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201	Interoperabilita slovenského mýtného systému se sousedními státy / Interoperabilita slovenského mýtneho systému so susednými štátmi Kačala, Tomáš January 2012 (has links) Abstract: The purpose of this thesis is to provide a complex overview of selection of toll system fees for the usage of charged sections of highways and first class roads in countries Poland, Slovakia, Hungary and Czech Republic in present time. Familiarization with various types of toll systems used in Europe, with legislative preconditions for pricing of road infrastructure in European Union and with basic principles of freight and road transport. A part of thesis is a description of companies' functioning which intermediate payments for the usage of charged road communications. Followed by a proposal of common toll system for countries of Visegrad Four, its technical aspect, price calculation and legislative requirements for its introduction into practice. At the end of thesis there are recommendations and possibilities of this system implementation into commom european toll system.
202	Zpoplatnění dopravní infrastruktury v Běloruské republice / Payments in a transport Infrastructure of the Republic of Belarus Liasun, Alina January 2014 (has links) The thesis is about a transport Infrastructure payments in the selected transport branches of the Republic of Belarus. The first part is about a general description of the transport infrastructure of the country that connects the European countries with the Russian Federation and the Baltic States. Focus on the actual state, quality, development of the infrastructure. The second part - the description of the methods and tools of payment. In connection with a progressive development of road infrastructure and different methods of payment more attention is given to this type of communication. There are several systems of road payment in the world. The first method is based on the principle of time, such as vignettes. Another method is payment before road use (Toll). The first method is not working in Belarus, so the work described the second method. The last part of the thesis is about the payment on the certain types of transport infrastructure in Belarus. Focus on such transport types as rail and road transport, also made attention to the air and river transport.
203	Avaliação do papel da IL-10 nos efeitos anti-inflamatórios do exercício aeróbio na síndrome do desconforto respiratório agudo experimental / Evaluation of the role of interleukin-10 in anti inflammatory effects of aerobic exercise on experimental acute respiratory distress syndrome Oliveira, Nicole Cristine Rigonato de 19 December 2014 (has links) Submitted by Nadir Basilio (nadirsb@uninove.br) on 2016-05-25T16:04:47Z No. of bitstreams: 1 Nicole Cristine Rigonato de Oliveira.pdf: 1240943 bytes, checksum: 14fa67b6692555f3bc76fb1f34186220 (MD5) / Made available in DSpace on 2016-05-25T16:04:47Z (GMT). No. of bitstreams: 1 Nicole Cristine Rigonato de Oliveira.pdf: 1240943 bytes, checksum: 14fa67b6692555f3bc76fb1f34186220 (MD5) Previous issue date: 2014-12-19 / The acute respiratory distress syndrome (ARDS) is a disease characterized by respiratory failure due to an inflammatory response, which has high morbidity and mortality. Several cytokines seem to orchestrate the acute and chronic processes, mainly mediated by toll like receptors (TLRs). The literature demonstrates that aerobic exercise (AE) is capable of decreasing the secretion of pro-inflammatory cytokines in the lungs mediated increased release of interleukin 10 (IL-10), and AE modulate expression of TLRs and antioxidant enzymes. The objective of this study was to evaluate whether the anti-inflammatory effects of AE in an experimental model of intra and extrapulmonary ARDS are mediated by IL-10. For this, the animals were subjected to physical training on a treadmill, moderate for 4 weeks. 24 hours after the last physical test, animals received LPS by intratracheally (it) (10ug / animal) or intraperitoneally (ip) (100ug / animal). After 24 hours, the animals were assessed for the number of cells and pro- and anti-inflammatory cytokines in bronchoalveolar lavage fluid (BAL) and serum were the number of neutrophils in the lung parenchyma and expression of TLR4, TLR7, SOD, ânion and QL in lung homogenates. AE reduced accumulation of neutrophils in the lung parenchyma, so it LPS and LPS ip (p <0.01) and BAL (p <0.01). AE attenuate the levels of proinflammatory cytokines in BAL and serum (p <0.05), as measured by ELISA. AE had levels of anti-inflammatory cytokine IL-10 increased in the serum and BAL (p <0.05). AE also reduced the expression of TLR4 in lung homogenates (p <0.05) and increased the expression of TLR7 in group LPS + AE evaluated by western blotting (p <0.05). The results for the antioxidant enzyme SOD showed a significant increase in the groups submitted to AE. It follows that the impact of reduced LPS-induced ARDS, regardless of etiology, and these effects appear to be mediated by modulation of the AE secretion of anti-inflammatory cytokines, especially IL-10, modulating TLR4 and TLR7 and increased expression of SOD (p <0.05). / A síndrome do desconforto respiratório agudo (SDRA) é uma doença caracterizada pela insuficiência respiratória decorrente a uma resposta inflamatória, que apresenta alta morbi-mortalidade. Diversas citocinas parecem orquestrar os processos agudo e crônico, mediados principalmente por receptores toll like (TLRs). A literatura demonstra que o exercício aeróbio (EA) é capaz de diminuir a secreção de citocinas pró-inflamatórias nos pulmões, mediado pelo aumento da liberação de interleucina 10 (IL-10), além de o EA modular a expressão de TLRs e enzimas antioxidantes. Assim, o objetivo desse estudo foi avaliar se os efeitos anti-inflamatórios do EA em modelo experimental da SDRA intra e extrapulmonar são mediados por IL-10. Para isso, os animais foram submetidos ao treinamento físico em esteira, de intensidade moderada, durante 4 semanas. Após 24 horas ao último teste físico, os animais receberam LPS por via intra-traqueal (it) (10ug/animal) ou por via intra-peritoneal (ip) (100ug/animal). Após 24 horas, os animais foram avaliados para o número de células e de citocinas pró e anti-inflamatórias no fluído do lavado broncoalveolar (LBA) e no soro, número de neutrófilos no parênquima pulmonar e expressão do TLR4, TLR7, SOD, ânion e QL nos homogenatos de pulmão. EA reduziu a acumulação de neutrófilos no parênquima pulmonar, tanto LPS it e LPS ip (p <0,01) e no LBA (p <0,01). EA atenuou os níveis de citocinas pró-inflamatórias no LBA e soro (p <0,05), avaliada por ELISA. EA teve os níveis da citocina anti-inflamatória IL-10 aumentados no soro e LBA (p <0,05). EA também reduziu a expressão de TLR4 nos homogenatos de pulmão (p <0,05) e aumentou a expressão de TLR7 no grupo de LPS + EA avaliada por western blotting (p <0,05). Os resultados para a enzima antioxidante SOD apresentou aumento significante nos grupos submetidos ao EA. Conclui-se que EA reduziu o impacto de SDRA induzida por LPS, independente da etiologia e tais efeitos parecem estar mediados pela modulação do EA na secreção de citocinas anti-inflamatórias, principalmente da IL-10, na modulação de TLR4 e TLR7 e no aumento da expressão de SOD (p<0,05). exercício aeróbio interleucina-10 receptor toll like 4 receptor toll like 7 SOD aerobic exercise acute respiratory distress syndrome interleukin-10 toll like receptor 4 toll like receptor 7 SOD CIENCIAS DA SAUDE
204	Modulation of Tissue Toll-Like Receptor 2 and 4 During the Early Phases of Polymicrobial Sepsis Correlates With Mortality Williams, David L., Ha, Tuanzhu, Li, Chuanfu, Kalbfleisch, John H., Schweitzer, John, Vogt, William, Browder, I. William 01 June 2003 (has links) Objective: To determine whether there was a correlation between induction of polymicrobial sepsis, modulation of tissue Toll-like receptor (TLR) gene, and protein expression and survival outcome. Design: Prospective, randomized animal study. Setting: University medical school research laboratory. Subjects: Age- and weight-matched ICR/HSD mice. Interventions: Sepsis was induced by cecal ligation and puncture (CLP). No-surgery and sham (laparotomy)-operated mice were controls. We also examined tissue TLR2 and TLR4 messenger RNA and TLR4 protein levels in mice treated with an immunomodulator that increases survival in polymicrobial sepsis. In the immunomodulator study, mice were treated with glucan phosphate (50 mg/kg, intraperitoneally) 1 hr before CLP. No-surgery, sham surgery, glucan + no-surgery, sham surgery + glucan, and CLP groups were employed as controls. Measurements and Main Results: Total RNA was isolated from liver, lung, and spleen at 0, 1, 3, 6, 8, and 24 hrs after CLP. TLR gene expression was assessed by reverse transcription-polymerase chain reaction. Tissue TLR4 protein levels were evaluated at 24 hrs by Western blot and immunohistochemistry. CLP sepsis increased (p < .05) liver and lung TLR2 and TLR4 gene expression compared with controls. TLR4 protein concentrations also were increased. Increased TLR2/4 gene and TLR4 protein expression correlated with mortality. Immunoprophylaxis with glucan phosphate increased (p < .001) long-term survival (20% vs. 70%) but inhibited (p < .05) CLP-induced increases in tissue TLR2 and TLR4 messenger RNA expression as well as TLR4 protein expression. Conclusions: Early increases in TLR2/4 gene and TLR4 protein expression correlated with mortality, whereas blunting TLR gene and protein expression correlated with improved long-term survival. This suggests that early up-regulation of tissue TLR2/4 may play a role in the proinflammatory response and pathophysiology of polymicrobial sepsis. cecal ligation and puncture sepsis toll-like receptor Surgery Internal Medicine
205	Valsartan Blocked Alcohol-Induced, Toll-Like Receptor 2 Signaling-Mediated Inflammation in Human Vascular Endothelial Cells Wang, Yushu, Li, Yi, Shen, Qingyu, Li, Xiangpen, Lu, Juan, Li, Xiangping, Yin, Deling, Peng, Ying 01 January 2014 (has links) Background: Alcohol consumption induces inflammatory damage in vessels, and the underlying mechanism is unclear. Valsartan, as one of the angiotensin receptor blockers (ARBs), plays a role in the inhibition of inflammatory reactions in vascular dysfunction. This study is to investigate the role of Toll-like receptor 2 (TLR2) in alcohol-induced inflammatory damage in vascular endothelial cells in vitro and to explore the protective effect of valsartan on alcohol-induced and TLR2-mediated inflammatory damage. Methods: The human umbilical vein cell line (EA.hy926) were exposed to alcohol at 0 to 80 mM for 0 to 48 hours with or without valsartan pretreatment. The expression of TLR2 signaling, including TLR2, tumor necrosis factor receptor associated factor 6 (TRAF-6) and nuclear factor kappa B (NF-κB) p65 were detected by Western blot. The levels of proinflammatory cytokines, tumor necrosis factor-α (TNF-α) and interleukin-6 (IL-6), were determined by ELISA. To confirm the role of TLR2, we functionally up-regulated or down-regulated TLR2 by using TLR2 agonist or TLR2 small interfering RNA (siRNA), respectively. To further investigate the mechanism of alcohol on renin-angiotensin system, we detected the expression of angiotensin II receptor type 1 (AGTR1) in protein levels. Results: The expression of TLR2, TRAF-6, NF-κB p65, and the proinflammatory cytokines, TNF-α and IL-6, were significantly increased after alcohol exposure in EA.hy926 endothelial cells. This was enhanced by TLR2 agonist, and was inhibited by TLR2 siRNA transfection. The pretreatment of valsartan resulted in an inhibition of TLR2 signaling and proinflammatory cytokines. The expression of AGTR1 was up-regulated after alcohol exposure, and was blocked by valsartan pretreatment. Conclusions: TLR2 signaling-mediated alcohol induced inflammatory response in human vascular epithelial cells in vitro, which was inhibited by valsartan. alcohol EA.hy926 Cells toll-like receptor 2 valsartan Internal Medicine
206	Transcriptional Suppression of miR-29b-1/miR-29a Promoter by c-Myc, Hedgehog, and NF-kappaB Mott, Justin L., Kurita, Satoshi, Cazanave, Sophie C., Bronk, Steven F., Werneburg, Nathan W., Fernandez-Zapico, Martin E. 01 August 2010 (has links) MicroRNAs regulate pathways contributing to oncogenesis, and thus the mechanisms causing dysregulation of microRNA expression in cancer are of significant interest. Mature mir-29b levels are decreased in malignant cells, and this alteration promotes the malignant phenotype, including apoptosis resistance. However, the mechanism responsible for mir-29b suppression is unknown. Here, we examined mir-29 expression from chromosome 7q32 using cholangiocarcinoma cells as a model for mir-29b downregulation. Using 5′ rapid amplification of cDNA ends, the transcriptional start site was identified for this microRNA locus. Computational analysis revealed the presence of two putative E-box (Myc-binding) sites, a Gli-binding site, and four NF-κB-binding sites in the region flanking the transcriptional start site. Promoter activity in cholangiocarcinoma cells was repressed by transfection with c-Myc, consistent with reports in other cell types. Treatment with the hedgehog inhibitor cyclopamine, which blocks smoothened signaling, increased the activity of the promoter and expression of mature mir-29b. Mutagenesis analysis and gel shift data are consistent with a direct binding of Gli to the mir-29 promoter. Finally, activation of NF-κB signaling, via ligation of Toll-like receptors, also repressed mir-29b expression and promoter function. Of note, activation of hedgehog, Toll-like receptor, and c-Myc signaling protected cholangiocytes from TRAIL-induced apoptosis. Thus, in addition to c-Myc, mir-29 expression can be suppressed by hedgehog signaling and inflammatory pathways, both commonly activated in the genesis of human malignancies. cholangiocellular carcinoma FRA7H inflammation miRNA sonic toll-like receptor
207	Overexpression of TLR2 and TLR4 Susceptibility to Serum Deprivation-Induced Apoptosis in CHO Cells Fan, Wei, Ha, Tuanzhu, Li, Yan, Ozment-Skelton, Tammy, Williams, David L., Kelley, Jim, Browder, I. William, Li, Chuanfu 25 November 2005 (has links) We examined the effect of overexpression of TLR2 and TLR4 on apoptosis. TLR2 and TLR4 transfected CHO cells were subjected to serum deprivation for 0, 24, and 48 h. CHO cells served as control. The survival was 80.4% and 66.8% in CHO cells, 73.8% and 47.6% in TLR2/CHO, and 70.5% and 53.0% in TLR4/CHO, respectively. Flow cytometry examination suggested that apoptotic cells were 7.17% and 32.91% in control CHO cells, 29.0% and 64.6% in TLR2/CHO, and 41.4% and 64.6% in TLR4/CHO, respectively. The levels of FasL and caspase-8 activity in TLR2/CHO and TLR4/CHO cells were significantly higher than that of CHO cells. Transfection of dominant negative FADD into TLR2/CHO and TLR4/CHO cells significantly reduced apoptosis. Our results suggest that overexpression of TLR2 and TLR4 in CHO cells sensitizes the cells to serum deprivation-induced apoptosis and that the mechanisms are involved in the death receptor-mediated signaling pathway. apoptosis serum deprivation signaling transduction toll-like receptors Surgery
208	Wirkmechanismus neuartiger Adjuvantien bei einer Herpes-Virus-Vakzine: Welche Rolle spielen NK-Zellen? / Mechanism of action of novel herpes vaccine adjuvants: the relative role of NK cells Eisermann, Philip January 2012 (has links) (PDF) 2,3-Dipalmitoyl-S-Glycerylcystein (Pam2Cys), ein Toll-like-Rezeptor 2 (TLR2)-Ligand, aktiviert dendritische Zellen und erhöht die Expression von HLA-DR auf deren Zelloberfläche. Natürliche Killerzellen (NK-Zellen) können über die Ausschüttung von Zytokinen das erworbene Immunsystem stimulieren. Zudem weist die Entdeckung von HLA-DR auf NK-Zellen, besonders auf CD56bright-NK-Zellen, auf eine Verbindung zwischen angeborenem und erworbenem Immunsystem hin. Gekoppelt an ein immundominantes Peptidepitop aus dem Glykoprotein D des Herpes-Simplex-Virus (HSV) Typ 2, wurde Pam2Cys in dieser Arbeit als potentieller lipopeptidbasierter HSV-Impfstoff eingesetzt, um die Effekte dieser Vakzine auf NK-Zellen zu untersuchen. Die Einflüsse der Vakzine wurden anhand der CD69-, HLA-DR- und TLR2-Expression auf und in NK-Zellen nach Inkubation mit Pam2Cys untersucht. Die Analyse der Gesamt-NK-Zellpopulation ließ nur mit Hilfe der quantitativen Real-Time-PCR einen signifikanten Anstieg der TLR2-Expression erkennen, jedoch nicht durchflusszytometrisch. Inkubierte NK-Zellen zeigten deutlich mehr HLA-DR auf der Zelloberfläche, als unstimulierte NK-Zellen. Die Untersuchung der zwei großen NK-Zellsubpopulationen, CD56bright und CD56dim, ergab, dass stimulierte CD56bright-Zellen wesentlich mehr HLA-DR und TLR2 aufwiesen, als stimulierte CD56dim-Zellen. Die Expression des Aktivierungsmarkers CD69 stieg in der Gesamtpopulation der NK-Zellen nicht in signifikantem Maße an, zeigte jedoch eine Zunahme nach Inkubation mit den Pam2Cys-Molekülen. Die Aufnahme der Lipopeptide in NK-Zellen wurde mit der konfokalen Mikroskopie bestätigt. Diese Ergebnisse zeigen, dass die hier verwendete HSV-Vakzine von NK-Zellen aufgenommen wird und sie die Ausbildung von Oberflächenrezeptoren auf diesen Zellen moduliert. Insbesondere die Expressionssteigerung von HLA-DR auf CD56bright-NK-Zellen deutet auf die Fähigkeit dieser Zellen hin, Antigene zu präsentieren und stellt einen weiteren Mechanismus vor, der eine impfstoffbezogene Immunantwort unterstützen kann. Die vorliegende Arbeit bildet eine Basis für weiterführende Studien an NK-Zellen hinsichtlich der Antigenpräsentation im Allgemeinen und der Antigenpräsentation nach Stimulation durch eine Vakzine im Besonderen. / The Toll-like receptor 2 (TLR2) ligand 2,3-Dipalmitoyl-S-Glycerylcystein (Pam2Cys) enhances the surface expression of HLA-DR on dendritic cells and activates them. Natural killer cells (NK cells) may stimulate the adaptive immune system via the production of cytokines. Furthermore the detection of HLA-DR on NK cells, especially on CD56bright NK cells, hints at a connection between innate and adaptive immunity. In this study Pam2Cys was used as a potential lipopeptide-based HSV vaccine attached to an immunodominant epitope in herpes simplex virus (HSV) type 2 glycoprotein D. The effects of this vaccine on NK cells were analysed here. Examination of the influence of this vaccine was performed by measuring the expression of CD69, HLA-DR and TLR2 on and in NK cells after incubating them with Pam2Cys. Using quantitative real-time PCR, a significant increase of TLR2-mRNA in the entire NK cell population was detectable; however flow cytometry was not able to confirm these results. Incubated NK cells showed considerably more HLA-DR than unstimulated NK cells. Analysis of the two big NK cell subpopulations, CD56bright and CD56dim, revealed essentially more HLA-DR and TLR2 on stimulated CD56bright cells, compared to stimulated CD56dim cells. Expression of the activation marker CD69 after incubation was not triggered significantly on NK cells altogether; nevertheless an increase could be measured. Confocal microscopy confirmed an uptake of lipopeptides into NK cells. These data demonstrate the surface receptor modulation on NK cells by a potential HSV vaccine and the ability of NK cells to endocytose Pam2Cys. Particularly, the increase of HLA-DR on CD56bright NK cells points at the ability of these cells to present antigens, introducing a new mechanism able to support a potent immune response to a vaccination. This study provides a basis for further work on NK cells in terms of antigen presentation in general and antigen presentation after stimulation by a vaccine in particular. Herpes simplex Adjuvans Toll-like-Rezeptor Pam2Cys ddc:610
209	Ausreifung humaner dendritischer Zellen durch die TLR-Agonisten Poly(I:C) und R848 mit PGE\(_2\). Auswirkungen auf Phänotyp, Zytokinproduktion, Migration und das antigenspezifische Priming von naiven CD8\(^p\)\(^o\)\(^s\) T-Zellen / Maturation of human dendritic cells through TLR agonists poly(I:C) and R848 with PGE\(_2\). Effects on phenotype, cytokine production, migration and the antigen specific priming of CD8\(^p\)\(^o\)\(^s\) t-cells Gierlich, Philipp January 2019 (has links) (PDF) Gegenstand der Arbeit: Es wurde der Einfluss einer Ausreifung dendritischer Zellen mit Poly(I:C), R848 und Prostaglandin E2 (=tlrDCs) zur Verwendung im Rahmen der Tumorvakzine untersucht. Für den Einsatz einer doppelten TLR-Stimulation gibt es zahlreiche zellphysiologische Gründe, wobei PGE2 als Motilitätsförderer eingesetzt wird. Es besitzt negative Teilwirkungen auf die Zytokinsekretion, eine verbesserte Migration stellt aber die wichtigste Stellgröße zur Optimierung der Tumorvakzine dar. Ergebnisse: Für tlrDCs konnte neben einer hohen Fähigkeit zu Migration und Kostimulation eine überlegene Immunstimulation für naive CTLs und TH1/TC1-Antworten in einem antigenspezifischen Primingmodell nachgewiesen werden. Eine Ausreifungsdauer von 16 h erscheint für die Zytokinsekretion der DCs günstig. Es lässt sich eine hohe Wahrscheinlichkeit für die Generation von Central-Memory-T-Zellen und das T-Zell-Homing ins ZNS ableiten. / Subject: This thesis investigated the impact of dendritic cell maturation with poly(I:C), R848 and prostaglandine E2 (=tlrDCs) for use in the context of tumor vaccines. There are several cell-physiological rationales for a dual TLR stimulation whilst PGE2 is acting as a promoter of mobility. It has partially negative effects on cytokine secretion, however improving migration is believed to be the most important variable for optimizing tumor vaccines. Results: Besides their high capacity in migration and co-stimulation tlrDCs showed superior immuno-stimulation for naive CTLs and TH1/TC1 responses in a model of antigen-specific priming. A maturation period of 16 h seemed to be favorable for cytokine secretion of DCs. A good chance for the generation of central memory T-cells and T-cell homing into the CNS can be deduced. Reifung Dendritische Zelle Toll-like-Rezeptoren Tumor Impfstoff ddc:615
210	Development Of An Artificial Neural Networks Model To Estimate Delay Using Toll Plaza Transaction Data Muppidi, Aparna 01 January 2005 (has links) In spite of the most up-to-date investigation of the relevant techniques to analyze the traffic characteristics and traffic operations at a toll plaza, there has not been any note worthy explorations evaluating delay from toll transaction data and using Artificial Neural Networks (ANN) at a toll plaza. This thesis lays an emphasis on the application of ANN techniques to estimate the total vehicular delay according to the lane type at a toll plaza. This is done to avoid the laborious task of extracting data from the video recordings at a toll plaza. Based on the lane type a general methodology was developed to estimate the total vehicular delay at a toll plaza using ANN. Since there is zero delay in an Electronic Toll Collection (ETC) lane, ANN models were developed for estimating the total vehicular delay in a manual lane and automatic coin machine lane. Therefore, there are two ANN models developed in this thesis. These two ANN models were trained with three hours of data and validated with one hour of data from AM and PM peak data. The two ANN models were built with the dependent and independent variables. The dependent variables in the two models were the total vehicular delay for both the manual and automatic coin machine lane. The independent variables are those, which influence delay. A correlation analysis was performed to see if there exists any strong relationship between the dependent (outputs) and independent variables (inputs). These inputs and outputs are fed into the ANN models. The MATLABTB code was written to run the two ANN models. ANN predictions were good at estimating delay in manual lane, and delay in automatic coin machine lane. Delay Artificial Neural Networks Toll plaza Civil Engineering Engineering

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