43 results on '"Roth, Johannes"'
Search Results
2. Phason-elastic energy in a model quasicrystal
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Koschella, Ulrich, Gähler, Franz, Roth, Johannes, and Trebin, Hans-Rainer
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- 2004
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3. Phason elastic constants of a binary tiling quasicrystal
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Koschella, Ulrich, Gähler, Franz, Roth, Johannes, and Trebin, Hans-Rainer
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- 2002
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4. S100A12 (EN-RAGE) in monitoring Kawasaki disease
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Foell, Dirk, Ichida, Fukiko, Vogl, Thomas, Yu, Xianyi, Chen, Rui, Miyawaki, Toshio, Sorg, Clemens, and Roth, Johannes
- Published
- 2003
5. Shock waves in quasicrystals
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Roth, Johannes
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- 2000
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6. Numerical simulation of dislocation motion in an icosahedral quasicrystal
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D. Schaaf, Gunther, Mikulla, Ralf, Roth, Johannes, and Trebin, H.-R
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- 2000
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7. Molecular dynamic studies of atomic jumps in d-Al–Cu–Co
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Bunz, Dietmar, Zeger, Gabriele, Roth, Johannes, Hohl, Martin, and Trebin, Hans-Rainer
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- 2000
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8. Hyperzincaemia and hypercalprotectinaemia: a new disorder of zinc metabolism. (Mechanisms of disease)
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Sampson, Barry, Fagerhol, Magne K, Sunderkotter, Cord, Golden, Barbara E, Richmond, Peter, Klein, Nigel, Kovar, Ilya Z, Beattie, John H, Wolska-Kusnierz, Beata, Saito, Yoshiaki, and Roth, Johannes
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Zinc metabolism -- Diseases - Published
- 2002
9. S100A8/A9-alarmin promotes local myeloid-derived suppressor cell activation restricting severe autoimmune arthritis.
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von Wulffen, Meike, Luehrmann, Veronika, Robeck, Stefanie, Russo, Antonella, Fischer-Riepe, Lena, van den Bosch, Martijn, van Lent, Peter, Loser, Karin, Gabrilovich, Dmitry I., Hermann, Sven, Roth, Johannes, and Vogl, Thomas
- Abstract
Immune-suppressive effects of myeloid-derived suppressor cells (MDSCs) are well characterized during anti-tumor immunity. The complex mechanisms promoting MDSC development and their regulatory effects during autoimmune diseases are less understood. We demonstrate that the endogenous alarmin S100A8/A9 reprograms myeloid cells to a T cell suppressing phenotype during autoimmune arthritis. Treatment of myeloid precursors with S100-alarmins during differentiation induces MDSCs in a Toll-like receptor 4-dependent manner. Consequently, knockout of S100A8/A9 aggravates disease activity in collagen-induced arthritis due to a deficit of MDSCs in local lymph nodes, which could be corrected by adoptive transfer of S100-induced MDSCs. Blockade of MDSC function in vivo aggravates disease severity in arthritis. Therapeutic application of S100A8 induces MDSCs in vivo and suppresses the inflammatory phenotype of S100A9ko mice. Accordingly, the interplay of T cell-mediated autoimmunity with a defective innate immune regulation is crucial for autoimmune arthritis, which should be considered for future innovative therapeutic options. [Display omitted] • S100A8/S100A9-alarmin induces MDSCs in autoimmune arthritis • S100A8-induced MDSC differentiation in vitro suppresses T cell proliferation • Adoptive transfer of MDSCs ameliorates disease severity in arthritis • Blockade of MDSC function aggravates disease severity in arthritis Von Wulffen et al. show that the alarmin S100A8/A9 reprograms myeloid cells to a regulatory phenotype (MDSCs) during autoimmune arthritis dampening T cell functions and disease severity. Isolated S100A8 treatment induces MDSC differentiation with the capacity to suppress T cell proliferation. The adoptive transfer of S100-induced MDSCs attenuates disease symptoms in arthritis. [ABSTRACT FROM AUTHOR]
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- 2023
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10. Biallelic TLR4 deficiency in humans.
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Capitani, Melania, Al-Shaibi, Ahmad A., Pandey, Sumeet, Gartner, Lisa, Taylor, Henry, Hubrack, Satanay Z., Agrebi, Nourhen, Al-Mohannadi, Muneera Jassim, Al Kaabi, Saad, Vogl, Thomas, Roth, Johannes, Kotlarz, Daniel, Klein, Christoph, Charles, Adrian K., Vijayakumar, Vinayan, Karim, Mohammed Yousuf, George, Bruce, Travis, Simon P., Elawad, Mamoun, and Lo, Bernice
- Abstract
Toll-like receptors (TLRs) mediate functions for host defense and inflammatory responses. TLR4 recognizes LPS, a component of gram-negative bacteria as well as host-derived endogenous ligands such as S100A8 and S100A9 proteins. We sought to report phenotype and cellular function of individuals with complete TLR4 deficiency. We performed genome sequencing and investigated exome and genome sequencing databases. Cellular responses were studied on primary monocytes, macrophages, and neutrophils, as well as cell lines using flow cytometry, reporter, and cytokine assays. We identified 2 individuals in a family of Qatari origin carrying a homozygous stop codon variant p.Q188X in TLR4 presenting with a variable phenotype (asymptomatic and inflammatory bowel disease consistent with severe perianal Crohn disease). A third individual with homozygous p.Y794X was identified in a population database. In contrast to hypomorphic polymorphisms p.D299G and p.T399I, the variants p.Q188X and p.Y794X completely abrogated LPS-induced cytokine responses whereas TLR2 response was normal. TLR4 deficiency causes a neutrophil CD62L shedding defect, whereas antimicrobial activity toward intracellular Salmonella was intact. Biallelic TLR4 deficiency in humans causes an inborn error of immunity in responding to LPS. This complements the spectrum of known primary immunodeficiencies, in particular myeloid differentiation primary response 88 (MYD88) or the IL-1 receptor-associated kinase 4 (IRAK4) deficiency that are downstream of TLR4 and TLR2 signaling. [ABSTRACT FROM AUTHOR]
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- 2023
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11. Blindness following severe midfacial trauma – Case report and review.
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Roth, Johannes, Hingst, Volker, and Lenz, Jan-Hendrik
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BLINDNESS ,FACIAL injuries ,FACIAL bones ,EPIDEMIOLOGY ,MAXILLA surgery ,MAXILLOFACIAL surgery ,PLASTIC surgery ,HYDROCORTISONE - Abstract
Abstract: Purpose: Severe trauma of the viscerocranium or neurocranium may result in impaired visual acuity or even blindness. Case based epidemiology, pathomechanism and actual strategies in midfacial trauma for initial therapy and prevention of posttraumatic blindness are discussed. Case and review: A 58-year old patient was treated at our Department of Oral and Maxillofacial Plastic Surgery after his central midface had been hit by a swinging steel girder. Initially he was blind on both eyes. Initial treatment started by applying 24 mg of dexamethasone and omeprazole. During the following 2 weeks, amaurosis persisted on the left eye. On the right eye complete visual acuity was regained. On the basis of data from our Department of Oral and Maxillofacial Plastic Surgery an Odds Ratio of 0.12 was calculated for the combination of blindness and midfacial trauma. Today cortisol therapy is still used. However, hypothermia, anti-Trendelenburg position, and application of mannitol seem to be more effective therapeutic strategies. Erythropoetine and progesterone are promising drugs with neuroprotective, anti-inflammatory as well as anti-oedematous effects. Conclusion: The risk of blindness is higher than expected. Latest findings regarding the neuroprotective effects of erythropoetine or/and progesterone seem to promise a more successful treatment. [Copyright &y& Elsevier]
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- 2012
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12. Preoxygenated hyperventilated hypocapnic apnea-induced radiation (PHAIR) in breast cancer patients
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Roth, Johannes, Engenhart-Cabillic, Rita, Eberhardt, Leo, Timmesfeld, Nina, and Strassmann, Gerd
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BREATH holding , *HYPERVENTILATION , *RADIOTHERAPY , *EPIDEMIOLOGY , *APNEA , *OXYGEN , *BREAST cancer patients , *RESPIRATION - Abstract
Abstract: Introduction: The study was performed to quantify the benefit of preoxygenated hyperventilated hypocapnic apnea-induced radiation (PHAIR) for breath hold (BH) time in patients with breast cancer. Methods and materials: We compared in a single blind study 6 healthy volunteers and 10 breast cancer patients using PHAIR. Both groups were subdivided into two arms, each including 4min eupnea and hyperventilation with 20breaths/min to 19–20mmHG FeCO2 before apnea without (hBH) and with 100% oxygen (ohBH). Apnea times were measured with an in-house breathholding device and an adapted ventilator, and blood and respiration gas parameters through our laboratory. Results: The experiment was well-tolerated by patients without compromising their security. A significant increase in BH was observed upon hBH and ohBH compared to standard breath hold – up to 700% in ohBH. There is evidence that the patients interrupted their breath hold before the actual physiological end. Conclusion: PHAIR is a feasible, safe and recommendable technique that could be used to improve BH for high precision radiotherapy. Further research is necessary to obtain a clinical value for this technique. [Copyright &y& Elsevier]
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- 2011
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13. Phagocyte-specific S100 proteins: a novel group of proinflammatory molecules
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Roth, Johannes, Vogl, Thomas, Sorg, Clemens, and Sunderkötter, Cord
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PHAGOCYTES , *LEUCOCYTES , *LYMPHOCYTES , *INFLAMMATION - Abstract
Three members of the S100 family of calcium-binding proteins comprise a new group of proinflammatory molecules released by phagocytes. A novel inflammatory syndrome defined by extraordinarily high expression of S100A8 and S100A9 confirmed recent observations in vitro demonstrating a role of these proteins during recruitment of leukocytes. S100A12 directly activates endothelial cells, mononuclear phagocytes and lymphocytes through interaction with the receptor for advanced glycation end products. Thus, these S100-proteins are attractive targets to modulate inflammation. [Copyright &y& Elsevier]
- Published
- 2003
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14. L'échographie dans la détection de l'enthésite chez l'enfant : revue systématique de la littérature.
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Rossi-Semerano, Linda, Ravagnani, Viviana, Collado, Paz, Vojinovic, Jelena, Roth, Johannes, Magni-Manzoni, Silvia, Naredo, Esperanza, D'Agostino, Maria Antonietta, and Jousse-Joulin, Sandrine
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ULTRASONIC imaging , *JUVENILE idiopathic arthritis , *LEG , *ACOUSTIC imaging - Abstract
Une revue systématique visant à évaluer l'apport de l'échographie dans la détection de l'enthésite chez les patients porteurs d'arthrite juvénile idiopathique (AJI). Une recherche bibliographique a été menée dans les bases de données PubMed et Embase pour la période comprise entre janvier 1966 et mai 2021 ; les articles qui répondaient aux critères d'inclusion selon la définition de l'enthésite échographique et les propriétés métrologiques étudiées ont été sélectionnés. Nous avons évalué les caractéristiques cliniques de la population cible, le design de l'étude, le type et le nombre d'enthèses examinées, la définition et le système de cotation de l'enthésite échographique ainsi que les propriétés métrologiques définies par le filtre OMERACT (vérité, discrimination et faisabilité). La qualité méthodologique des études a été analysée au moyen de l'échelle QUADAS-2 (Quality Assessment of Diagnostic Accuracy Studies 2). Cinq publications remplissaient les critères d'inclusion (26 à 146 patients et 1 à 10 sites d'enthèse examinés bilatéralement). Toutes les études étaient axées sur les enthèses des membres inférieurs. Les lésions élémentaires incluses dans la définition de l'enthésite chez l'adulte ont été généralement évaluées. Peu d'études ont rapporté la fiabilité de l'échographie et aucune n'a évalué sa sensibilité au changement. Les anomalies échographiques des enthèses étaient visibles chez 9,4 % à 53 % des patients atteints d'AJI et 20 % à 83 % des cas d'arthrite liée à l'enthésite (ERA). Il n'a été retrouvé aucune anomalie significative chez les sujets sains. L'exploration échographique a été faiblement corrélée à l'examen clinique. La qualité globale des études était faible, en raison notamment de l'absence de test de référence. L'échographie est un outil qui affiche une bonne sensibilité pour la détection des anomalies des enthèses dans l'AJI. D'après les données actuelles, il n'existe pas de définition échographique standardisée de l'enthésite dans la population pédiatrique. Par ailleurs, les critères de validité externe et interne de l'échographie n'ont pas été établis. A systematic review to assess the value of ultrasonography (US) for detecting enthesitis in juvenile idiopathic arthritis (JIA). PubMed and Embase databases were searched for articles published from January 1966 to May 2021; we selected those meeting the inclusion criteria according to the US definition of enthesitis and metric properties studied. We assessed the clinical features of the population, study design, the type and number of entheses examined, the definition and scoring system of US enthesitis and metric properties according to the OMERACT filter (truth, discrimination, feasibility). The quality of the studies was evaluated with the Quality Assessment of Diagnostic Accuracy Studies 2. Five publications met the inclusion criteria (26 to 146 patients and 1 to 10 bilaterally examined entheses). All studies focused on lower-limb entheses. The elementary lesions included in the definition of adult enthesitis were generally assessed. Few studies reported US reliability, and none evaluated sensitivity to change of US. US revealed entheseal abnormalities in 9.4 % to 53 % of JIA patients and 20 % to 83 % of enthesitis-related arthritis cases. No significant abnormalities were found in healthy children. US findings were poorly correlated with clinical examination. The overall quality of the studies was low, mainly because of the lack of a reference standard. US is a sensitive tool to detect entheseal abnormalities in JIA. The current evidence highlights that a standardized US definition of enthesitis in children is lacking and US criteria and discriminant validity have not been established. [ABSTRACT FROM AUTHOR]
- Published
- 2024
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15. Alarmins MRP8 and MRP14 Induce Stress Tolerance in Phagocytes under Sterile Inflammatory Conditions.
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Austermann, Judith, Friesenhagen, Judith, Fassl, Selina Kathleen, Petersen, Beatrix, Ortkras, Theresa, Burgmann, Johanna, Barczyk-Kahlert, Katarzyna, Faist, Eugen, Zedler, Siegfried, Pirr, Sabine, Rohde, Christian, Müller-Tidow, Carsten, von Köckritz-Blickwede, Maren, von Kaisenberg, Constantin S., Flohé, Stefanie B., Ulas, Thomas, Schultze, Joachim L., Roth, Johannes, Vogl, Thomas, and Viemann, Dorothee
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- 2015
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16. S100A8/A9: From basic science to clinical application.
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Pruenster, Monika, Vogl, Thomas, Roth, Johannes, and Sperandio, Markus
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NEUTROPHILS , *MULTIPLE sclerosis , *DEMYELINATION , *INFLAMMATORY bowel diseases , *RHEUMATOID arthritis , *ANATOMY - Abstract
Neutrophils and monocytes belong to the first line of immune defence cells and are recruited to sites of inflammation during infection or sterile injury. Both cells contain huge amounts of the heterodimeric protein S100A8/A9 in their cytoplasm. S100A8/A9 belongs to the Ca 2 + binding S100 protein family and has recently gained a lot of interest as a critical alarmin modulating the inflammatory response after its release (extracellular S100A8/A9) from neutrophils and monocytes. Extracellular S100A8/A9 interacts with the pattern recognition receptors Toll-like receptor 4 (TLR4) and Receptor for Advanced Glycation Endproducts (RAGE) promoting cell activation and recruitment. Besides its biological function, S100A8/A9 (also known as myeloid related protein 8/14, MRP8/14) was identified as interesting biomarker to monitor disease activity in chronic inflammatory disorders including inflammatory bowel disease and rheumatoid arthritis. Furthermore, S100A8/A9 has been tested successfully in pre-clinical imaging studies to localize sites of infection or sterile injury. Finally, recent evidence using small molecule inhibitors for S100A8/A9 also suggests that blocking S100A8/A9 activity exerts beneficial effects on disease activity in animal models of autoimmune diseases including multiple sclerosis, systemic lupus erythematosus, rheumatoid arthritis and inflammatory bowel disease. This review will provide a comprehensive and detailed overview into the structure and biological function of S100A8/A9 and also will give an outlook in terms of diagnostic and therapeutic applications targeting S100A8/A9. [ABSTRACT FROM AUTHOR]
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- 2016
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17. W1788 GM-CSF Induced Monocyte Subsets Ameliorates Intestinal Inflammation by Specific Immune Activation.
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Däbritz, Jan, Ehrchen, Jan M., Barczyk, Katarzyna, Varga, Georg, Roth, Johannes, and Foell, Dirk
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- 2010
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18. S1707 The Mediator S100a12 Is Critically Involved in Early Inflammatory Events of Inflammatory Bowel Disease.
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Foell, Dirk, Wittkowski, Helmut, Lüken, Aloys, Däbritz, Jan, Viemann, Dorothee, Heidemann, Jan, Vogl, Thomas, and Roth, Johannes
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- 2009
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19. S1702 GM-CSF Induces Differentiation of Specifically Activated Monocyte Subsets and Cell Death of Proinflammatory-Primed Monocytes.
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Däbritz, Jan, Ehrchen, Jan M., Barczyk, Katarzyna, Roth, Johannes, and Foell, Dirk
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- 2009
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20. T1258 Phagocyte-Specific S100 Proteins Are Activators of Pattern Recognition Receptors and Released During Active Inflammatory Bowel Disease.
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Foell, Dirk, Ren, Zhigang, Wittkowski, Helmut, Daebritz, Jan, Heidemann, Jan, Roth, Johannes, Borody, Thomas J., and Clancy, Robert
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- 2008
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21. S1196 S100 Proteins in Inflammatory Bowel Disease and Irritable Bowel Syndrome.
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Wittkowski, Helmut, Langhorst, Jost, Kaiser, Thomas, Rueffer, Andreas, Roth, Johannes, and Foell, Dirk
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- 2008
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22. Potentials and pitfalls of DNA array analysis of the endothelial stress response
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Viemann, Dorothee, Schulze-Osthoff, Klaus, and Roth, Johannes
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NUCLEIC acids , *GENE expression , *GENETIC regulation , *IMMUNE response - Abstract
Abstract: Endothelial cells respond to inflammatory stimuli with complex genetic alterations that determine the immune response and the outcome of the inflammatory process. An additional layer of complexity is added by the different phenotypes and functional heterogeneity of endothelial cells in the various tissues. To understand these complex gene response patterns and the regulatory pathways involved, many investigators increasingly use DNA microarray analysis. There are, however, many potential pitfalls in the use of microarrays that can result in false data and erroneous conclusions. This review surveys the principles of DNA microarray technology and its applications in endothelial cell research. We also attempt to outline some of the caveats and standard criteria that have to be considered in order to realize the full potential of microarrays in inflammation research. [Copyright &y& Elsevier]
- Published
- 2005
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23. Nickel Chloride and Cobalt Chloride, Two Common Contact Sensitizers, Directly Induce Expression of Intercellular Adhesion Molecule-1 (ICAM-1), Vascular Cell Adhesion Molecule-1 (VCAM-1), and Endothelial Leukocyte Adhesion Molecule (ELAM-1) by Endothelial Cells
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Goebeler, Matthias, Meinardus-Hager, Georg, Roth, Johannes, Goerdt, Sergij, and Sorg, Clemens
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CELL adhesion , *CYTOKINES , *EPITHELIUM , *BLOOD vessels , *CHEMICAL reactions , *IMMUNOREGULATION - Abstract
Intercellular adhesion molecule-1 (ICAM-1), vascular cell adhesion molecule-1 (VCAM-1), and endothelial leukocyte adhesion molecule-1 (ELAM-1, E-selection) are endothelial surface molecules that play a role for leukocyte recruitment to sites of inflammation, e.g., during contact hypersensitivity. We studied the effects of sensitizing agents (2,4-dinitrobenzenesulfonic acid, metal salt haptens) and chemically related substances on endothelial adhesion molecule expression. Using flow cytometry and an enzyme-linked immunosorbent assay, NiCl2 and, to a lesser extent, CoCl2 were found to up-regulate ICAM-1, VCAM-1, and ELAM-1 expression on cultured human umbilical vein endothelium whereas the other substances tested showed no effects. Induction of adhesion molecules by NiCl2 required de novo mRNA and protein synthesis. Up-regulation could be blocked by kinase inhibitor H-7 but not staurosporine, suggesting involvement of phosphorylation events independent of protein kinase C activation. Concomitant application of NiCl2 and neutralizing antibodies to IL-1 did not block up-regulation by the hapten demonstrating that the latter did not act via an IL-1- dependent autocrine mechanism. Regarding ELAM-1 induction, pre-treatment for 24 h with NiCl2 produced hyporesponsiveness to IL-1 and TNF-α upon restimulation, suggesting that NiCl2 and these cytokines may partially share a common pathway of activation. In addition, analysis of cultured foreskin specimens revealed that NiCl2 may induce up-regulation of ELAM-1 on microvascular endothelium in vivo. Our data demonstrate that both Ni++ and Co++ to which simultaneous contact sensitivity is frequently observed have the ability to directly up-regulate endothelial adhesion molecules. This shared property may represent an adjuvant mechanism that promotes senitization and elicitation events in contact hypersensitivity to these haptens [ABSTRACT FROM AUTHOR]
- Published
- 1993
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24. Validity of ultrasonography in detecting enthesitis in children: A systematic literature review.
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Rossi-Semerano, Linda, Ravagnani, Viviana, Collado, Paz, Vojinovic, Jelena, Roth, Johannes, Magni-Manzoni, Silvia, Naredo, Esperanza, D'Agostino, Maria Antonietta, and Jousse-Joulin, Sandrine
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JUVENILE idiopathic arthritis , *ULTRASONIC imaging , *TEST validity , *SYMPTOMS - Abstract
• Enthesitis is a relevant clinical sign of juvenile idiopathic arthritis (JIA), especially enthesitis-related arthritis. • Ultrasonography might be a first-line imaging technique to evaluate enthesitis. • Because of the peculiarities of the growing skeleton, consensual definitions and a scoring system for enthesitis in JIA are essential. A systematic review to assess the value of ultrasonography (US) for detecting enthesitis in juvenile idiopathic arthritis (JIA). PubMed and Embase databases were searched for articles published from January 1966 to May 2021; we selected those meeting the inclusion criteria according to the US definition of enthesitis and metric properties studied. We assessed the clinical features of the population, study design, the type and number of entheses examined, the definition and scoring system of US enthesitis and metric properties according to the OMERACT filter (truth, discrimination and feasibility). The quality of the studies was evaluated with the Quality Assessment of Diagnostic Accuracy Studies 2. Five publications met the inclusion criteria (26 to 146 patients and 1 to 10 bilaterally examined entheses). All studies focused on lower-limb entheses. The elementary lesions included in the definition of adult enthesitis were generally assessed. Few studies reported US reliability and none evaluated sensitivity to change of US. US revealed entheseal abnormalities in 9.4 to 53% of JIA patients and 20 to 83% of enthesitis-related arthritis cases. No significant abnormalities were found in healthy children. US findings were poorly correlated with clinical examination. The overall quality of the studies was low, mainly because of the lack of a reference standard. US is a sensitive tool to detect entheseal abnormalities in JIA. The current evidence highlights that a standardized US definition of enthesitis in children is lacking and US criteria and discriminant validity have not been established. [ABSTRACT FROM AUTHOR]
- Published
- 2023
- Full Text
- View/download PDF
25. O-68 - Development and evaluation of new small molecule PET-radiotracers for the molecular imaging of inflammatory processes targeting S100A9.
- Author
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Steiner, Simon, Faust, Andreas, Scholz, Katja, Vogl, Thomas, Hermann, Sven, Schäfers, Michael, Junker, Anna, and Roth, Johannes
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RADIOACTIVE tracers , *SMALL molecules , *INFLAMMATION - Published
- 2022
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26. The calcium-binding protein complex S100A8/A9 has a crucial role in controlling macrophage-mediated renal repair following ischemia/reperfusion.
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Dessing, Mark C, Tammaro, Alessandra, Pulskens, Wilco P, Teske, Gwendoline J, Butter, Loes M, Claessen, Nike, van Eijk, Marco, van der Poll, Tom, Vogl, Thomas, Roth, Johannes, Florquin, Sandrine, and Leemans, Jaklien C
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CALCIUM-binding proteins , *REPERFUSION injury , *MACROPHAGE activation , *LABORATORY mice , *ACUTE kidney failure - Abstract
Upon ischemia/reperfusion (I/R)-induced injury, several damage-associated molecular patterns are expressed including the calcium-binding protein S100A8/A9 complex. S100A8/A9 can be recognized by Toll-like receptor-4 and its activation is known to deleteriously contribute to renal I/R-induced injury. To further test this, wild-type and S100A9 knockout mice (deficient for S100A8/A9 complex) were subjected to renal I/R. The expression of S100A8/A9 was significantly increased 1 day after I/R and was co-localized with Ly6G (mouse neutrophil marker)-positive cells. These knockout mice displayed similar renal dysfunction and damage and neutrophil influx compared with wild-type mice at this early time point. Interestingly, S100A9 knockout mice displayed altered tissue repair 5 and 10 days post I/R, as reflected by increased renal damage, sustained inflammation, induction of fibrosis, and increased expression of collagens. This coincided with enhanced expression of alternatively activated macrophage (M2) markers, while the expression of classically activated macrophage (M1) markers was comparable. Similarly, S100A9 deficiency affected M2, but not M1 macrophage polarization in vitro. During the repair phase following acute kidney injury, S100A9 deficiency affects M2 macrophages in mice leading to renal fibrosis and damage. Thus, S100A8/A9 plays a crucial part in controlling macrophage-mediated renal repair following I/R. [ABSTRACT FROM AUTHOR]
- Published
- 2015
- Full Text
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27. In vivo imaging of microenvironmental and anti-PD-L1-mediated dynamics in cancer using S100A8/S100A9 as an imaging biomarker.
- Author
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Helfen, Anne, Rieß, Jan, Fehler, Olesja, Stölting, Miriam, An, Zhengwen, Kocman, Vanessa, Schnepel, Annika, Geyer, Christiane, Gerwing, Mirjam, Masthoff, Max, Vogl, Thomas, Höltke, Carsten, Roth, Johannes, Ng, Tony, Wildgruber, Moritz, and Eisenblätter, Michel
- Subjects
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IMMUNE checkpoint inhibitors , *BIOMARKERS , *TUMOR microenvironment - Abstract
Purpose: As a promotor of tumor invasion and tumor microenvironment (TME) formation, the protein complex S100A8/S100A9 is associated with poor prognosis. Our aim was to further evaluate its origin and regulatory effects, and to establish an imaging biomarker for TME activity. Methods: S100A9−/−cells (ko) were created from syngeneic murine breast cancer 4T1 (high malignancy) and 67NR (low malignancy) wildtype (wt) cell lines and implanted into either female BALB/c wildtype or S100A9−/− mice (n = 10 each). Anti-S100A9-Cy5.5-targeted fluorescence reflectance imaging was performed at 0 h and 24 h after injection. Potential early changes of S100A9-presence under immune checkpoint inhibition (anti-PD-L1, n = 7 vs. rat IgG2b as isotype control, n = 3) were evaluated. Results: In S100A9−/−mice contrast-to-noise-ratios were significantly reduced for wt and S100A9−/−tumors. No significant differences were detected for 4T1 ko and 67NR ko cells as compared to wildtype cells. Under anti-PD-L1 treatment S100A9 presence significantly decreased compared with the control group. Conclusion: Our results confirm a secretion of S100A8/S100A9 by the TME, while tumor cells do not apparently release the protein. Under immune checkpoint inhibition S100A9-imaging reports an early decrease of TME activity. Therefore, S100A9-specific imaging may serve as an imaging biomarker for TME formation and activity. [ABSTRACT FROM AUTHOR]
- Published
- 2022
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28. Inhibition of p38 Mitogen-activated Protein Kinase Impairs Influenza Virus-induced Primary and Secondary Host Gene Responses and Protects Mice from Lethal H5N1 Infection.
- Author
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Börgeling, Yvonne, Schmolke, Mirco, Viemann, Dorothee, Nordhoff, Carolin, Roth, Johannes, and Ludwig, Stephan
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CELLULAR immunity , *RESPIRATORY infections , *PROTEIN kinases , *GENE expression , *IMMUNOREGULATION , *INFLUENZA viruses - Abstract
Highly pathogenic avian influenza viruses (HPAIV) induce severe inflammation in poultry and men. One characteristic of HPAIV infections is the induction of a cytokine burst that strongly contributes to viral pathogenicity. This cell-intrinsic hypercytokinemia seems to involve hyperinduction of p38 mitogen- activated protein kinase. Here we investigate the role of p38 MAPK signaling in the antiviral response against HPAIV in mice as well as in human endothelial cells, the latter being a primary source of cytokines during systemic infections. Global gene expression profiling of HPAIV-infected endothelial cells in the presence of the p38-specific inhibitor SB 202190 revealed that inhibition of p38 MAPK leads to reduced expression of IFNβ and other cytokines afterH5N1andH7N7infection. More than 90% of all virus-induced genes were either partially or fully dependent on p38 signaling. Moreover, promoter analysis confirmed a direct impact of p38 on the IFNβ promoter activity. Furthermore, upon treatment with IFN or conditioned media from HPAIV-infected cells, p38 controls interferon-stimulated gene expression by coregulating STAT1 by phosphorylation at serine 727. In vivo inhibition of p38 MAPK greatly diminishes virus-induced cytokine expression concomitant with reduced viral titers, thereby protecting mice from lethal infection. These observations show that p38MAPKacts on two levels of the antiviral antiviral IFN response. Initially the kinase regulates IFN induction and, at a later stage, p38 controls IFN signaling and thereby expression of IFN-stimulated genes. Thus, inhibition of MAP kinase p38 may be an antiviral strategy that protects mice from lethal influenza by suppressing excessive cytokine expression [ABSTRACT FROM AUTHOR]
- Published
- 2014
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29. Induction of an anti-inflammatory human monocyte subtype is a unique property of glucocorticoids, but can be modified by IL-6 and IL-10
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Tsianakas, Athanasios, Varga, Georg, Barczyk, Katarzyna, Bode, Guenther, Nippe, Nadine, Kran, Nelli, Roth, Johannes, Luger, T.A., Ehrchen, Jan, and Sunderkoetter, Cord
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GLUCOCORTICOIDS , *IMMUNOSUPPRESSIVE agents , *MONOCYTES , *CYTOKINES , *MACROPHAGES , *INTERLEUKIN-10 , *INTERLEUKIN-6 - Abstract
Abstract: Glucocorticoids (GC) are the most widely used immunosuppressive agents in clinical medicine. Recently we showed that GC enhance survival of human monocytes and induce a specific anti-inflammatory monocyte subtype which actively induces resolution of inflammation. We now investigated if cytokines IL-4, IL-6 and IL-10, which, like GC, have mostly anti-inflammatory effects on macrophages, would have GC-like effects also on monocytes. Human monocytes were stimulated with either cytokine, GC or combination thereof, and resulting effects on apoptosis, adherence, migration, phagocytosis, ROS production and cell surface phenotype were determined. We found that IL-4, IL-6, and IL-10 had either less or different effects on various anti-inflammatory functions of monocytes compared to GC. As such, IL-4 and IL-6 alone did not delay apoptosis while IL-10 even enhanced it. However, IL-6 or IL-10 increased GC-mediated protection from apoptosis when applied together with GC. Thus, the potential of GC to induce anti-inflammatory human monocytes is unique and not mimicked by the investigated cytokines. However, IL-6 and IL-10 amplify GC-induced anti-inflammatory and pro-resolution mechanisms by enhancing survival of GC-induced monocytes and thus sustaining their function. This combined effect of GC and cytokines could be important for the physiological switch from amplification towards resolution phase of inflammation. [Copyright &y& Elsevier]
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- 2012
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30. A Novel Intronic cAMP Response Element Modulator (CREM) Promoter Is Regulated by Activator Protein-1 (AP-1) and Accounts for Altered Activation-induced CREM Expreβion in T Cells from Patients with Systemic Lupus Erythematosus.
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Rauen, Thomas, Benedyk, Konrad, Yuang-Taung Juang, Kerkhoff, Claus, Kyttaris, Vasileios C., Roth, Johannes, Tsokos, George C., and Tenbrock, Klaus
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PHYSIOLOGICAL effects of adenylic acid , *PHYSIOLOGICAL effects of adenosine , *T cells , *GENETIC transcription , *TRANSCRIPTION factors , *LUPUS erythematosus , *GENETICS , *PHYSIOLOGY - Abstract
The transcriptional repressor cAMP response element modulator (CREM) a has important roles in normal T cell physiology and contributes to aberrant T cell function in patients with systemic lupus erythematosus (SLE). Recently, we characterized a specificity protein-1-dependent promoter located upstream of the CREM gene that accounts for increased basal CREM expression in SLE T cells and reflects disease activity. Here, we identify a novel intronic CREM promoter (denoted P2) in front of the second exon of the CREM gene that harbors putative binding sites for TATA-binding proteins and the transcriptional activator AP-1. DNA binding studies, chromatin immunoprecipitation, and reporter assays confirmed the functional relevance of these sites, and T cell activation through CD3/CD28 stimulation or phorbol 12-myristate 13-acetate/ionomycin treatment enhances P2 promoter activity. Although the basal CREM levels are increased in T cells from SLE patients compared with healthy controls, there are remarkable differences in the regulation of CREM expression in response to T cell activation. Whereas T cells from healthy individuals display increased CREM expression after T cell activation, most likely through AP-1-dependent up-regulation of the P2 promoter, SLE T cells fail to further increase their basal CREM levels upon T cell activation due to a decreased content of the AP-1 family member c-Fos. Because CREM trans-represses c-fos transcription in SLE T cells, we propose an autoregulatory feedback mechanism between CREM and AP-1. Our findings extend the understanding of CREM gene regulation in the context of T cell activation and disclose another difference in the transcriptional machinery in SLE T cells. [ABSTRACT FROM AUTHOR]
- Published
- 2011
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31. Subcutaneous Infection with S. aureus in Mice Reveals Association of Resistance with Influx of Neutrophils and Th2 Response.
- Author
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Nippe, Nadine, Varga, Georg, Holzinger, Dirk, Löffler, Bettina, Medina, Eva, Becker, Karsten, Roth, Johannes, Ehrchen, Jan M, and Sunderkötter, Cord
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STAPHYLOCOCCUS aureus , *LEUCOCYTES , *BIOLOGICAL transport , *IMMUNE response , *LYMPH nodes , *SOFT tissue infections - Abstract
Staphylococcus aureus is the leading cause of bacterial skin infection. Once it overcomes the epithelial barrier, it either remains locally controlled or spreads in the dermis causing soft tissue infection. These different courses depend not only on its virulence factors, but also on the immune response of the infected individual. The goal of this study was to identify host factors that influence different outcomes. We, therefore, established comparative analysis of subcutaneous footpad infection with S. aureus (SH1000) in different inbred mouse strains. We found that C57BL/6 mice are more susceptible than BALB/c and DBA/2 mice, reflected by significantly higher footpad swelling and bacterial load, as well as increased dissemination of bacteria into inguinal lymph nodes and kidneys. This susceptibility was associated with lower influx of polymorphonuclear leukocytes (PMNs), but higher secretion of CXCL-2. Remarkably, resistance correlated with S. aureus-specific Th2-cell response in BALB/c and DBA/2 mice, whereas susceptible C57BL/6 mice generated a Th1-cell response. As Th1 cells are able to induce release of CXCL-2, and as CXCL-2 is able to increase the survival of S. aureus within PMNs, interactions between PMNs and Th1 or Th2 cells need to be considered as important mechanisms of resistance in murine soft tissue infection with S. aureus. [ABSTRACT FROM AUTHOR]
- Published
- 2011
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32. Erk5 Activation Elicits a Vasoprotective Endothelial Phenotype via Induction of Krüppel-like Factor 4 (KLF4).
- Author
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Ohnesorge, Nils, Viemann, Dorothee, Schmidt, Nicole, Czymai, Tobias, Spiering, Désirée, Schmolke, Mirco, Ludwig, Stephan, Roth, Johannes, Goebeler, Matthias, and Schmidt, Marc
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MITOGEN-activated protein kinases , *LAMINAR flow , *VASCULAR diseases , *APOPTOSIS , *GENES , *STATINS (Cardiovascular agents) - Abstract
The MEKS/Erk5 MAPK cascade has recently been implicated in the regulation of endothelial integrity and represents a candidate pathway mediating the beneficial effects of laminar flow, a major factor preventing vascular dysfunction and disease. Here we expressed a constitutively active mutant of MEK5 (MEKSD) to study the transcriptional and functional responses to Erk5 activation in human primary endothelial cells. We provide evidence that constitutive Erk5 activation elicits an overall protective phenotype characterized by increased apoptosis resistance and a decreased angiogenic, migratory, and inflammatory potential. This is supported by bioinformatic microarray analysis, which uncovered a statistical overrepresentation of corresponding functional clusters as well as a significant induction of anti-thrombotic, hemostatic, and vasodilatory genes. We identify KLF4 as a novel Erk5 target and demonstrate a critical role of this transcription factor downstream of Erk5. We show that KLF4 expression largely reproduces the protective phenotype in endothelial cells, whereas KLF4 siRNA suppresses expression of various Erk5 targets. Additionally, we show that vasoprotective statins potently induce KLF4 and KLF4-dependent gene expression via activation of ErkS. Our data underscore a major protective function of the MEK5/Erk5/KLF4 module in ECs and implicate agonistic Erk5 activation as potential strategy for treatment of vascular diseases. [ABSTRACT FROM AUTHOR]
- Published
- 2010
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33. LFA-1 Contributes to Signal I of T-Cell Activation and to the Production of Th1 Cytokines.
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Varga, Georg, Nippe, Nadine, Balkow, Sandra, Peters, Thorsten, Wild, Martin K., Seeliger, Stephan, Beissert, Stefan, Krummen, Mathias, Roth, Johannes, Sunderkötter, Cord, and Grabbe, Stephan
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T cells , *INTEGRINS , *CELL adhesion molecules , *LEUCOCYTES , *IMMUNOGLOBULINS - Abstract
The β2 integrins are important for both transendothelial migration of leukocytes and T-cell activation during antigen presentation. In T cells, triggering of leukocyte functional antigen-1 (LFA-1) is required for full activation and T-helper (Th)1/Th2 differentiation. We used CD18-deficient (CD18−/−) mice to examine the role of LFA-1 in the activation of T cells. Compared with wild-type controls, CD18−/− T cells proliferated normally when stimulated with antibodies against CD3 and CD28, but secreted significantly less IFN-γ and IL-2 than their wild-type counterparts. However, when T cells were stimulated with dendritic cells (DCs) that provide additional LFA-1 ligation, the proliferation of CD18−/− T cells was significantly reduced, whereas cytokine production remained impaired. The diminished proliferative capacity of CD18−/− T cells could be fully compensated for by additional triggering of the T-cell receptor, but not by additional stimulation through the costimulatory molecule, CD28. Thus, ligation of LFA-1 on T cells participates in regulation of Th1 cytokines in vivo. In addition, LFA-1 primarily exerts an effect as an enhancer of TCR signalling and does not facilitate classical costimulation. [ABSTRACT FROM AUTHOR]
- Published
- 2010
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34. Interaction between S100A8/A9 and Annexin A6 Is Involved in the Calcium-induced Cell Surface Exposition of S100A8/A9.
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Bode, Günther, Lüken, Aloys, Kerkhoff, Claus, Roth, Johannes, Ludwig, Stephan, and Nacken, Wolfgang
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ANNEXINS , *CALCIUM , *CELL receptors , *BINDING sites , *INFLAMMATION , *CANCER cells , *CELL lines , *MOLECULAR biology - Abstract
The calcium binding S100A8/A9 complex (MRP8/14; calgranulin) is considered as an important proinflammatory mediator in acute and chronic inflammation and has recently gained attention as a molecular marker up-regulated in various human cancers. Here, we report that S100A8/A9 is expressed in breast cancer cell lines and is up-regulated by interleukin-1β and tumor necrosis factor-α in SKBR3 and MCF-7 cells. We identified the phospholipid-binding protein annexin A6 as a potential S100A8/A9 binding protein by affinity chromatography. This finding was verified by Southwestern overlay experiments and by coimmunoprecipitation with the S100A8/A9-specific monoclonal antibody 27E10. Immunocytochemical experiments demonstrated that S100A8/A9 and annexin A6 colocalize in SKBR3 breast cancer cells predominantly in membranous structures. Upon calcium influx both S100A8/A9 and annexin A6 are exposed on the cell surface of SKBR3 cells. Subcellular fractionation studies suggested that after A23187 stimulation membrane association of S100A8/A9 is not enhanced. However, both S100A8/A9 and annexin A6 are exposed on the cell surface of SKBR3 cells upon calcium influx. Experiments with artificial liposomes indicated that S100A8/A9 is able to associate with membranes independently of both annexin A6 and independently of calcium. Finally, cell surface expression of S100A8/A9 could not be observed in A23187-treated A431 and HaCaT cells. Both cell lines are known to be devoid of annexin A6. Repression of annexin A6 expression by small interfering RNA in SKBR3 cells abolishes the cell surface exposition of S100A8/A9 upon calcium influx, suggesting that annexin A6 contributes to the calcium-dependent cell surface exposition of the membrane associated-S100A8/A9 complex. [ABSTRACT FROM AUTHOR]
- Published
- 2008
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35. Similar effects of long-term exogenous growth hormone (GH) on bone and muscle parameters: A pQCT study of GH-deficient and small-for-gestational-age (SGA) children
- Author
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Schweizer, Roland, Martin, David D., Haase, Martin, Roth, Johannes, Trebar, Branko, Binder, Gerhard, Schwarze, C. Philipp, and Ranke, Michael B.
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SOMATOTROPIN , *STATURE , *BONE growth , *MUSCLES , *CHILD development - Abstract
Abstract: Background and aims : Treatment with GH in short children has focused on height development. Little is known about the concomitant changes in muscle mass, bone structure and bone strength. Methods : Muscle area as well as parameters of bone architecture (bone mineral content, BMC; volumetric cortical density, total bone area, TBA; cortical area, cortical thickness, CT; and marrow area) were measured by means of pQCT (Stratec) at 65% of the proximal length of the forearm. The strength–strain index (SSI) was calculated as an indicator of bone strength. Results : Prepubertal children with GHD (mean values: age; 7.2 years; height SDS=−2.9 SDS; GH dose: 30 μg/kg/d) were followed at 0, 6, 12 (n =74) and 24 (n =55) months. Prepubertal children with SGA (mean values: age: 7.1 years; height SDS=−3.4 SDS; GH dose: 55 μg/kg/d) were followed at 0, 6, 12 (n =47) and 24 (n =35) months. Both groups showed a similar increase in height. At GH start, muscle mass and bone characteristics were lower than normal but similar in SGA vs. GHD. Muscle area (mean values, SDS) increased from −3.0 to −1.5 in SGA and from −2.4 to −1.0 in GHD. Bone geometry changed in a biphasic mode, with an increase in total bone area and lowering of bone mineral content (BMC) during the first 12 months, followed by an increase of BMC and CT thereafter. SSI (mean values, mm3) improved from 78 to 114 in GHD and from 62 to 101 in SGA after 24 months on GH. The increment in terms of SDS did not reach significance in SGA. SSI correlated positively with muscle area before and during GH treatment. Conclusions : Bone strength and muscle mass are impaired in prepubertal children with GHD and SGA. Exogenous GH can indirectly improve bone structure and strength by inducing an increase in muscle mass. Our findings support the assumption that, in SGA, there is impaired tissue responsiveness to GH. [Copyright &y& Elsevier]
- Published
- 2007
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36. Site of Blood Vessel Damage and Relevance of CD18 in a Murine Model of Immune Complex-Mediated Vasculitis.
- Author
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Sindrilaru, Anca, Seeliger, Stephan, Ehrchen, Jan M., Peters, Thorsten, Roth, Johannes, Scharffetter-Kochanek, Karin, and Sunderkötter, Cord H.
- Subjects
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NEUTROPHILS , *BLOOD vessels , *WOUNDS & injuries , *VASCULITIS , *GLOMERULONEPHRITIS , *AUTOIMMUNE diseases , *IMMUNE complexes , *ACTIVE oxygen in the body , *LABORATORY mice - Abstract
How neutrophils (polymorphonuclear neutrophils, PMNs) damage vessels in leukocytoclastic vasculitis (LcV) mediated by immune complexes (ICs) is unclear. If degradative enzymes and oxygen radicals are released from PMNs while adhering to the inner side of the vessel wall, they could be washed away by the blood stream or neutralized by serum protease inhibitors. We investigated if in LcV PMNs could damage vessels from the tissue side after transmigration. We used CD18-deficient (CD18−/−) mice because the absence of CD18 excludes transmigration of PMNs. When eliciting the Arthus reaction in ears of CD18−/− mice, deposition of ICs was not sufficient to recruit PMNs or to induce IC-mediated LcV. Injection of PMNs intradermally in CD18−/− mice allowed us to investigate if bypassing diapedesis and placing PMNs exclusively on the abluminal side leads to vascular destruction. We found that injected PMNs gathered around perivascular ICs, but did not cause vessel damage. Only intravenous injection of wild-type PMNs could re-establish the Arthus reaction in CD18−/− mice. Thus, PMNs cause vessel damage during diapedesis from the luminal side, but not from the perivascular space. We suggest that in order to shield the cytotoxic products from the blood stream, ICs induce particularly tight interactions between them, PMNs and endothelial cells.Journal of Investigative Dermatology (2007) 127, 447–454. doi:10.1038/sj.jid.5700563; published online 28 September 2006 [ABSTRACT FROM AUTHOR]
- Published
- 2007
- Full Text
- View/download PDF
37. Biophysical characterization of S100A8 and S100A9 in the absence and presence of bivalent cations
- Author
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Vogl, Thomas, Leukert, Nadja, Barczyk, Katarzyna, Strupat, Kerstin, and Roth, Johannes
- Subjects
- *
CATIONS , *MOLECULES , *PROTEINS , *CALCIUM in the body - Abstract
Abstract: S100A8 and S100A9 are two proinflammatory molecules belonging to the S100 family of calcium-binding proteins. Common to all S100 proteins S100A8 and S100A9 form non-covalently associated complexes which have been shown to exhibit different functional properties. Besides dimerization, recent research is focused on the importance of higher oligomeric structures of S100 proteins induced by bivalent cations. While S100A8/S100A9-heterodimers are formed in the absence of calcium, tetramerization is strictly calcium-dependent. Heterodimer formation is not a simple process and our biophysical analyses (FRET, ESI-MS) demonstrate that simply mixing both subunits is not sufficient to induce complex formation. Steps of denaturation/renaturation are necessary for the recombinant complex to show identical biophysical properties as S100A8/S100A9 obtained from granulocytes. In addition to calcium both proteins are able to bind zinc with high affinity. Here we demonstrate for the first time by different biophysical methods (MALDI-MS, ESI-MS, fluorescence spectroscopy) that zinc-binding, like calcium, induces (S100A8/S100A9)2-tetramers. Using mass spectrometric investigations we demonstrate that zinc triggers the formation of (S100A8/S100A9)2-tetramers by zinc-specific binding sites rather than by interactions with calcium-specific EF-hands. The zinc-induced tetramer is structurally very similar to the calcium-induced tetramer. Thus, like calcium, zinc acts as a regulatory factor in S100A8/S100A9-dependent signaling pathways. [Copyright &y& Elsevier]
- Published
- 2006
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38. Expression of Myeloid-Related Protein-8 and -14 in Patients With Acute Kawasaki Disease
- Author
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Hirono, Keiich, Foell, Dirk, Xing, Yanlin, Miyagawa-Tomita, Sachiko, Ye, Fei, Ahlmann, Martina, Vogl, Thomas, Futatani, Takeshi, Rui, Chen, Yu, Xianyi, Watanabe, Kazuhiro, Wanatabe, Sayaka, Tsubata, Shinichi, Uese, Keiichiro, Hashimoto, Ikuo, Ichida, Fukiko, Nakazawa, Makoto, Roth, Johannes, and Miyawaki, Toshio
- Subjects
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MUCOCUTANEOUS lymph node syndrome , *CORONARY arteries , *GLOBULINS , *BLOOD vessels - Abstract
Objectives: This study investigated patients with acute Kawasaki disease (KD) to validate myeloid-related protein (MRP)-8/MRP-14 as a marker of disease activity and severity of coronary artery lesion development. Background: Both MRP-8 and -14, which are S100-proteins secreted by activated neutrophils and monocytes, bind specifically to endothelial cells and induce thrombogenic and inflammatory responses in a variety of disease conditions. Methods: We investigated 61 patients with acute KD and examined sequential changes in serum levels of MRP-8/MRP-14, messenger ribonucleic acid (mRNA) expression of MRP-8 and -14 in circulating granulocytes and monocytes, and amounts of MRP-8/MRP-14 bound to circulating endothelial cells. Results: The serum MRP-8/MRP-14 levels as well as mRNA expressions of MRP-8 and -14 in granulocytes were strongly upregulated during the early stage of acute KD, and decreased dramatically within 24 h of intravenous immune globulin therapy (p < 0.05) in 45 responders. In contrast, in 16 nonresponders both of these increased after the initial treatment. The number of MRP-8/MRP-14–positive circulating endothelial cells was higher in patients with acute KD than in control patients and increased significantly by 2 weeks after the onset of KD, especially in patients in whom coronary artery lesions developed. Conclusions: We show for the first time that MRP-8/MRP-14 are exclusively secreted by granulocytes in patients with acute KD, and intravenous immune globulin treatment suppresses their gene expression. Serum levels of MRP-8/MRP-14 may be useful markers of disease activity, and the levels of MRP-8/MRP-14–positive circulating endothelial cell may predict the severity of vasculitis, confirming an important role for distinct inflammatory reactions in endothelium. [Copyright &y& Elsevier]
- Published
- 2006
- Full Text
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39. Neutrophil-derived S100A12 is profoundly upregulated in the early stage of acute Kawasaki disease
- Author
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Ye, Fei, Foell, Dirk, Hirono, Kei-ich, Vogl, Thomas, Rui, Chen, Yu, Xianyi, Watanabe, Sayaka, Watanabe, Kazuhiro, Uese, Kei-ichiro, Hashimoto, Ikuo, Roth, Johannes, Ichida, Fukiko, and Miyawaki, Toshio
- Subjects
- *
NEUTROPHILS , *MUCOCUTANEOUS lymph node syndrome , *IMMUNOGLOBULINS , *GENE expression - Abstract
Neutrophil-derived S100A12 is strongly upregulated during the acute stage of Kawasaki disease and decreases significantly in response to intravenous immune globulin (IVIG) treatment, whereas in nonresponders, serum concentrations increases after initial treatment. Decreased S100A12 expression in neutrophils was detected initially in nonresponders but increased significantly after IVIG treatment, suggesting delayed inflammatory response of neutrophils in nonresponders. Furthermore, in vitro S100A12 secretion increased with tumor necrosis factor-α (TNF-α) stimulation, whereas intracellular levels were lower in neutrophils with the higher TNF-α dose, suggesting intracellular depletion. S100A12 expression in neutrophils appears to reflect responsiveness to IVIG treatment and is possibly involved in the pathophysiology of acute vasculitis. [Copyright &y& Elsevier]
- Published
- 2004
- Full Text
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40. Phagocyte-specific calcium-binding S100 proteins as clinical laboratory markers of inflammation
- Author
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Foell, Dirk, Frosch, Michael, Sorg, Clemens, and Roth, Johannes
- Subjects
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PROTEINS , *INFLAMMATION , *PHAGOCYTES , *CALCIUM-binding proteins - Abstract
The EF-hand homolog family of S100 proteins comprises the largest group of calcium-binding proteins. Within this S100 family, the phagocyte-specific calcium-binding proteins are pro-inflammatory molecules expressed and secreted by phagocytes, which play a pivotal role within the innate immune system. Although the exact biological functions of these proteins still remain to be defined in greater detail, there is evidence that they are involved in a pro-inflammatory axis associated with various inflammatory conditions. The three members of this group, S100A8, S100A9 and S100A12 are overexpressed at local sites of inflammation. High concentrations are found in synovial fluid, sputum, stool and blood plasma/serum during inflammation. Both the S100A8/S100A9 complex and S100A12 have been proven to be useful as diagnostic markers of inflammation especially in non-infectious inflammatory diseases such as arthritis, chronic inflammatory lung and bowel disease. They indicate phagocyte activation more sensitively than conventional parameters of inflammation. As a consequence, there is a strong correlation to the inflammation of various acute and chronic disorders, making these proteins sensitive parameters for the monitoring of disease activity and response to treatment in individual patients. The phagocyte-specific S100 proteins are able to indicate minimal residual inflammation, which is not detected by other diagnostic tests, and they may even be prospective markers for the outcome of patients. In this review, pro-inflammatory functions of S100 proteins and their usefulness as biomarkers of inflammation are presented. [Copyright &y& Elsevier]
- Published
- 2004
- Full Text
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41. Determination of the peptide binding motif and high-affinity ligands for HLA-DQ4 using synthetic peptide libraries
- Author
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Volz, Thomas, Schwarz, Gerold, Fleckenstein, Burkhard, Schepp, Carsten P., Haug, Markus, Roth, Johannes, Wiesmüller, Karl-Heinz, and Dannecker, Günther E.
- Subjects
- *
ARTHRITIS , *AUTOIMMUNE diseases , *JOINT diseases , *AUTOIMMUNITY - Abstract
Juvenile idiopathic arthritis (JIA) is considered to be an autoimmune disease. Various human leukocyte antigen (HLA) associations for different subgroups of this heterogeneous disease have been found. For early-onset pauciarticular arthritis (now oligoarthritic JIA), a strong association with the HLA class II haplotype DQA1*0401/DQB1*0402 (DQ4) has been described. We determined the peptide-binding specificities of this HLA-DQ molecule by screening a synthetic acetylated nonapeptide amide library with one defined and eight random sequence positions. A characteristic binding motif could be deduced. By use of these data, we designed defined specific nonapeptides and identified high-affinity ligands binding to HLA-DQ4. The peptide binding motif of HLA-DQ4 is very similar to the motif of HLA-DQ7, also associated with oligoarthritic JIA. It is, however, different from binding motifs of neutral or protective HLA-DQ molecules. Our results further support the idea of differential peptide presentation in the pathogenesis of oligoarthritic JIA. [Copyright &y& Elsevier]
- Published
- 2004
- Full Text
- View/download PDF
42. Selective Expression of Calcium-Binding Proteins S100A8 and S100A9 at Distinct Sites of Hair Follicles.
- Author
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Schmidt, Marc, Gillitzer, Reinhard, Toksoy, Atiye, Bröcker, Eva-B., Rapp, Ulf R., Paus, Ralf, Roth, Johannes, Ludwig, Stephan, and Goebeler, Matthias
- Subjects
- *
CALCIUM-binding proteins , *KERATINOCYTES , *IN situ hybridization , *HAIR follicles - Abstract
Studies the spatial expression profile of calcium-binding proteins S100A8 and S100A9 mRNA in the human hair follicle and its correlation with established markers of keratinocyte differentiation. Use of the radioactive in situ hybridization process in the study; Tissue distribution of the proteins; Expression in distinct differentiation stages of myelomonocytic cells as well as by epithelial cells including keratinocytes.
- Published
- 2001
- Full Text
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43. THE TOLL-LIKE RECEPTOR 4 LIGANDS S100A8 AND S100A9 ARE CRUCIAL FACTORS IN VIRAL CARDIOMYOPATHY
- Author
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Becher, Peter Moritz, Lindner, Diana, Savvatis, Kostantinos, Müller, Irene, Fröhlich, Matthias, Vogl, Thomas, Roth, Johannes, Schultheiss, Heinz-Peter, and Tschöpe, Carsten
- Published
- 2013
- Full Text
- View/download PDF
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