaB p65 INTHE ENDOTHELIAL CELL INDUCTION OF PRO-INFLAMMATORYCHEMOKINES Harris, Daniel Pellerin 27 January 2016 (has links) No description available. Biochemistry Molecular Biology Physiology Cellular Biology PRMT5 arginine methylation SDMA NF-kappaB p76 post-translational modification endothelial cell inflammation CXCL10 IP-10 CXCL11 I-TAC TNF-a IFNg transcription
443	The effect of androstenediol on gene expression and NF-κB activation in vitro Farrow, Michael John 30 August 2007 (has links) No description available. Androstenediol Glucocorticoid Inflammation Nuclear Factor Kappa B NF-kappaB p65 Chromatin Immunoprecipitation TransAM Transcription Gene Expression tumor necrosis factor alpha TNF-alpha cytokine
444	Effets d'une diète riche en oméga-3 sur l'infarctus du myocarde chez le rat Dubois, Mélanie January 2007 (has links) Mémoire numérisé par la Direction des bibliothèques de l'Université de Montréal. Acides gras essentiels Acides gras polyinsaturés Oméga-3 Huile de poisson Maladies cardiovasculaires Infactus du myocarde Rat Apoptose Caspase-3 AKT Eicosanoïde COX-2 TNF-a Cytokine Inflammation Agrégation plaquettaire
445	Análise da coinfecção entre ureaplasmas e o vírus do Papiloma Humano (HPV) em amostras cervicais e em um modelo de estudo \"in vitro\" de queratinócitos primários humanos (PHK). / Analysis of co-infection among ureaplasmas and the Human Papilloma Vírus (HPV) in cervical samples and in a infection model in vitro in primary human keratinocytes (PHK). Amorim, Aline Teixeira 30 April 2015 (has links) O desenvolvimento do câncer cervical depende da exposição ao HPV, fator necessário, mas não suficiente. Outras bactérias, tais como ureaplasmas, têm sido associadas como cofatores. O objetivo deste estudo foi avaliar a presença de ureaplasmas em mulheres com lesão cervical, e observar alterações em PHK causadas pela infecção por ureaplasmas. 140 swabs vaginais foram coletados. O material foi submetido a PCR para a detecção de HPV, Mollicutes, U. urealyticum, U. parvum e seus sorotipos, e outras bactérias de importância ginecológica; e qPCR para U. urealyticum e U. parvum. Também foi realizada a infecção de ureaplasmas em PHK transformados com HPV. As células foram contadas e realizou-se a dosagem das citocinas IL1-β, IL-6 e TNF-α. HPV, Mollicutes, U. parvum, sorotipos 1 e 6 de U. parvum, T. vaginalis e G. vaginalis, além de alguns fatores socioeconômicos, foram associados com lesão cervical. Verificou-se maior carga de U. parvum entre mulheres com lesão. Houve diminuição do número de células e maior liberação de IL-6 e TNF-α nos grupos infectados. Com os resultados obtidos neste estudo, foi possível verificar uma associação entre os ureaplasmas e HPV no início das lesões cervicais, contudo mais estudos precisam ser realizados para aprimorar essa hipótese. / The development of cervical cancer depends on the exposure to HPV, necessary factor, but not enough. Other bacteria, such as ureaplasmas, have been associated as cofactors. The aim of this study was to evaluate the presence of ureaplasmas in women with cervical injury, and observe changes in PHK infected by ureaplasmas. 140 vaginal swabs were collected. The material was subjected to PCR for detection of HPV, Mollicutes, Ureaplasma urealyticum, U. parvum (and serotypes) and other bacteria gynecological importance; qPCR for U. urealyticum and U. parvum was made. PHK transformed by HPV was infected by ureaplasma. Cells were counted and it was done titration of IL1-β, IL-6 and TNF-α. HPV, Mollicutes, U. parvum, serotypes 1 and 6 U. parvum, T. vaginalis and G. vaginalis, and some socioeconomic factors were associated with cervical injury. Besides this, it was detected higher load U. parvum among women with injury. There was decrease in cell number and increased release of IL-6 and TNF-α in infected groups. With the results of this study, we found an association among HPV and ureaplasmas at the beginning of cervical lesions, but more studies are needed to enhance this hypothesis. Câncer cervical Cell growth curve Cervical câncer Cervical injury Curva de crescimento celular HPV HPV IL-1β IL-1β IL-6 IL-6 Lesão cervical PCR PCR Primary Human Keratinocytes (PHK) qPCR qPCR Queratinócitos primário humano (PHK) TNF-α TNF-α Ureaplasmas Ureaplasmas
446	Isolement et caractérisation de saponosides extraits de deux plantes médicinales : Cyclamen africanum, Zygophyllum cornutum et évalution de leur activité anti-inflammatoire / Isolation and characterization of two saponosides extracts herbs Cyclamen africanum, Zygophyllum cornutum and assessment of their anti-inflammatory activity Betina-Bencharif, Soumeya 13 October 2014 (has links) L’apparition de plusieurs maladies, telles que le cancer, le diabète, l'hypertension artérielle et la propagation d'infections de type virus mutagènes peuvent être liées à la qualité et au mode de vie que nous menons aujourd’hui. En effet, plusieurs études sur les facteurs déclenchant ces maladies dites "morbides" à long ou à court terme, sont liées au stress et à la qualité des aliments consommés, qu'ils soient d'origine végétale ou animale. Ces maladies deviennent un phénomène courant, elles touchent différentes races et toutes les catégories de la société. D'après les recherches ethnobotaniques, les substances d’origine naturelle, ont permis à des civilisations de survivre à des maladies mortelles. A titre d'exemple, on retrouve ainsi des références à des périodes de fièvre paludique en Chine et à des symptômes de cette maladie dans le «Huangdi Neijiang» Le Canon de Médecine datant des environs du premier siècle avant notre ère, plus de 2000 ans, qui relate de l'emploi de plantes médicinales, pour soulager les fièvres (Desgrouas et al., 2014).Vers 186 avant J.-C. apparaît, dans certaines régions de Chine, l'utilisation en tisane, du Qing hao su, appelé plus tard artémisinine en Occident et extrait d'une plante médicinale utilisée comme antipyrétique appelée "Qing hao", Artemisia annua ou Armoise annuelle. L'artemisinine bloque une enzyme qui permet au parasite de pomper le calcium et l'empêche ainsi de se développer. Au jour d'aujourd'hui l’Artemisinin-based combination therapy, en français Thérapie combinée à base d'artémisinine et en sigle ACT, est une thérapie et une prévention tertiaire dans les cas de paludisme simple.Dans cette optique notre étude vient s'ajouter à une longue série d'études menées sur les plantes médicinales et les substances naturelles extraites. Elle a pour objectif de révéler de nouvelles biomolécules, de mettre en évidence leurs activités biologiques grâce à des techniques de biotechnologies d'une part. D'autre part ces investigations permettront de valoriser les ressources naturelles qui se distinguent par leur endémicité.Pour se faire, notre choix s'est porté sur deux plantes médicinales endémiques à l'Algérie Cyclamen africanum Boiss. & Reuter et Zygophyllum cornutum Coss. , après une recherche ethnobotanique sur la pharmacopée traditionnelle du Nord de l'Afrique, et qui a révélé l’efficacité de ces plantes dans les problèmes inflammatoires minimes chez les autochtones, nous avons entrepris des investigations pharmaco- biochimiques.Ces dernières nous ont permis d'isoler : cinq composés à partir de l'extrait méthanolique des racines de l'espèce Cyclamen africanum Boiss. & Reuter, deux nouvelles saponines triterpéniques de type Oleanane, Afrocyclamin A et B (1, 2), ainsi que trois saponines triterpénoïdes connus sous le nom de lysikokianoside (3), deglucocyclamin I (4) et de son dérivé d'acide dicrotalique (5); et Sept saponosides connus à partir de l'extrait méthanolique de la plante entière de Zygophyllum cornutum Coss., ces saponosides sont de type ursane, ce type de triterpène est rapporté dans cette espèce pour la première fois et peuvent être considérés comme un marqueur chimio-taxonomique (chemotype) du genre Zygophyllum. Les structures ont été élucidées, sur la base de l'analyse des spectres de l'expérience RMN-1D et RMN- 2D (COSY, TOCSY, NOESY, HMBC et HSQC) et spectrométrie de masse en source FAB mode ion négatif. Des activités biologiques, des fractions saponosidiques Fr.1 et Fr.2, ont été testées sur des lignées de Rats mâles et femelles, de la race Winstar pour évaluer l'activité anti inflammatoire.La fraction saponosidique Fr.1 de Cyclamen africanum à la dose 5 mg, a montré un effet significatif sur l'inflammation causé par la carragénine, en réduisant l'oedème et la réponse immunitaire, qui s'est traduite par la concentration des protéines de la réponse inflammatoire (PRI) à travers leurs action sur les pro-médiateurs de l'inflammation (COX-2, PGE2, TNF -α, iNOS). / The appearance of several diseases, such as cancer, diabetes, high blood pressure and spread of infections mutagenic virus type can be linked to the quality and lifestyle that we lead today. Indeed, several studies on the factors triggering these so-called "morbid" long-or short-term illnesses are related to stress and quality of food consumed, whether of plant and animal origin. These diseases are becoming a common occurrence, they affect different races and all classes of society. According ethnobotanical research, naturally occurring substances, allowed civilizations to survive deadly diseases. For example, we thus find references to periods of malarial fever in China and one of the symptoms of this disease in the "Huangdi Neijiang" The Canon of Medicine dating from around the first century BC, more than 2000 years, which relates to the use of herbal medicines to relieve fevers (Desgrouas et al., 2014).Around 186 BC appears, in some parts of China, the use in herbal tea, Qing hao su, later known as artemisinin in the West and extracted from a medicinal plant used as antipyretic called "Qing hao" Artemisia annua or annual wormwood. Artemisinin blocks an enzyme which enables the parasite to pump calcium and prevents it from developing. As of today the Artemisinin-based combination therapy in French Combination therapy of artemisinin and ACT acronym, is a therapy and tertiary prevention in cases of uncomplicated malaria.From this perspective our study adds to a long series of studies on medicinal plants and natural substances extracted. It aims to reveal new biomolecules, highlighting their biological activities through techniques of biotechnology on the one hand. Moreover, these investigations will develop natural resources that are characterized by endemic.To do this, our choice is focused on two endemic medicinal plants in Algeria Cyclamen africanum Boiss. & Reuter and Zygophyllum cornutum Coss. After an ethnobotanical research on traditional medicine in Northern Africa, which showed the effectiveness of these plants in minimal inflammatory problems among Aboriginal, we undertook biochemical pharmacological investigations.The latter allowed us to isolate, five compounds from the methanol extract of the roots of the species Cyclamen africanum Boiss. Reuter & two new oleanane triterpene saponins type, Afrocyclamin A and B (1, 2) and three triterpenoid saponins known lysikokianoside of (3), deglucocyclamin I (4) and its derivative dicrotalique acid (5) September and known from the methanol extract saponins from the whole plant of Zygophyllum cornutum Coss. these saponins are ursane type, type triterpenes are reported in this species for the first time and can be considered a chemotherapy marker Taxonomic (chemotype) of Zygophyllum kind. The structures were elucidated on the basis of the analysis of NMR spectra of the experience-1D and 2D-NMR (COSY, TOCSY, NOESY, HSQC and HMBC) and mass spectrometry method negative ion FAB source. The biological activities of saponosidiques FR.1 and Fr.2 fractions were tested on lines of male and female rats of the Winstar rats to evaluate the anti-inflammatory activity. The saponosidique fraction FR.1 Cyclamen africanum the 5 mg dose, showed a significant effect on inflammation caused by carrageenan, reducing edema and immune response, which resulted in the concentration of protein the inflammatory response (PRI) through their action on the pro-inflammatory mediators (COX-2, PGE2, TNF -α, iNOS). The fraction of Fr.2 saponosidique Zygophyllum dose 20 mg did not show a significant effect on inflammation in general. Cyclamen africanum Zygophyllum cornutum Activité anti inflammatoire Saponines triterpéniques RMN 1D RMN 2D Spectrométrie de masse Anti-inflammatoires (AINS) Médiateurs pro-inflammatoire (COX-2) PGE2 TNF -α INOS Cyclamen africanum Zygophyllum cornutum Anti inflammatory activity Saponins triterpene 1D and 2D NMR Mass spectrometry Protein inflammatory response (PRI) Anti-inflammatory drugs (NSAIDs) Pro-inflammatory mediators COX-2 PGE2 TNF -α INOS 615.3
447	Die Bedeutung löslicher TNF-Familienmitglieder für die multiple Sklerose Ehrlich, Stefan 13 June 2006 (has links) Bei Autoimmunkrankheiten wie der Multiplen Sklerose (MS) kommt es zu einer fehlgesteuerten Immunantwort mit Aktivierung und Persistenz autoreaktiver T-Zellen. Apoptose-regulierende Mechanismen wie das CD95-Rezeptor/CD95-Ligand- und TRAIL-Rezeptor/TRAIL-System könnten dabei eine wichtige Rolle spielen. Die lösliche Form des CD95-Rezeptor (sCD95) kann an CD95L binden und so die Apoptose aktivierter T-Zellen verhindern. Die systemische Blockade von TRAIL führt zur Exazerbation von Autoimmunerkrankungen in Tierversuchen. In der vorliegenden Arbeit wurden deshalb die Expression, Regulation und Bedeutung sowohl von sCD95 als auch von löslichem TRAIL (sTRAIL) und membranständigem TRAIL bei gesunden Probanden und Patienten mit schubförmig remittierender MS (RRMS) untersucht. Zytokine wurden mit ELISAs, Zelloberflächenproteine sowie Apoptose im Durchflusszytometer gemessen. Die Untersuchungen mit magnetisch gereinigten humanen Leukozytensubpopulationen und Zelllinien zeigten, dass sCD95 lediglich von zelltyp-spezifisch aktivierten humanen T-Zellen, sezerniert wird. TRAIL wurde vor allem von Monozyten, die mit IFN-beta stimuliert waren, sezerniert und auf der Zelloberfläche exprimiert. Zellkulturüberstände, die sTRAIL enthielten, lösten Apoptose in suszeptiblen Tumorzellen aus. TRAIL führte zu einer signifikanten Inhibition der Proliferation und der Produktion von Th1- und Th2-spezifischen Zytokinen bei humanen (auto)antigenspezifischen T-Zellen. Weder für die sCD95- noch für die TRAIL-Expression wurden Unterschiede zwischen RRMS-Patienten und gesunden Probanden nachgewiesen. Die Ergebnisse dieser Arbeit zeigen ein komplexes Regulations- und Expressionsmuster von sCD95 und TRAIL, ohne jedoch Anhaltspunkte für Unterschiede zwischen MS-Patienten und Gesunden zu liefern. Es ergaben sich wichtige Hinweise darauf, dass der protektive immunomodulatorische Effekt einer systemischen IFN-beta-Therapie bei MS durch TRAIL vermittelt werden könnte. / Autoimmune disorders such as Multiple Sclerosis (MS) are characterized by an aberrant immune response with activation and persistence of autoreactive T-cells. Apoptosis-regulating mechanism such as the CD95-Rezeptor/CD95-Ligand- and the TRAIL-Rezeptor/TRAIL-System may play a major role in this process. The soluble CD95 receptor (sCD95) can bind to CD95L and subsequently inhibit apoptosis of activated T-cells. The systemic blockade of TRAIL leads to the exacerbation of autoimmune disease in animal experiments. In this work I investigated the expression, regulation and significance of sCD95, soluble TRAIL (sTRAIL) and membrane-bound TRAIL in patients with remitting-relapsing MS (RRMS), and in healthy controls. Cytokines were measured by ELISA, membrane bound proteins and apoptosis were measured by flow cytometry. The experiments with magnetically sorted human leucocyte subpopulations and cell lines showed, that only cell-type specific activated human T-cells secrete sCD95. Both forms of TRAIL were expressed by monocytes stimulated with IFN-beta. Cell supernatants containing sTRAIL induced apoptosis in susceptible tumour cells. Furthermore TRAIL inhibited proliferation of (auto)antigen-specific T cells and the production of Th-1 and Th-2 specific cytokines. There were no differences in the expression of sCD95 and TRAIL between RRMS patients and healthy controls. This work shows a complex regulation pattern of sCD95 and TRAIL without being able to detect differences between MS patients and healthy controls. However, results point out that TRAIL could be an important mediator of the immunomodulatory effects of systemic IFN-beta therapy in MS. Multiple Sklerose Apoptose sCD95 IFN-beta T-Zelle B-Zelle Monozyt Multiple Sclerosis Apoptosis sCD95 IFN-beta T-cell B-cell Monocyte 610 Medizin 33 Medizin YG 6004 YG 6018 YG 6021 ddc:610
448	Arthritisinduktion durch Immunität gegen ein systemisch exprimiertes Autoantigen Schubert, David 01 June 2005 (has links) Ungefähr 1% der Bevölkerung der westlichen Welt leidet an rheumatoider Arthritis (RA). In einem T-Zellrezeptor transgenen Mausmodell, dem K/BxN Modell, wird die ubiquitär exprimierte Glukose-6-phosphat Isomerase (G6PI) von autoreaktiven T- und B-Zellen erkannt. Diese Mäuse entwickeln spontan eine antikörpervermittelte Arthritis, die viele Gemeinsamkeiten mit der humanen RA aufweist. In dieser Arbeit wurde untersucht, ob die Immunisierung mit G6PI eine Arthritis auch in nicht-transgenen Mäuse induzieren kann. Die Immunisierung mit heterologer humaner G6PI führte zur Entwicklung einer peripheren symmetrischen Polyarthritis in über 95% der DBA/1 Mäuse. Damit konnte zum ersten Mal gezeigt werden, dass eine Immunreaktion gegen ein systemisches exprimiertes Antigen zur einer organspezifischen Erkrankung in normalen nicht-transgenen Mäusen führt. Die Tiere entwickeln nach 9 Tagen eine Arthritis, die bis Tag 15 ihr Maximum erreicht hat und dann langsam abnimmt. Histologisch ist die Arthritis durch eine frühe Synovitis charakterisiert, gefolgt von massiven Erosionen des Knorpel und Knochens und anschließenden Reparaturprozessen, inklusive Fibrose. Obwohl die Tiere hohe Antikörpertiter entwickeln, kann die Arthritis nicht durch aufgereinigte Antikörper kranker Mäuse transferiert werden. Trotzdem spielen Antikörper eine große Rolle, da FcR-gamma-Kette defiziente Mäuse eine Arthritis mit geringer Inzidenz und mildem Verlauf entwickeln. Die Depletion der CD4 positiven Zellen verhindert die Entwicklung der Arthritis völlig, und eine Depletion während der Erkrankung führt zur schnellen Heilung. Daneben ist für die Entwicklung der Arthritis auch das Komplementsystem und TNF-alpha entscheidend, was durch Depletion von C5 bzw. durch Blockade von TNF-alpha gezeigt wurde. Zusätzlich wurde die Rolle der G6PI bei der Pathogenese der RA im Menschen untersucht. RA-Patienten zeigten keine erhöhte Frequenz von CD4 positiven T-Zellen, die nach Restimulation mit G6PI TNF-alpha oder IFN-gamma produzierten. Außerdem konnten keine erhöhten anti-G6PI Titer in Patienten mit RA oder anderen rheumatischen Erkrankungen detektiert werden. / About 1% of the of the population of the western world suffers from rheumatoid arthritis (RA). In a T-cell receptor transgenic mouse model, the K/BxN model, the ubiquitously expressed glucose-6-phosphate isomerase (G6PI) is recognized by autoreactive T- and B-cells. These mice do develop an antibody dependent arthritis which show a lot of features of human RA. In this study it was examined whether arthritis could be induced in normal non-transgenic mice by immunization with G6PI. Immunization with heterologous human G6PI induces a symmetric polyarthritis in over 95% of DBA/1 mice. Therewith showing for the first time that an immune reaction against an systemic expressed antigen will lead to the development of an organ specific disease in normal non-transgenic mice. The mice develop arthritis 9d after immunization, reach their maximum at d15 and then arthritis slowly resolve. Histologically, the disease is characterized by early synovitis followed by massive cartilage destruction and erosions of the bones and later repair processes including fibrosis. Although antibody titers in the mice are high, transfer of purified anti-G6PI antibodies of sick mice alone do not transfer disease. Anyway, antibodies seem to play a major role since FcR-gamma-chain deficient mice develop disease with a much lower frequency and reduced severity. Depletion of CD4 positive T cells completely prevents disease and depletion during disease leads to an rapid resolution of arthritis. Aside this, complement and TNF-alpha is critical for the development of arthritis, which could shown by depletion of C5 and blockade of TNF-alpha. In addition, the role of G6PI in the pathogenesis of RA in humans was examined. RA patients do not show a higher frequency of CD4 positive T-cells which produce TNF-alpha and IFN-gamma after restimulation with G6PI. Furthermore, no elevated anti-G6PI titers could be detected in RA patients and in patients with other rheumatic diseases. Rheumatoide Arthritis Antikörper T-Zellen Autoimmunerkrankungen Tiermodelle Glukose-6-phosphat Isomerase (G6PI) TNF-alpha Komplement T-cells rheumatoid arthritis autoimmune disease animal models glucose-6-phosphat isomerase (G6PI) antibodies TNF-alpha complement 570 Biowissenschaften, Biologie 32 Biologie YC 9504 YC 9513 YC 9522 YC 9560 ddc:570
449	Einfluß von Genen der MHC-Klasse II und anderer polymorpher Gene auf Epidemiologie und klinische Manifestationen der Plasmodieninfektion May, Jürgen 04 December 2001 (has links) Die Infektion mit dem Erreger der Malaria tropica, Plasmodium falciparum, verläuft individuell unterschiedlich. Während manche der Infizierten rasch an einer komplizierten Malaria versterben, zeigen andere keinerlei Symptomatik, obwohl jahrelang eine Parasitämie besteht. Was diese Individuen voneinanderen unterscheidet, ist weitgehend unbekannt. Morbidität und Mortalität der Erkrankung sind von der Auseinandersetzung zwischen Wirt und Parasit abhängig, die von exogenen und endogenen Faktoren beeinflußt wird. Unter den endogenen Faktoren spielen die genetischen Determinanten, die sowohl an angeborenen als auch an erworbenen Resistenz- und Immunmechanismen beteiligt sind, eine besondere Rolle. In den hier zusammengefaßten Arbeiten wurden als Determinanten der angeborenen Resistenz gegenüber Malaria die Sichelzellanämie, Alpha-Thalassämie, G6PD-Mangel und der HLA-Klasse-II-Polymorphismus und als genetische Einflußfaktoren von erworbenen Immunmechanismen Varianten des TNF-Promotors, von ICAM-1 und iNOS untersucht. Die Arbeiten unterstützen die Hypothese, daß die Interaktion von Mensch und Plasmodien zu einer ständigen gegenseitigen Beeinflussung und Anpassung geführt hat. Die koevolutonäre Veränderung der Genome der beiden Organismen ist wahrscheinlich mitverantwortlich für die unterschiedliche geographische Verteilung von Genvarianten sowohl des Menschen als auch der Plasmodien und scheint auch heute noch Teil einer komplexen und dynamischen Anpassung von Wirt und Parasit zu sein. / The manifestation of an infection with Plasmodium falciparum, the pathogen of malaria, is individually different. Some indiviuals have a high risk of developing severe malaria, whereas others remain asymptomatic despite a long-lasting parasitemia. The basis of these differences is unknown. Morbidity and mortality of malaria are dependent on the interaction between the host and the parasite which is influenced by exogenic and endogenic factors. The latter are determined by genetic elements involved in innate and acquired mechanisms of resistance and immunity. The studies summerized here address genetic determinants of innate resistance against malaria (sickle cell trait, alpha-thalassemia, G6PD deficiency, blood groups and HLA class II alleles) and those of acquired immunity (variants of the TNF promoter, ICAM-1, and iNOS). The results support the view that the interaction between humans and plasmodia has led to continuous mutual influences and adaptations. Probably, the co-evolution of the genomes of both organisms is jointly responsible for the different geographical distribution of parasitic and human gene variants. This process seems to be part of an ongoing complex and dynamic adaptation of the host and the parasite. ICAM-1 Malaria MHC Plasmodium falciparum HLA TNF iNOS Sichelzellanämie Alpha-Thalassämie G6PD-Mangel Gabun Nigeria ICAM-1 malaria MHC Plasmodium falciparum HLA sickle cell anemia alpha thalassemia G6PD deficiency TNF iNOS Gabun Nigeria 610 Medizin 33 Medizin XD 9500 ddc:610
450	Beurteilung des therapeutischen Potenzials von intraperitoneal injiziertem Metallothionein-II im ischämischen Schlaganfallmodell an der Maus / Assessment of the Therapeutic Potential of intraperitoneal Metallothionein-II Application in Focal Cerebral Ischemia in Mouse Eidizadeh, Abass 07 March 2019 (has links) No description available. 610 Schlaganfall MCAO Metallothionein Ischämie Mausmodell TNF RT-PCR Inflammation Neurologie Zerebrale Ischämie Therapie Metallothionein Cerebral ischemia Mouse model MCAO Stroke Inflammasom Inflammation TNF RT-PCR Ischemic Neurology GOK-MEDIZIN Pharmakotherapie (PPN619875534) Pathobiochemie {Medizin} (PPN619875348) Humanmedizin

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