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Molekulare Mechanismen einer Yersinia enterocolitica induzierten WirtszellaktivierungSchmid, Yvonne, January 2005 (has links)
Tübingen, Univ., Diss., 2005.
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The role of interleukin-8 in the immunopathogenesis of HIV-1 disease and tuberculosisMeddows-Taylor, Stephen 27 May 2014 (has links)
Interleukin-8 (IL-8), a member of the C-X-C chemokine subfamily, is an important
chemoattractant and cellular activator. This study was conducted to determine the role of IL-8
in the immunopathogenesis of HIV-I disease and tuberculosis.
The first section involved determining the effect of infection with HIV-1, Mycobacterium
tuberculosis and co-infection with both of these organisms on IL-8 j_ roduction in vivo. This was
monitored by the determination of levels of serum or plasma EL-8 and peripheral cell-associated
IL-8, assessing peripheral mononuclear (PBMC) and polymorphonuclear (PMN) cell capacity to
produce IL-8 spontaneously or in response to various stimuli, and the detection of constitutive
IL-8 mKNA expression in purified subsets of mononuclear cells. Results show that whereas there
is evidence of detectable levels of cell-associated EL-8 (mKNA and protein) in peripheral cells of
healthy individuals, this is largely lost in the disease states studied. Coupled with this was
significantly increased circulating levels of EL-8 in serum and plasma found in HIV-1 infected
individuals with or without concomitant pulmonary TB. On the other hand, the capacity of PBMC
to produce IL-8 spontaneously ex vivo was enhanced in HIV-1 and TB patients and many of the
HFV/TB group, but their corresponding capacities to respond to various stimuli was significantly
diminished when compared to that of the normal donors. The release of IL-8 from PMN in the
presence of an agonist was diminished mainly in individuals with pulmonary TB, which was
further exacerbated by the presence of HIV-1 infection.
HIV-1-infected individuals have an increased incidence of bacterial infections which could
be related to defective functioning of PMN. The second section was aimed at detecting PMN
abnormalities in HIV and I-HV/TB patients by monitoring EL-8-induced p-glucuronidase release
and PMN chemotaxis in response to IL-8. IL-8-induced (I-glucuronidase release from PMN of
normal individuals and TB patients occurred in a dose-dependent manner. In contrast, PMN from
HTV-1 infected individuals, whether co-infected with M tuberculosis or not, showed a reciprocal
response in that increasing IL-8 concentrations resulted in decreased enzyme release. This
reciprocal slope of the IL-8 dose-response curve was altered for the majority of HIV-1 positive
individuals tested irrespective of their CD4+ cell counts. In addition, PMN chemotaxis in response
to IL-8 was also found to be significantly impaired in a group of HIV-1 infected patients coinfected
w ithM tuberculosis when compared to healthy individuals.
The third section of the study involved analysing the expression of the PMN cell surface
markers, FcyRIII (CD 16), and the two human IL-8 receptors, designated IL -8RA and 1L-8RB.
FcyRIII (CD 16) expression on the surface of PMN was significantly reduced in HIV-1
seropositive patients with pulmonary tuberculosis when compared to those individuals with either
disease alone or healthy blood donors. A significant reduction in the percentage of PMN
expressing IL-8RA and IL-8RB and in their respective fluorescence intensities was found in TB,
HIV, and HTV/TB groups when compared to that obtained for the ND group. IL-8RA intensity
of fluorescence was significantly decreased in the HTV/TB group when compared to the TB and
HIV groups indicating a further down-regulation of IL-8RA expression owing to dual infection.
On the other hand, IL-8RB fluorescence intensity was substantially reduced on PMN from
patients with pulmonary TB and to a greater degree in those patients co-infected with HIV-1 and
M. tuberculosis. Having found a reduction in the expression of both IL-8 receptors on PMN in
all the infection groups, cellular events following the binding of IL-8 to IL-8 receptors on PMN
isolated from dually infected patients, the group which showed the greatest reduction in IL-8
expression was analysed. Results indicated that the impairment of DL-8-dependent PMN functions
such as degranulation and chemotaxis was associated with the reduced expression of IL-8
receptors on these cells.
Increased circulating levels of IL-8 in HIV-1 infection and a diminished cellular capacity
to produce IL-8 as shown in this study may have important implications for antimicrobial defences
and normal immune processes. A dysregulated production of IL-8 in vivo is likely to play a role
in the pathogenesis of HIV-1 disease, pulmonary tuberculosis, and dual infections with both
organisms. In addition, cellular responses dependent on specific receptor engagement and the
subsequent translation of signal transducing events that lead to phagocyte effector functions are
clearly impaired in IL-8 receptor deficient phagocytes. Abnormal PMN functioning in HTV-1
infected individuals, as shown here by defective degranulation and chemotactic responses, have
important implications in the pathogenesis of HIV-1 infection in terms of their ability to clear
secondary microbial infections. Future attempts should be aimed at defining the mechanisms that
bring about these changes in order to contribute to a greater understanding of the mechanisms that
lead to an enhanced risk of superinfections in immunosuppressed individuals.
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Analysis of Interieukin-8 Gene Promoter function in Human Osteoblast-like Cells : Regulation by Ca^<2+>-signaling and Cyclosporin AMITSUYAMA, Hirohito, KAMBE, Fukushi, MURAKAMI, Ryuichiro, ISHIGURO, Naoki, SEO, Hisao 12 1900 (has links)
国立情報学研究所で電子化したコンテンツを使用している。
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Klinische Wertigkeit und pathophysiologische Aspekte der Serumparameter Procalcitonin, Interleukin-8 und Interleukin-18 bei akuter PankreatitisBaumgart, Katja. January 2001 (has links)
Ulm, Univ., Diss., 2001.
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The effect of glycosaminoglycans on cytokine-mediated inflammatory cell recruitmentRamdin, Lara S. P. January 1998 (has links)
No description available.
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Einflussfaktoren auf Interleukin-8-Konzentrationen in Plasma und lysiertem Vollblut beim NeugeborenenSiedler, Diana, January 2007 (has links)
Tübingen, Univ., Diss., 2007.
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The effects of pseudomonas aeruginosa pyocyanin on interleukin-8 expression in bronchial epithelium and therapeutic implications in bronchiectasis /Pan, Ninyuan. January 2006 (has links)
Thesis (M. Res.)--University of Hong Kong, 2006.
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Leukocyte sequestration associated with inflammation : mechanisms and modulations /Nyhlén, Kristina January 2003 (has links) (PDF)
Diss. (sammanfattning) Linköping : Univ., 2003. / Härtill 4 uppsatser.
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The immunology and infection of the cystic fibrosis lungDrummond Massengale, Andrea Rene. January 1900 (has links)
Thesis (Ph. D.)--West Virginia University, 1999. / Title from document title page. Document formatted into pages; contains xi, 131 p. : ill. Vita. Includes abstract. Includes bibliographical references.
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Einfluss von Stickstoffdioxid auf die Zytokininduktion nasaler Epithelzellen bei Exposition mit dem Hausstaubmilbenallergen Der p 1 / Influence of nitrogen dixoide on the cytokine induction of nasal epithelial cells by exposition with the house dust mite allergen Der p 1Paulus, Michael Georg January 2017 (has links) (PDF)
Stickstoffdioxid ist ein Luftschadstoff, der mit dem Auftreten von allergischen Atemwegserkrankungen assoziiert ist. In dieser Studie wurde ein möglicher proallergischer Effekt von Stickstoffdioxid auf die durch eine Hausstaubmilbenallergie verursachte allergische Rhinitis untersucht. Primärzellkulturen aus nasalen Epithelzellen wurden einer einstündigen Gasexposition mit 0,1 ppm, 1 ppm und 10 ppm Stickstoffdioxid unterzogen, gefolgt von einer Exposition mit dem Hausstaubmilbenallergen Der p 1. Zellkulturen, die einer kombinierten Exposition aus 0,1 ppm Stickstoffdioxid und Der p 1 oder 1 ppm Stickstoffdioxid unterzogen wurden, zeigten eine erhöhte Induktion der Zytokine IL-6 und IL-8. Kein Effekt war bei einer reinen Exposition mit Der p 1 oder einer reinen Gasexposition zu beobachten. Über eine verstärkte Induktion von IL-6 und IL-8 kann Stickstoffdioxid einen proinflammatorischen Einfluss auf das Entzündungsgeschehen der allergischen Rhinitis nehmen und die Entstehung einer Sensibilisierungsreaktion fördern. Ein proinflammatorischer Effekt wurde bereits bei einer Stickstoffdioxidkonzentration von 0,1 ppm nachgewiesen, welche in Ballungsräumen von Industriestaaten regelmäßig erreicht wird. / Nitrogen dioxide is an airborne pollutant which is associated with the prevalence of allergic airway disease. This study investigated a possible proallergic effect of nitrogen dioxide on the allergic rhintis caused by a house dust mite allergy. Primary cell cultures of human nasal epithelial cells were exposed with 0,1 ppm, 1 ppm or 10 ppm nitrogen dioxide for one hour, followed by an exposition with the house dust mite allergen Der p 1. Cell cultures who were exposed with 0,1 ppm or 1 ppm nitrogen dioxide and Der p 1 showed an increase in the induction of the cytokines IL-6 und IL-8. No effect was observed in cells only exposed to Der p 1 or only exposed to nitrogen dioxide. By increasing the production of these cytokines, nitrogen dioxide can possibly enhance the underlying immune response which leads to allergic inflammation and sensitization. A proinflammatoric effect was demonstrated at 0,1 ppm nitrogen dioxide, a concentration which is common in urban areas of industrialized nations.
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