TY - THES A1 - Wellner, Mirjam T1 - T-Zell-Charakterisierung im peripheren Blut bei Kindern mit chronisch entzündlichen Darmerkrankungen T1 - Peripheral Blood T Cell Characterization in Children with Inflammatory Bowel Disease N2 - Die Inzidenz von chronisch entzündlichen Darmerkrankungen (CED), insbesondere von Morbus Crohn (MC), nimmt weltweit zu, was auch eine Vielzahl an Kindern betrifft. Obwohl die Krankheit in den letzten Jahrzehnten Gegenstand zahlreicher Forschungsarbeiten war, ist die Pathogenese nicht abschließend geklärt. Diese Arbeit vergleicht T-Zellen gesunder pädiatrischer Probanden mit T-Zellen pädiatrischer CED Patienten mittels Flowcytometrie unter Berücksichtigung von Differenzierungsstadium, Krankheitsaktivität, Therapie und CMV-Status. Die Verteilung der T-Zell-Subpopulationen zeigt keine signifikanten Unterschiede zwischen Patienten und Kontrollen, jedoch zeigen sich für TH1 und TH17 Zellen Unterschiede zwischen MC Patienten und Kontrollen, welche auch mit Krankheitsaktivität und Therapie korrelieren. Der Anteil von CXCR3+ Zellen ist innerhalb der CD4+ Memory-Populationen und innerhalb der CD8+ Memory- und Effektor-Populationen bei MC Patienten – vor allem mit aktiver Erkrankung bzw. ohne Therapie – deutlich geringer als bei Kontrollen. Gleichzeitig zeigt sich der Anteil an CCR6+ Zellen sowie der Anteil an IL 17+CCR6+ Zellen bei MC Patienten in Remission sowie unter Therapie mit TNFα-Blockern höher als bei Kontrollen. Zudem sind die Effektor-Zell-Gleichgewichte bei MC zugunsten von TH17 Zellen verschoben. Somit unterstützt die Arbeit die weitverbreitete Hypothese einer gesteigerten TH17-Antwort bei MC. Auch zeigt sich eine Verminderung der TH1-Zellen im peripheren Blut bei aktiv erkrankten MC Patienten im Vergleich zu Kontrollen, was sich möglicherweise durch eine Abwanderung oder Umwandlung dieser Zellen bei aktivem MC erklären lässt. Desweiteren zeigt sich, dass CED Patienten eine verstärkte Neigung zur vorzeitigen Immunoseneszenz aufzuweisen scheinen, was durch eine latente CMV-Infektion nochmals verstärkt erscheint. Einige CMV-assoziierte Veränderungen der T-Zell-Differenzierung, wie z.B. die CD45RA-Reexpression sowie die TNFα- und IFNγ-Mehrexpression, zeigen sich bei CMV+ CED Patienten zudem ausgeprägter als bei CMV+ Kontrollen. Interessant ist daher, dass CMV+ Probanden und CED Patienten Veränderungen aufweisen, die sich teilweise zu addieren scheinen. N2 - There is a globally increasing incidence of Inflammatory Bowel Disease (IBD), especially of Crohn’s disease, which can also be seen in children. Despite the disease being studied intensively over the recent decades, the pathogenesis is not yet completely understood. This study compares t cells isolated from pediatric IBD patients with those of healthy donors using flow cytometry and taking into account cell differentiation status, disease activity, current therapeutic regime and the donor’s CMV status. T cell subsets show no significant distributional differences between patients and controls. However, TH1 and TH17 cells show differences between patients with Crohn’s disease and controls, which correlate with disease activity and therapy. The proportion of CXCR3+ cells is reduced within CD4+ memory subsets and CD8+ memory and effector subsets, especially in patients with active disease or without therapy. At the same time CCR6+ and IL-17+CCR6+ subsets are increased in patients with Crohn’s disease in remission or under therapy compared to controls. Furthermore, effector cell balances are shifted towards TH17 cells in patients with Crohn’s disease, supporting the widespread hypothesis of an increased TH17 response in Crohn’s disease. Additionally, TH1 cells are diminished in peripheral blood of patients with active Crohn’s disease compared to controls, possibly suggesting a migration of these cells into tissue or a differentiation into other subsets. As an additional finding, IBD patients exhibited an increased tendency for premature immunosenscence, which was even more distinct in patients with latent CMV infection. Some changes in t cell differentiation commonly attributed to CMV infection, like reexpression of CD45RA and increased expression of TNFα and IFNγ, are more pronounced in CMV positive IBD patients, than in CMV positive healthy donors. Interestingly, the combination of IBD with CMV infection partially add up to more pronounces changes in CD4+ t cells and especially in CD8+ t cells. KW - Chronisch-entzündliche Darmerkrankung KW - Morbus Crohn KW - T-Lymphozyt KW - Colitis ulcerosa KW - T-Zelle KW - Immunoseneszenz KW - Cytomegalievirus Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-192424 ER - TY - THES A1 - Streng, Katja T1 - Erfassung der körperlichen Aktivität mittels Accelerometrie und Pedometrie T1 - Assessment of physical activity using accelerometers and pedometers N2 - Accelerometrie und Pedometrie sind objektive Verfahren zur Erfassung körperlicher Aktivität, wobei die Accelerometrie die Intensität körperlicher Bewegung durch Messung der Beschleunigung zeitlich hochaufgelöst misst, während bei der Pedometrie die Zahl der Schritte, typischerweise über einen ganzen Tag, erfasst wird. Ziel dieser Studie war es, das Pedometer-Modell Omron HJ-322 und zwei Accelerometer-Modelle der Marke ActiGraph (Modell GT1M und dessen Nachfolger GT3X+) hinsichtlich ihrer Beschreibung von Aktivität unter Alltagsbedingungen miteinander zu vergleichen. Dies erfolgte durch das parallele Tragen der jeweiligen Geräte über 7 Tage durch 40 gesunden Probanden sowie 15 Mukoviszidose-Patienten, bei welchen die Aktivitätsmessung im Rahmen der Studie ACTIVATE-CF (internationale Multicenterstudie zur Untersuchung der Auswirkung körperlicher Aktivität auf den Krankheitsverlauf bei Mukoviszidose) durchgeführt wurde. Während eine Vergleichbarkeit zwischen beiden Accelerometer-Modellen gegeben ist, zeigten sich deutliche Unterschiede in der Schrittzählung zwischen Accelerometer und Pedometer. Starke Zusammenhänge zwischen der mittels Schrittzähler gemessenen Schrittzahl und verschiedenen Aktivitäts-Indikatoren der Accelerometer konnten nachgewiesen werden. N2 - Wearable devices like accelerometers and pedometers provide an objective way to assess physical activity. Accelerometers provide detailed information on physical activity like duration, frequency and intensity, whereas pedometers measure daily step-count. The objective of this study was to analyze the comparability of one pedometer (Omron HJ-322) and two accelerometers (ActiGraph GT1M and its successor ActiGraph GT3X+), regarding the description of physical activity under free-living-conditions. 40 healthy participants wore these devices simultaneously for 7 days. Also activity-data was available from 15 patients with cystic fibrosis, who took part in the international multicenter study ACTIVATE-CF, a randomized controlled study that examines the effects of a partially supervised physical trainings on the lung functions of the patients. While there is a good comparability between both accelerometer-models, we saw a large difference between accelerometer- and pedometer-counted steps. Good correlations were obtained between the number of pedometer-steps and different accelerometer-measures. KW - Körperliche Aktivität KW - Beschleunigungssensor KW - Schrittzähler KW - Mukoviszidose KW - Accelerometer KW - Pedometer Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-185428 ER - TY - JOUR A1 - Streng, Andrea A1 - Goettler, David A1 - Haerlein, Miriam A1 - Lehmann, Lisa A1 - Ulrich, Kristina A1 - Prifert, Christiane A1 - Krempl, Christine A1 - Weißbrich, Benedikt A1 - Liese, Johannes G. T1 - Spread and clinical severity of respiratory syncytial virus A genotype ON1 in Germany, 2011–2017 JF - BMC Infectious Diseases N2 - Background The Respiratory Syncytial Virus (RSV) A genotype ON1, which was first detected in Ontario (Canada) in 2010/11, appeared in Germany in 2011/12. Preliminary observations suggested a higher clinical severity in children infected with this new genotype. We investigated spread and disease severity of RSV-A ON1 in pediatric in- and outpatient settings. Methods During 2010/11 to 2016/17, clinical characteristics and respiratory samples from children with acute respiratory tract infections (RTI) were obtained from ongoing surveillance studies in 33 pediatric practices (PP), one pediatric hospital ward (PW) and 23 pediatric intensive care units (PICU) in Germany. RSV was detected in the respiratory samples by PCR; genotypes were identified by sequencing. Within each setting, clinical severity markers were compared between RSV-A ON1 and RSV-A non-ON1 genotypes. Results A total of 603 children with RSV-RTI were included (132 children in PP, 288 in PW, and 183 in PICU). Of these children, 341 (56.6%) were infected with RSV-A, 235 (39.0%) with RSV-B, and one child (0.2%) with both RSV-A and RSV-B; in 26 (4.3%) children, the subtype could not be identified. In the 341 RSV-A positive samples, genotype ON1 was detected in 247 (72.4%), NA1 in 92 (26.9%), and GA5 in 2 children (0.6%). RSV-A ON1, rarely observed in 2011/12, was the predominant RSV-A genotype in all settings by 2012/13 and remained predominant until 2016/17. Children in PP or PW infected with RSV-A ON1 did not show a more severe clinical course of disease compared with RSV-A non-ON1 infections. In the PICU group, hospital stay was one day longer (median 8 days, inter-quartile range (IQR) 7–12 vs. 7 days, IQR 5–9; p = 0.02) and duration of oxygen treatment two days longer (median 6 days, IQR 4–9 vs. 4 days, IQR 2–6; p = 0.03) for children infected with RSV-A ON1. Conclusions In children, RSV-A ON1 largely replaced RSV-A non-ON1 genotypes within two seasons and remained the predominant RSV-A genotype in Germany during subsequent seasons. A higher clinical severity of RSV-A ON1 was observed within the group of children receiving PICU treatment, whereas in other settings clinical severity of RSV-A ON1 and non-ON1 genotypes was largely similar. KW - Children KW - Respiratory tract infection KW - RSV-A ON1 KW - Epidemiology KW - Disease severity Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-201516 VL - 19 ER - TY - JOUR A1 - Silwedel, Christine A1 - Speer, Christian P. A1 - Haarmann, Axel A1 - Fehrholz, Markus A1 - Claus, Heike A1 - Schlegel, Nicolas A1 - Glaser, Kirsten T1 - Ureaplasma species modulate cytokine and chemokine responses in human brain microvascular endothelial cells JF - International Journal of Molecular Science N2 - Ureaplasma species are common colonizers of the adult genitourinary tract and often considered as low-virulence commensals. Intraamniotic Ureaplasma infections, however, facilitate chorioamnionitis and preterm birth, and cases of Ureaplasma-induced neonatal sepsis, pneumonia, and meningitis raise a growing awareness of their clinical relevance. In vitro studies are scarce but demonstrate distinct Ureaplasma-driven impacts on immune mechanisms. The current study addressed cytokine and chemokine responses upon exposure of native or lipopolysaccharide (LPS) co-stimulated human brain microvascular endothelial cells (HBMEC) to Ureaplasma urealyticum or U. parvum, using qRT-PCR, RNA sequencing, multi-analyte immunoassay, and flow cytometry. Ureaplasma exposure in native HBMEC reduced monocyte chemoattractant protein (MCP)-3 mRNA expression (p < 0.01, vs. broth). In co-stimulated HBMEC, Ureaplasma spp. attenuated LPS-evoked mRNA responses for C-X-C chemokine ligand 5, MCP-1, and MCP-3 (p < 0.05, vs. LPS) and mitigated LPS-driven interleukin (IL)-1α protein secretion, as well as IL-8 mRNA and protein responses (p < 0.05). Furthermore, Ureaplasma isolates increased C-X-C chemokine receptor 4 mRNA levels in native and LPS co-stimulated HBMEC (p < 0.05). The presented results may imply immunomodulatory capacities of Ureaplasma spp. which may ultimately promote chronic colonization and long-term neuroinflammation. KW - Ureaplasma urealyticum KW - Ureaplasma parvum KW - neuroinflammation KW - meningitis KW - blood–brain barrier KW - HBMEC Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-201848 SN - 1422-0067 VL - 20 IS - 14 ER - TY - JOUR A1 - Silwedel, Christine A1 - Haarmann, Axel A1 - Fehrholz, Markus A1 - Claus, Heike A1 - Speer, Christian P. A1 - Glaser, Kirsten T1 - More than just inflammation: Ureaplasma species induce apoptosis in human brain microvascular endothelial cells JF - Journal of Neuroinflammation N2 - Background Ureaplasma species (spp.) are commonly regarded as low-virulent commensals but may cause invasive diseases in immunocompromised adults and in neonates, including neonatal meningitis. The interactions of Ureaplasma spp. with host defense mechanisms are poorly understood. This study addressed Ureaplasma-driven cell death, concentrating on apoptosis as well as inflammatory cell death. Methods Human brain microvascular endothelial cells (HBMEC) were exposed to Ureaplasma (U.) urealyticum serovar 8 (Uu8) and U. parvum serovar 3 (Up3). Resulting numbers of dead cells as well as mRNA levels and enzyme activity of key agents in programmed cell death were assessed by flow cytometry, RNA sequencing, and qRT-PCR, respectively. xCELLigence data were used for real-time monitoring of changes in cell adhesion properties. Results Both Ureaplasma isolates induced cell death (p < 0.05, vs. broth). Furthermore, Ureaplasma spp. enhanced mRNA levels for genes in apoptosis, including caspase 3 (Up3 p < 0.05, vs. broth), caspase 7 (p < 0.01), and caspase 9 (Up3 p < 0.01). Caspase 3 activity was increased upon Uu8 exposure (p < 0.01). Vice versa, Ureaplasma isolates downregulated mRNA levels for proteins involved in inflammatory cell death, namely caspase 1 (Uu8 p < 0.01, Up3 p < 0.001), caspase 4 (Uu8 p < 0.05, Up3 p < 0.01), NOD-like receptor pyrin domain-containing 3 (Uu8 p < 0.05), and receptor-interacting protein kinase 3 (p < 0.05). Conclusions By inducing apoptosis in HBMEC as main constituents of the blood-brain barrier, Ureaplasma spp. may provoke barrier breakdown. Simultaneous suppression of inflammatory cell death may additionally attenuate host defense strategies. Ultimate consequence could be invasive and long-term CNS infections by Ureaplasma spp. KW - Ureaplasma urealyticum KW - Ureaplasma parvum KW - Neuroinflammation KW - Meningitis KW - Caspase KW - Apoptosis KW - HBMEC Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-200711 VL - 16 ER - TY - JOUR A1 - Scheer, Monika A1 - Vokuhl, Christian A1 - Blank, Bernd A1 - Hallmen, Erika A1 - von Kalle, Thekla A1 - Münter, Marc A1 - Wessalowski, Rüdiger A1 - Hartwig, Maite A1 - Sparber-Sauer, Monika A1 - Schlegel, Paul-Gerhardt A1 - Kramm, Christof M. A1 - Kontny, Udo A1 - Spriewald, Bernd A1 - Kegel, Thomas A1 - Bauer, Sebastian A1 - Kazanowska, Bernarda A1 - Niggli, Felix A1 - Ladenstein, Ruth A1 - Ljungman, Gustaf A1 - Jahnukainen, Kirsi A1 - Fuchs, Jörg A1 - Bielack, Stefan S. A1 - Klingebiel, Thomas A1 - Koscielniak, Ewa T1 - Desmoplastic small round cell tumors: Multimodality treatment and new risk factors JF - Cancer Medicine N2 - Background To evaluate optimal therapy and potential risk factors. Methods Data of DSRCT patients <40 years treated in prospective CWS trials 1997-2015 were analyzed. Results Median age of 60 patients was 14.5 years. Male:female ratio was 4:1. Tumors were abdominal/retroperitoneal in 56/60 (93%). 6/60 (10%) presented with a localized mass, 16/60 (27%) regionally disseminated nodes, and 38/60 (63%) with extraperitoneal metastases. At diagnosis, 23/60 (38%) patients had effusions, 4/60 (7%) a thrombosis, and 37/54 (69%) elevated CRP. 40/60 (67%) patients underwent tumor resection, 21/60 (35%) macroscopically complete. 37/60 (62%) received chemotherapy according to CEVAIE (ifosfamide, vincristine, actinomycin D, carboplatin, epirubicin, etoposide), 15/60 (25%) VAIA (ifosfamide, vincristine, adriamycin, actinomycin D) and, 5/60 (8%) P6 (cyclophosphamide, doxorubicin, vincristine, ifosfamide, etoposide). Nine received high-dose chemotherapy, 6 received regional hyperthermia, and 20 received radiotherapy. Among 25 patients achieving complete remission, 18 (72%) received metronomic therapies. Three-year event-free (EFS) and overall survival (OS) were 11% (±8 confidence interval [CI] 95%) and 30% (±12 CI 95%), respectively, for all patients and 26.7% (±18.0 CI 95%) and 56.9% (±20.4 CI 95%) for 25 patients achieving remission. Extra-abdominal site, localized disease, no effusion or ascites only, absence of thrombosis, normal CRP, complete tumor resection, and chemotherapy with VAIA correlated with EFS in univariate analysis. In multivariate analysis, significant factors were no thrombosis and chemotherapy with VAIA. In patients achieving complete remission, metronomic therapy with cyclophosphamide/vinblastine correlated with prolonged time to relapse. Conclusion Pleural effusions, venous thrombosis, and CRP elevation were identified as potential risk factors. The VAIA scheme showed best outcome. Maintenance therapy should be investigated further. KW - C-reactive protein KW - desmoplastic small round cell tumor KW - maintenance therapy KW - soft tissue sarcoma KW - Trousseau's syndrome Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-228444 VL - 8 IS - 2 ER - TY - JOUR A1 - Ruf, Katharina A1 - Thomas, Wolfgang A1 - Brunner, Maximilian A1 - Speer, Christian P. A1 - Hebestreit, Helge T1 - Diverging effects of premature birth and bronchopulmonary dysplasia on exercise capacity and physical activity – a case control study JF - Respiratory Research N2 - Background Extreme prematurity has been associated with exercise intolerance and reduced physical activity. We hypothesized that children with bronchopulmonary dysplasia (BPD) would be especially affected based on long-term lung function impairments. Therefore, the objective of this study was to compare exercise capacity and habitual physical activity between children born very and extremely preterm with and without BPD and term-born children. Methods Twenty-two school-aged children (aged 8 to 12 years) born with a gestational age < 32 weeks and a birthweight < 1500 g (9 with moderate or severe BPD (=BPD), 13 without BPD (=No-BPD)) and 15 healthy term-born children (=CONTROL) were included in the study. Physical activity was measured by accelerometry, lung function by spirometry and exercise capacity by an incremental cardiopulmonary exercise test. Results Peak oxygen uptake was reduced in the BPD-group (83 ± 11%predicted) compared to the No-BPD group (91 ± 8%predicted) and the CONTROL group (94 ± 9%predicted). In a general linear model, variance of peak oxygen uptake was significantly explained by BPD status and height but not by prematurity (p < 0.001). Compared to CONTROL, all children born preterm spent significantly more time in sedentary behaviour (BPD 478 ± 50 min, No-BPD 450 ± 52 min, CONTROL 398 ± 56 min, p < 0.05) and less time in moderate-to-vigorous-physical activity (BPD 13 ± 8 min, No-BPD 16 ± 8 min, CONTROL 33 ± 16 min, p < 0.001). Prematurity but not BPD contributed significantly to explained variance in a general linear model of sedentary behaviour and likewise moderate-to-vigorous-physical activity (p < 0.05 and p < 0.001 respectively). Conclusion In our cohort, BPD but not prematurity was associated with a reduced exercise capacity at school-age. However, prematurity regardless of BPD was related to less engagement in physical activity and more time spent in sedentary behaviour. Thus, our findings suggest diverging effects of prematurity and BPD on exercise capacity and physical activity." KW - Bronchopulmonary dysplasia KW - Physical activity KW - Exercise testing KW - Preterm birth KW - Exercise capacity Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-202449 VL - 20 ER - TY - JOUR A1 - Ruf, Katharina A1 - Beer, Meinrad A1 - Köstler, Herbert A1 - Weng, Andreas Max A1 - Neubauer, Henning A1 - Klein, Alexander A1 - Platek, Kathleen A1 - Roth, Kristina A1 - Beneke, Ralph A1 - Hebestreit, Helge T1 - Size-adjusted muscle power and muscle metabolism in patients with cystic fibrosis are equal to healthy controls – a case control study JF - BMC Pulmonary Medicine N2 - Background Skeletal muscle function dysfunction has been reported in patients with cystic fibrosis (CF). Studies so far showed inconclusive data whether reduced exercise capacity is related to intrinsic muscle dysfunction in CF. Methods Twenty patients with CF and 23 age-matched controls completed an incremental cardiopulmonary cycling test. Further, a Wingate anaerobic test to assess muscle power was performed. In addition, all participants completed an incremental knee-extension test with 31P magnetic resonance spectroscopy to assess muscle metabolism (inorganic phosphate (Pi) and phosphocreatinine (PCr) as well as intracellular pH). In the MRI, muscle cross-sectional area of the M. quadriceps (qCSA) was also measured. A subgroup of 15 participants (5 CF, 10 control) additionally completed a continuous high-intensity, high-frequency knee-extension exercise task during 31P magnetic resonance spectroscopy to assess muscle metabolism. Results Patients with CF showed a reduced exercise capacity in the incremental cardiopulmonary cycling test (VO2peak: CF 77.8 ± 16.2%predicted (36.5 ± 7.4 ml/qCSA/min), control 100.6 ± 18.8%predicted (49.1 ± 11.4 ml/qCSA/min); p < 0.001), and deficits in anaerobic capacity reflected by the Wingate test (peak power: CF 537 ± 180 W, control 727 ± 186 W; mean power: CF 378 ± 127 W, control 486 ± 126 W; power drop CF 12 ± 5 W, control 8 ± 4 W. all: p < 0.001). In the knee-extension task, patients with CF achieved a significantly lower workload (p < 0.05). However, in a linear model analysing maximal work load of the incremental knee-extension task and results of the Wingate test, respectively, only muscle size and height, but not disease status (CF or not) contributed to explaining variance. In line with this finding, no differences were found in muscle metabolism reflected by intracellular pH and the ratio of Pi/PCr at submaximal stages and peak exercise measured through MRI spectroscopy. Conclusions The lower absolute muscle power in patients with CF compared to controls is exclusively explained by the reduced muscle size in this study. No evidence was found for an intrinsic skeletal muscle dysfunction due to primary alterations of muscle metabolism. KW - Cystic fibrosis KW - Exercise capacity KW - MRI spectroscopy KW - Muscle power KW - Phosphorylation KW - Lung disease, KW - Muscle function Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-200981 VL - 19 ER - TY - THES A1 - Riekert, Maximilian T1 - Der Einfluss mesenchymaler Stammzellen auf T-Zellsubpopulationen bei gesunden Probanden und Patienten mit rheumatischen Erkrankungen T1 - The influence of mesenchymal stem cells on T-cell subsets in healthy donors and patients with rheumatic diseases N2 - In dieser Arbeit wurde der Einfluss mesenchymaler Stammzellen (MSC) auf verschiedene T-Zellsubpopulationen in vitro untersucht. Dazu wurden Naive- und Nicht-Naive CD4+ T-Zellen aus humanen PBMCs von gesunden Probanden und Patienten mit Autoimmun-Arthritis bei rheumatischen Erkrankungen isoliert und im Beisein/in Abwesenheit von MSCs unter Th-17-polarisierenden Bedingungen kultiviert. Nach einer 6 Tage umfassenden Inkubationszeit erfolgte die flowzytometrische Bestimmung des Phänotyps, der Proliferation, der Apoptose, des Zytokinprofils und der Chemokinrezeptorexpression Naiver und Nicht-Naiver-CD4+ T-Zellen im Beisein/in Abwesenheit von MSCs. Die Phänotypen wurden als CD45RA+CD27+ Naive-, CD45RA-CD27+ Gedächtnis-, CD45RA- CD27- Effektor- und CD45RA+CD27- TEMRA-Zellen definiert und ihre jeweiligen prozentualen Anteile an allen CD4+ T-Zellen bestimmt. Nach Beurteilung der Proliferation und Apoptose, erfolgte die Analyse der IFNγ-, IL-17-, IL-9- und IL-13-Produktion für jeden der vier Phänotypen. Zusätzlich wurde der prozentuale Anteil an FoxP3+CD25+CD127- Tregs und deren IL-10-Produktion bestimmt. Abschließend erfolgte die Messung der CCR5-, CCR6- und CXCR3- Expression. Insgesamt konnte sowohl in der Naiven CD4+- als auch in der Nicht-Naiven CD4+ T- Zellfraktion eine Hemmung der Proliferation und Apoptose CD4+ T-Zellen durch MSCs gemessen werden. Zudem supprimierten MSCs die Produktion der Zytokine IFNγ, IL-17, IL-9 und IL-10 und steigerten teilweise die Produktion von antiinflammatorischem IL-13. In den vier untersuchten Phänotypen verhielt sich die Zytokinproduktion variabel und war bei CD45RA-CD27+ Gedächtnis- und CD45RA-CD27- Effektor-Zellen am größten. Der hemmende Einfluss der MSCs war auf diese beiden Phänotypen ebenfalls am stärksten ausgeprägt. CD45RA+CD27+ Naive- und CD45RA+CD27- TEMRA-Zellen produzierten in Kultur mit MSCs mitunter vermehrt proinflammatorische Zytokine. Analog zur Proliferation und Apoptose verminderten MSCs die Expression von CCR5, CCR6 und CXCR3 auf CD4+ T-Zellen. Die beschriebenen Effekte der MSCs konnten sowohl bei gesunden Probanden, als auch bei Patienten mit rheumatischen Erkrankungen nachgewiesen werden. Durch die Verwendung eines Transwell®-Systems konnte gezeigt werden, dass MSCs ihre Wirkung auf T-Lymphozyten nicht nur durch direkten Zell-Zell-Kontakt, sondern auch über lösliche Faktoren ausüben. Die Resultate dieser Arbeit verdeutlichen den immunsuppressiven Charakter der MSCs auf Naive und Nicht-Naive CD4+ T-Zellen unter Th17-polarisierenden Bedingungen in vitro. Jedoch zeigt die Analyse der Zytokinproduktion in den untersuchten T-Zell-Phänotypen, dass MSCs neben ihrer immunsuppressiven Eigenschaft die Zytokinantwort einzelner T-Zellphänotypen steigern können. MSCs scheinen daher am ehesten eine immunmodulatorische Rolle zu spielen, indem sie übersteigerte Immunreaktionen herabsetzen und bei Bedarf immunstimulierend wirken. N2 - In this thesis the influence of mesenchymal stem cells (MSCs) on different T cell subsets was investigated in vitro. Naive- and Non-Naive CD4+ T cells were isolated from human PBMCs of healthy donors and patients with rheumatic diseases and cultured in presence/in absence of MSCs under Th17 polarizing conditions. After incubation for six days phenotype, proliferation, apoptosis, cytokine profile and expression of chemokine receptors of Naive- and Non-Naive CD4+ T cells in presence/in absence of MSCs was determined by flow cytometry. T cell subsets were defined as CD45RA+CD27+ Naive, CD45RA-CD27+ Memory, CD45RA-CD27- Effektor and CD45RA+CD27- TEMRA cells and the percentage of total CD4+ T cells was calculated. After assessing proliferation and apoptosis, production of IFNγ, IL-17, IL-9 and IL-13 was analyzed for each of the four subsets. Additionally, the percentages of FoxP3+CD25+CD127- Tregs and the corresponding production of IL-10 were determined. Finally, the expression of chemokine receptors CCR5, CCR6 and CXCR3 was measured. In both the Naive and Non-Naive CD4+ cell fraction an inhibition of proliferation and apoptosis of CD4+ T cells through MSCs was analyzed. Moreover, MSCs suppressed the production of the cytokines IFNγ, IL-17, IL-9 and IL-10 and partially enhanced the production of IL-13. The cytokine production varied in the four analyzed T cell subsets, with the highest cytokine production among CD45RA-CD27+ Memory and CD45RA-CD27- Effector cells. The inhibiting influence of MSCs on these two subsets was most prominent. CD45RA+CD27+ Naive and CD45RA+CD27- TEMRA cells occasionally produced more proinflammatory cytokines in culture with MSCs. Like similar effects of MSCs on proliferation and apoptosis, MSCs diminished the expression of CCR5, CCR6 and CXCR3 on CD4+ T cells. The effects of MSCs were demonstrated in both, healthy donors and patients with rheumatic diseases. By the use of a Transwell®-System it was shown that MSCs exert their effects not only through direct cell-cell-contact but also by soluble factors. The results of this thesis elucidate the immunosuppressive character of MSCs on Naive and Non-Naive CD4+ T cells under Th17-polarizing conditions in vitro. However, the analysis of the cytokine production in the investigated T cell subsets showed, that MSCs are able to enhance the immune response besides their immunosuppressive properties. Therefore, MSCs most likely seem to play an immunomodulatory role, by reducing exaggerated immune reactions and, if required are also able to act immune stimulating. KW - mesenchymal KW - stem KW - cell KW - Rheuma KW - Mesenchymale Stammzellen KW - Mesenchymal Stem Cells KW - Rheuma KW - Immunologie KW - Immunology KW - T-Zellen KW - T-Cells KW - Subpopulationen KW - Subsets Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-178195 ER - TY - THES A1 - Rasche, Engelke Kristina T1 - Einfluss der Zytokingenpolymorphismen bei allogen transplantierten Kindern auf das Vorliegen einer Graft-versus-Host-Disease T1 - Influence of cytokine polymorphisms in allogeneic transplanted children on the presence of graft-versus-host disease N2 - Im Rahmen dieser Arbeit wurden 72 pädiatrische Patienten, die eine allogene Stammzelltransplantation erhielten, auf die Spender- und Empfänger-Zytokinpolymorphismen TNF-α, TGF-β1, IL-10, IL-6 und IFN-γ untersucht. Die Proben wurden mittels DNA-Extraktion, sequenzspezifischer PCR und Gelelektrophorese analysiert und auf deren Einfluss auf die Entstehung und den Verlauf maligner Erkrankungen sowie auf die Entstehung einer GvHD untersucht. N2 - Within the scope of this work, 72 pediatric patients who received allogeneic stem cell transplantations were examined for the donor and recipient cytokine polymorphisms TNF-α, TGF-β1, IL-10, IL-6 and IFN-γ. We analyzed the samples by means of DNA extraction, sequence-specific PCR and gel electrophoresis and investigated their influence on the development and course of malignant diseases as well as on the development of a GvHD. KW - allogeneic KW - Graft-versus-host-disease KW - Stammzelltransplantation KW - stem cell transplantation Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-179401 ER - TY - THES A1 - Paul, Luisa T1 - Charakterisierung von Individuen mit heterozygoter IGHD-Variante hinsichtlich B-Zell Differenzierung, Immunglobulin-Repertoire Entwicklung und Entstehung eines Antikörpermangels T1 - Characterization of individuals with heterozygous IGHD variant regarding B cell differentiation, immunoglobulin repertoire development and development of an antibody deficiency N2 - Die Expression eines funktionsfähigen BZR ist essentiell für die Entwicklung und Differenzierung von B-Zellen, für deren Toleranzinduktion und Sekretion protektiver Antikörper. Genetisch bedingte Defekte im BZR-Signaltransduktionsweg liegen den primären Immundefekten mit vorwiegendem Antikörpermangel („humoraler Immundefekt“) zu Grunde. Naive B-Zellen in der Peripherie exprimieren den BZR als zwei Isotypen (IgM und IgD), wohingegen unreife B-Zellen im Knochenmark nur IgM exprimieren. Die Bedeutung für diese differentielle IgM/IgD-Expression ist nicht bekannt. Es wird jedoch der Expression von IgD eine Rolle in der Generierung hochaffiner Antikörper und in der Regulation von B-Zell Toleranz zugeschrieben. In dieser Arbeit wurden die Familienmitglieder einer Indexpatientin klinisch, immunologisch und genetisch charakterisiert. Bei der Indexpatientin wurde ein Immundefekt im Sinne eines CVID diagnostiziert. Es zeigte sich eine auffällige Expression von IgD auf naiven B-Zellen, zudem konnte eine Variante in dem für IgD kodierenden IGHD-Gen nachgewiesen werden. Es konnte keine Korrelation zwischen dem Auftreten des Immundefektes und der p.Pro6Leu IGHD-Variante nachgewiesen werden. Ebenso zeigte sich bei den Trägern der IGHD-Variante kein Hinweis auf eine Störung der B-Zell Differenzierung oder ein Defekt der spezifischen Antikörperproduktion. Somit scheint die untersuchte p.Pro6Leu IGHD-Variante nicht ursächlich für den klinischen und immunologischen Phänotyp der Indexpatientin zu sein. Inwieweit die Variante ein relatives Risiko für die Entwicklung eines CVID darstellt, kann aus der Untersuchung der Familie nicht beurteilt werden und müsste in einer größeren CVID-Kohorte evaluiert werden. Da aus Untersuchungen von transgenen/knock-out Mausmodellen eine Bedeutung von IgD für die Regulation der peripheren B-Zell Toleranz vermutet wird, nutzten wir in dieser Arbeit charakterisierte heterozygote Träger der IGHD-Variante als „genetisches Modell“ zur Analyse der Bedeutung von IgD für die Entwicklung des Immunglobulin-Repertoires naiver B-Zellen des Menschen. Die durch allelische Exklusion bedingte chimäre Situation der IgD-Expression naiver B-Zellen bei heterozygoten IGHD-Variantenträgern machte den direkten Vergleich zwischen IgD+ Wildtyp-Populationen und IgD- Mutante im gleichen Organismus möglich. In den Untersuchungen des Immunglobulin-Repertoires von transitionalen und reifen, naiven B-Zellen in diesen Individuen zeigten sich jedoch keine wegweisenden Unterschiede zwischen IgD+ und IgD- Populationen. Insbesondere auch charakteristische Motive des Immunglobulin-Repertoires, die auf eine Autoreaktivität des kodierten Immunglobulins hin¬weisen (VH4-34 Gensegment, lange CDR3-Region, positive Ladung und Hydrophobizität der CDR3-Region) waren nicht unterschiedlich zwischen beiden Zellpopulationen. Somit scheint entweder die Expression von IgD auf naiven B-Zellen beim Menschen keinen Einfluss auf die Immunglobulin-Repertoire Entwicklung und die Regulation der Toleranzinduktion zu haben oder die verwendete Methodik ist nicht sensitiv genug, um mögliche Auffälligkeiten zu detektieren. Hier würde sich für zukünftige Untersuchungen des Immunglobulin-Repertoires eine Hochdurchsatzsequenzierung mittels next-generation sequencing und für die Analyse der Autoreaktivität die Expression und Reaktivitätstestung monoklonaler Antikörper aus individuellen B-Zellen anbieten. N2 - The expression of a functional BZR is essential for the development and differentiation of B-cells, for their tolerance induction and secretion of protective antibodies. Genetic defects in the BZR signal transduction pathway are based on the primary immunodeficiencies with predominant antibody deficiency ("humoral immune deficiency"). Naive B-cells in the periphery express the BZR as two isotypes (IgM and IgD), whereas immature B-cells express only IgM in the bone marrow. The significance for this differential IgM / IgD expression is unknown. However, the expression of IgD is thought to play a role in the generation of high affinity antibodies and in the regulation of B cell tolerance. In this study, the family members of an index patient were characterized clinically, immunologically and genetically. The index patient was diagnosed with an immunodeficiency in the sense of a CVID. There was a conspicuous expression of IgD on naive B-cells as well as a variant in the IGHD gene coding for IgD. There was no correlation between the occurrence of the immunodeficiency and the p.Pro6Leu IGHD variant. Similary, the carriers of the IGHD Variant showed no evidence of a disturbance of the B-cell differentiation or a defect in the specific antibody production. Thus, the investigated p.Pro6Leu IGHD variant does not seem to be causative for the clinical and immunological phenotype of the index patient. The extent to which the variant poses a relative risk for the development of a CVID can not be assessed from the family examination and would have to be evaluated in a larger CVID cohort. Since investigations of transgenic / knock-out mouse models suggest an interpretation of IgD for the regulation of peripheral B-cell tolerance, we used heterozygous carriers of the IGHD variant characterized in this work as a "genetic model" to analyze the significance of IgD for the development of the immunoglobulin repertoire of naive human B-cells. The chimeric situation of IgD expression of naive B-cells in heterozygous IGHD variant carriers caused by allelic exclusion made a direct comparison possible between IgD + wild-type populations and IgD mutants in the same organism. However, studies of the immunoglobulin repertoire of transitional and mature, naive B cells in these individuals, did not reveal any landmark differences between IgD + and IgD populations were found. In particular, characteristic motifs of the immunoglobulin repertoire indicating autoreactivity of the encoded immunoglobulin (VH4-34 gene segment, long CDR3 region, positive charge and hydrophobicity of the CDR3 region) were not different between the two cell populations. Thus, either the expression of IgD on naive B-cells in humans does not seem to have any effect on the immunoglobulin repertoire development and the regulation of tolerance induction or the methodology used is not sensitive enough to detect possible abnormalities. For future investigations of the immunoglobulin repertoire a high-throughput sequencing by next-generation sequencing and for the analysis of autoreactivity the expression and reactivity testing of monoclonal antibodies from individual B-cells would be appropriate. KW - Immundefekt KW - Durchflusscytometrie KW - Immunglobulin D KW - IGHD-Variante KW - B-Zell Differenzierung KW - Immunglobulin-Repertoire KW - CVID Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-185210 ER - TY - JOUR A1 - Nothhaft, Matthias A1 - Klepper, Joerg A1 - Kneitz, Hermann A1 - Meyer, Thomas A1 - Hamm, Henning A1 - Morbach, Henner T1 - Hemorrhagic bullous Henoch-Schönlein Purpura: case report and review of the literature JF - Frontiers in Pediatrics N2 - Henoch-Schönlein Purpura (HSP) or IgA vasculitis is the most common systemic vasculitis of childhood and may affect skin, joints, gastrointestinal tract, and kidneys. Skin manifestations of HSP are characteristic and include a non-thrombocytopenic palpable purpura of the lower extremities and buttocks. Rarely, HSP may initially present as or evolve into hemorrhagic vesicles and bullae. We present an otherwise healthy 5-year-old boy with an acute papulovesicular rash of both legs and intermittent abdominal pain. After a few days the skin lesions rapidly evolved into palpable purpura and hemorrhagic bullous lesions of variable size and severe hemorrhagic HSP was suspected. A histological examination of a skin biopsy showed signs of a small vessel leukocytoclastic vasculitis limited to the upper dermis and direct immunofluorescence analysis revealed IgA deposits in vessel walls, compatible with HSP. To further characterize the clinical picture and treatment options of bullous HSP we performed an extensive literature research and identified 41 additional pediatric patients with bullous HSP. Two thirds of the reported patients were treated with systemic corticosteroids, however, up to 25% of the reported patients developed skin sequelae such as hyperpigmentation and/or scarring. The early use of systemic corticosteroids has been discussed controversially and suggested in some case series to be beneficial by reducing the extent of lesions and minimizing sequelae of disease. Our patient was treated with systemic corticosteroids tapered over 5 weeks. Fading of inflammation resulted in healing of most erosions, however, a deep necrosis developing from a large blister at the dorsum of the right foot persisted so that autologous skin transplantation was performed. Re-examination 11 months after disease onset showed complete clinical remission with re-epithelialization but also scarring of some affected areas. KW - henoch-schönlein purpura KW - vasculitis KW - hemorrhagic KW - bullae KW - children Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-201435 VL - 6 ER - TY - JOUR A1 - Nentwich, Julia A1 - Ruf, Katharina A1 - Girschick, Hermann A1 - Holl-Wieden, Annette A1 - Morbach, Henner A1 - Hebestreit, Helge A1 - Hofmann, Christine T1 - Physical activity and health-related quality of life in chronic non-bacterial osteomyelitis JF - Pediatric Rheumatology N2 - Background Chronic non-bacterial osteomyelitis (CNO) is an autoinflammatory disorder of the skeletal system of yet unknown etiology. Patients present with local bone pain and inflammation and - to our experience - often suffer from functional impairment with significant disabilities of daily life. The objective of this study was to assess physical activity, fitness and health-related quality of life (HRQOL) in adolescents with established diagnosis of CNO versus healthy controls (HC). Methods 15 patients with CNO and 15 age and gender matched HC aged 13–18 years, completed questionnaires, performed an incremental exercise test with gas exchange measures up to voluntary fatigue and wore an accelerometer over 7 days at home to assess physical activity behavior. Results At the time of assessment, 5 CNO patients were in clinical, one in radiological and 5 in clinical and radiological remission. 7 did not receive any therapy at the time of assessment. The results of the exercise test and of the accelerometry did not show any significant difference between CNO and HC. However, reported sports participation was lower in patients with CNO and PedsQL3.0 and 4.0 showed significant lower values in most of the scores indicating reduced HRQOL. Conclusion Although most CNO patients showed a favorable course of disease without any relevant differences in objective measurements of physical activity and fitness versus HC at the time of assessment, questionnaires revealed perceived limitations. Further studies are needed to measure HRQOL and to validate questionnaires in patients with CNO against objective measures including more participants with a higher level of disease activity. KW - chronic non-bacterial osteomyelitis KW - CRMO KW - HRQOL KW - physical activity Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-323710 VL - 17 ER - TY - THES A1 - Lippert, Lena T1 - Untersuchung der Diversität des T-Zellrezeptor-Repertoires mittels CDR3-Längen Spectratyping im Rahmen der Immunrekonstitution nach CD3/19-depletierter versus CD34-positiv selektionierter Stammzelltransplantation bei pädiatrischen Patienten T1 - Examination of the diversity of the t-cell-receptor-repertoire using CDR3-length-spectratyping after CD3/19 depleted stem cell grafts versus CD34+ selected stem cell grafts in pediatric patients N2 - In unseren Untersuchungen zogen wir einen Vergleich zwischen dem Verlauf der Immunkonstitution bei Kindern nach CD3/19 depletierter Stammzell-Transplantation und historischen Daten von Kindern nach CD34+ selektionierter Stammzell-Transplantation. In der Frühphase nach Transplantation zeigen sich in unseren Ergebnissen signifikante Vorteile nach CD3/19 Depletion, insbesondere hinsichtlich des numerischen NK- sowie der T-Zell-Rekonstruktion. Auch qualitativ sahen wir vor Tag +100 anhand unserer Ergebnisse der CDR3-Längen-Analyse des TZR-Repertoires eine höhere Komplexizität nach CD3/19-Depletion. Zu einem späteren Zeitpunkt (>200d) zeigte sich auf Seite der CD34+-Selektionierten eine etwas bessere Repertoirekomplexizität. Zusammenfassend sehen wir die CD3/19-Depletion als eine positive Weiterentwicklung der T-Zell-Depletion bei haploidenter Stammzelltransplantation. N2 - In our studies we compared the process of childrens immune reconstitution between CD3/19 depleted stem cell Transplantation and historical data of children after CD34+ selected stem cell Transplantation. In the early Phase according to Transplantation, significant benefits were shown in the patients after CD3/19 depleted stem cell Transplantation, particularly regarding the numeric natural killer cells as well as within the T-cell reconstitution. Before day +100 we recognized, based on our results of a CDR3-lengths Analysis of the T cell receptor-Repertoire, a higher Quality of complexicity according to a CD3/19-depletion. Later in time (>day +200)a slight improvement could be discovered on side of the patients after CD34+ selected stem cell Transplantation regarding the repertoire-complexicity. As a summary we recognise the CD3/19-depletion as a positive development in the t-cell-depletion within haploidentical stem cell transplantation. KW - Haploidentical KW - CD3/19 depletierte Stammzelltransplantation KW - Immunoscope Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-185739 ER - TY - JOUR A1 - Kunzmann, S. A1 - Ngyuen, T. A1 - Stahl, A. A1 - Walz, J. M. A1 - Nentwich, M. M. A1 - Speer, C. P. A1 - Ruf, K. T1 - Necrotizing enterocolitis after intravitreal bevacizumab in an infant with Incontinentia Pigmenti – a case report JF - BMC Pediatrics N2 - Background Incontinentia Pigmenti is a rare disease affecting multiple organs. Fifty of patients show affection of the eye with retinopathy and possible amaurosis being the worst outcome. Treatment has commonly been panretinal laser coagulation but intravitreal application of bevacizumab as VEGF-inhibitor has shown to effectively suppress retinal neovascularization. Case presentation A six-week-old female infant with Incontinentia Pigmenti developed a foudroyant necrotizing enterocolitis shortly after intravitreal injection of bevazicumab due to a retinopathy with impending tractional detachment of the left eye. Since the onset of abdominal symptoms occurred immediately after the intravitreal application, a link between the two events seemed likely. Sequential analyses of the VEGF serum concentrations showed a massive suppression of endogenous VEGF with only a very slow recovery over weeks. Such a severe systemic adverse event has not been reported after intravitreal treatment with bevacizumab in an infant. Conclusion This case report shows a relevant systemic uptake of bevacizumab after intravitreal application as suppressed VEGF levels show. There seems to be a connection between suppressed VEGF levels and the onset of necrotizing enterocolitis. Therefore, treatment with bevacizumab should be carefully considered and further research is needed to assess this drug’s safety profile. KW - Necrotizing enterocolitis KW - Incontinentia pigmenti KW - Bevacizumab KW - Retinopathy KW - VEGF Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-201024 VL - 19 ER - TY - JOUR A1 - Krakow, Sören A1 - Crescimone, Marie L. A1 - Bartels, Charlotte A1 - Wiegering, Verena A1 - Eyrich, Matthias A1 - Schlegel, Paul G. A1 - Wölfl, Matthias T1 - Re-expression of CD14 in response to a combined IL-10/TLR stimulus defines monocyte-derived cells with an immunoregulatory phenotype JF - Frontiers in Immunology N2 - Interleukin 10 is a central regulator of the antigen-presenting function of myeloid cells. It exerts immunomodulatory effects in vivo and induces a regulatory phenotype in monocyte-derived cells in vitro. We analyzed phenotype and function of monocytic cells in vitro in relation to the cytokine milieu and the timing of TLR-based activation. In GM-CSF/IL-4 cultured human monocytic cells, we identified two, mutually exclusive cell populations arising from undifferentiated cells: CD83\(^+\) fully activated dendritic cells and CD14\(^+\) macrophage like cells. Re-expression of CD14 occurs primarily after a sequential trigger with a TLR signal following IL-10 preincubation. This cell population with re-expressed CD14 greatly differs in phenotype and function from the CD83+ cells. Detailed analysis of individual subpopulations reveals that exogenous IL-10 is critical for inducing the shift toward the CD14\(^+\) population, but does not affect individual changes in marker expression or cell function in most cases. Thus, plasticity of CD14 expression, defining a subset of immunoregulatory cells, is highly relevant for the composition of cellular products (such as DC vaccines) as it affects the function of the total product. KW - regulatory dendritic cells KW - MDSC KW - monocyte-derived DC KW - IL-10 KW - macrophages Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-201537 VL - 10 IS - 1484 ER - TY - THES A1 - Knecht [geb. Hauk], Franziska T1 - Der Einfluss der Ernährung auf das autonome Nervensystem – ein Modell kindlicher Essstörungen T1 - The impact of nutrition on the autonomic nervous system – a model of eating disorders in childhood N2 - Essstörungen sind durch eine autonome Regulationsstörung gekennzeichnet, die vermutlich pathophysiologisch relevant ist. Es konnte gezeigt werden, dass in unterschiedlichen Ernährungszuständen das autonome Nervensystem (ANS) verschieden reguliert wird. Adipöse Kinder weisen im Vergleich zu gesunden Gleichaltrigen eine reduzierte Herzfrequenzvariabilität (HRV) und einen erniedrigten Vagotonus auf, während Anorexia nervosa (AN)-Patienten eine erhöhte HRV mit Vagusdominanz besitzen. Während das momentane Körpergewicht und der aktuelle Body Mass Index (BMI) im Verlauf einer Ernährungsintervention weitgehend konstant bleiben, entwickelt sich die HRV nachhaltig positiv. Es konnte ein qualitativer Zusammenhang zwischen der Änderung des BMI und der HRV-Änderung nachgewiesen werden. Offensichtlich reagiert das ANS im Sinne einer „autonomen Wende“ auf die Ernährungsumstellung, noch bevor eine signifikante Änderung des Körpergewichts messbar wird. Der Reiz für die Anpassung des ANS liegt scheinbar in der Dynamik metabolischer Zustände, initiiert durch Änderung der Kalorienzufuhr, und wirkt sich erst langfristig auf den BMI aus. Am Beispiel der Anorexia nervosa führt das Refeeding aus einer Kalorienzufuhr gemäß modifiziertem NICE-Ernährungsprotokoll, mit Supplementierung von Vitamin B-Komplexen sowie Omega-3-Fettsäuren (O-3-FS), bereits frühzeitig zu einer „autonomen Wende“ mit Regulierung der HRV in Richtung altersentsprechenden Normbereich. Die autonome Regulationsstörung ist möglicherweise weniger die Ursache als die Folge des Hungerns bei AN. Die HRV ist bei adipösen Kindern reduziert und spiegelt so einen frühen kardiovaskulären Risikofaktor wider. Durch Ernährungsinterventionen zeigen sich zwar oft nur leichte Erfolge bei der Gewichtsreduzierung, jedoch können signifikante HRV-Verbesserungen, insbesondere in der Nacht, erreicht werden. Diese HRV-Zunahme gilt als Indikator für ein reduziertes kardiovaskuläres Risiko, das offensichtlich durch eine Ernährung knapp unterhalb des Solls erreicht werden kann. Das HRV-Profil adipöser Kinder und Jugendliche spiegelt sich auch abgestuft in der Einteilung in die verschiedenen Risikogruppen des Metabolischen Syndroms wider. Die HRV dient demzufolge bei Kindern und Jugendlichen als verlässlicher Surrogatparameter für das kardiovaskuläre Risiko. Pathophysiologisch ist ein Modell des normokalorischen Ernährungszustands anzunehmen, in dem das autonome Nervensystem in individuell bestimmten Grenzen ausgewogen reguliert wird. Aus einer Änderung der Ernährung resultiert ein autonomer Effekt: die vagotone Ausgangslage der AN-Patienten wird durch Refeeding positiv beeinflusst (HRV-Abnahme, Herzfrequenzanstieg); umgekehrt verhält es sich durch Kalorienrestriktion bei Adipositas (HRV-Zugewinn, Herzfrequenzabnahme). Der HF/LF (high frequency/low-frequency)-Quotient, als möglicher Repräsentant der autonomen Balance, bleibt jedoch unverändert. Bei kalorischer Unter- oder Überversorgung wird die intrinsische Herzfrequenz unabhängig vom Sympathikus-Parasympathikus-Gleichgewicht angepasst. VLF (very low frequency) kann wahrscheinlich als metabolischer Parameter angesehen werden und verhält sich umgekehrt proportional zur Thermogenese. Die metabolisch bedingten Veränderungen der autonomen Regulation werden durch Optimierung der Kalorienzufuhr unabhängig vom aktuellen BMI aufgehoben und normalisiert. Diese Anpassungsmechanismen werden offensichtlich auch von psychischen Veränderungen begleitet, die eine Verhaltensänderung der Kinder und Jugendliche bedingen. Im Rahmen der Essstörungen gilt diese Beobachtung als besonderes Therapiehindernis. O-3-FS und Betablocker haben möglicherweise einen zusätzlichen positiven Effekt auf die HRV. Die Orientierung am BMI als Messparameter für Interventionserfolg ist unzulänglich. Effekte einer hypo- bzw. hyperkalorischen Ernährung auf die HRV bzw. intrinsische Herzrate lassen sich einfach erfassen und sind im Langzeit-Elektrokardiogramm (LZ-EKG) zugängig. Therapieeffekte sind anhand der HRV-Analyse noch vor Änderung des BMI sichtbar. Die im LZ-EKG einfach praktikable HRV-Messung dient als objektive und aktuelle Diagnostik für die Therapiebewertung bei Essstörungen. Angesichts der Kenntnis um die Präsenz einer autonomen Regulationsstörung im Vorfeld vieler kardiovaskulärer Erkrankungen, verspricht die HRV-Analyse zukünftig präventiven Nutzen. N2 - Eating disorders are characterized by an autonomic dysfunction, measured by 24 hour heart rate variability (HRV) analysis, that is thought to be pathophysiologically relevant. Obese children have a reduced HRV and a decreased vagal tone compared to healthy peers, reflecting an early cardiovascular risk factor. In contrast, anorexia nervosa (AN) patients have an increased HRV with vagus dominance and respond poorly to treatment. It has been shown that the autonomic nervous system (ANS) is differently regulated depending on the nutritional state. The HRV profile also reflectes graded risk scores of the development of the metabolic syndrome. While the current body weight and the body mass index (BMI) remain largely constant in the course of a nutritional intervention, the HRV improves sustainably, especially at night. A correlation between the change in BMI and the HRV change could be demonstrated. Obviously, the ANS reacts to the change in diet in the sense of an "autonomous turn" even before a significant change in body weight becomes measurable. The stimulus for adapting ANS appears to be in the dynamics of metabolic states initiated by changes in caloric intake, and only affects BMI in the long term. Pathophysiologically, a model of the normocaloric nutritional state is assumed, in which the autonomic nervous system is balanced in individually determined limits. A change in diet results in an autonomous effect, independent of the current BMI: the vagotone starting position of the AN patients is positively influenced by refeeding (HRV decrease, increase in heart rate) and contrary changes occur among the obese children with optimized diet. However, the HF / LF (high frequency / low-frequency) quotient, as a possible representative of the autonomous balance, remains unchanged. Thus, in caloric under- or oversupply, the intrinsic heart rate is adjusted independently of the sympatho-vagal balance. VLF (very low frequency) can probably be considered as a metabolic parameter. O-3-FS and beta-blockers may have an additional positive effect on HRV. Dietary interventions often provide only modest weight-change benefits, but significant HRV improvements can be achieved. Therefore, focussing on BMI as major measuring parameter for intervention success is inadequate. HRV serves as a reliable surrogate parameter for cardiovascular risk in children and adolescents and promises future preventive benefits. KW - Herzfrequenzvariabilität KW - Anorexia nervosa KW - Adipositas KW - Essstörung KW - Autonomes Nervensystem KW - heart rate variability KW - eating disorder KW - childhood obesity KW - anorexia Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-174725 ER - TY - THES A1 - Klopsch, Bernhard Wolfgang T1 - Expression und Immunogenität von Melan-A in Glioblastomzellen T1 - Expression and Immunogenicity of Melan-A in Glioblastoma Cells N2 - Da mit der derzeitigen Therapie des Glioblastom bei Kindern die 2-Jahres Überlebensrate bei 26% liegt, wird die Suche nach neuen Therapiemöglichkeiten vorangetrieben. Die Immuntherapie könnte die Möglichkeiten einer spezifischen möglichst nebenwirkungsarmen Therapie bieten. Bereits bei Rezidiven werden bestehende Therapieverfahren z.B. mit monoklonalen Antikörpern wie Bevazizumab (Anti-VEGF) kombiniert und getestet. Auch die adoptive T-Zell-Therapie ist ein vielversprechender Ansatz. Ein wichtiger Faktor für eine erfolgreiche Therapie ist aber die Auswahl geeigneter Tumorantigene. Melan-A ist ein in der Immuntherapie der malignen Melanome gut charakterisiertes und mehrfach eingesetztes Ziel. Dies beruht unter anderem auf der Eigenschaft, in vitro tumorspezifische CD8+ T-Zellen in großer Zahl expandieren zu können. Angesichts der gemeinsamen neuroektodermalen Herkunft von Melanozyten und glialen Zellen gibt es Berichte, in denen MelanA in Gliomen nachgewiesen werden konnte. In dieser Arbeit wurde mit eigenen experimentellen Daten nochmals exakt nachvollzogen, inwieweit Melan-A als Tumorantigen bei Glioblastomen eine relevante Zielstruktur sein könnte. Dies wurde mit verschiedenen Methoden wie intrazelluläre Färbung, Cytospins, Realtime PCR, Westernblot und Immunhistochemie untersucht. Darüber hinaus unterstreichen die Ergebnisse auch die Bedeutung von potenziellen Kreuzreaktionen, die grundsätzlich für jeden T-Zell-Rezeptor auftreten können, möglicherweise aber gerade bei dem Melan-A-Epitop eine größere Relevanz haben. N2 - Cellular immunotherapy using tumor-specific T-cells may be an additional, beneficial treatment strategy to improve the overall poor prognosis of patients with glioblastoma, a malignant, gliale braintumor. Several suitable tumor-associated antigens have been described, some of which being also expressed in melanoma, due to the common neuroectodermal origin of melanocytes and glial cells. One of the best described melanosomal tumor/self-antigens is Melan-A /Mart-1, which has been targeted in several clinical immunotherapy trials for melanoma patients. Data available on expression of Melan-A in glioblastoma cell lines and samples is scarce, but recognition of glioblastoma cell lines has been described by J.G. Zhang et al.. As functional peptide-specific T-cells for the Melan-A derived HLA-A2 restricted, heteroclitic peptide (26-35L) can be easily expanded to large numbers using our recently published protocol, we asked, whether Melan-A would be a suitable target for immunotherapy in glioblastoma patients. KW - Glioblastom KW - Immuntherapie KW - Tumorantigen KW - Melan-A Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-192036 ER - TY - THES A1 - Härlein, Miriam T1 - Epidemiologie und Klinik respiratorischer Viruserkrankungen bei Kindern der Universitätskinderklinik Würzburg in den Jahren 2012 bis 2014 T1 - Epidemiology und clinical characteristics of virus associated acute respiratory infections in children at the University Hospital of Würzburg in 2012 until 2014 N2 - Ziel dieser retrospektiven, monozentrischen Studie war es, die virale Ätiologie und die klinischen Charakteristika bei hospitalisierten Kindern und Jugendlichen unter 17 Jahren mit ARE an der Universitäts-Kinderklinik Würzburg im Zeitraum Juni 2012 – Juni 2014 zu untersuchen. Die Virusdiagnostik erfolgte dabei aus respiratorischen Sekreten mittels Multiplex-RT-PCR für 18 respiratorische Viren. Es wurden insgesamt 960 Kinder mit ARE und Multiplex-PCR-Testung auf respiratorische Viren in die Untersuchung eingeschlossen. 566 Kinder (59%) waren männlich. Der Altersmedian betrug 1,9 Jahre (IQR 1,0-4,4). Die Patienten befanden sich im Median 3 Tage (IQR 2-5) in stationärer Behandlung. Die häufigsten mit ARE assoziierten Symptome waren Fieber (n=538, 56%), Husten (n=527, 55%) und Nahrungs-/ Trinkverweigerung (n=382, 40%). Bei 52% der Patienten (n=502) lag eine URTI und bei 48% (n=458) eine LRTI vor. Ca. 50% der Kinder (n=481) hatten eine oder mehrere Vorerkrankungen, wobei eine bestehende chronische Lungenerkrankung mit 18% (n=176) und Frühgeburtlichkeit (n=100, 10%) die häufigsten prädisponierenden Faktoren darstellten. 13 Kinder (1,4%) benötigten eine intensivstationäre Betreuung. 460 Kinder (48%) erhielten initial eine antibiotische Therapie. 168 Kinder (18%) benötigten eine Sauerstofftherapie. Zwei Kinder (0,2%) starben bei vorher bestehender Grunderkrankung. Zusammenfassend konnte in dieser Dissertation gezeigt werden, dass hospitalisierte Kinder mit LRTI, mit positivem Virusnachweis oder mit einer viralen Koinfektion wesentlich jünger waren als Kinder mit URTI, negativem Virusnachweis oder viraler Monoinfektion. Zudem wurde vor allem bei Kindern mit hMPV- oder RSV-Nachweis ein schwererer klinischer Verlauf verzeichnet, wobei sich insbesondere hMPV als häufigster Erreger bei Kindern mit viraler Pneumonie herausstellte. Insgesamt spiegeln die Studienergebnisse die hohe Krankheitslast der viral bedingten ARE im Kindesalter wieder, welche trotz vielseitiger Bestrebungen zu konsequenten Hygienemaßnahmen nur begrenzt reduziert werden können. Obwohl eine symptomatische Therapie mehrheitlich zu einer raschen Genese der Kinder führt, wäre der differenziertere und folglich reduzierte Einsatz einer Antibiotikatherapie unter Einbezug einer standardisierten Virusdiagnostik wünschenswert. N2 - In Germany, data on the aetiology, epidemiology and clinical characteristics of virus associated acute respiratory infections (ARI) in children with is limited. In a single-centre tertiary care pediatric hospital, respiratory specimens in children <17 years of age hospitalized with ARI were routinely tested by multiplex-PCR for 21 viral pathogens from July 2012 to June 2014. Clinical data were collected from hospital medical records using a standardized questionnaire. A total of 942 ARI patients (52.2% upper ARI; 47.8% lower ARI) with a median age of 23 months (IQR 12-53) were enrolled. Virus-positive children (n=696, 73.9%) were significantly younger than virus-negative children (n=246, 26,1%) (p<0,001) and lower ARI was diagnosed more frequently (virus-positive children: n=364, 52% vs. virus-negative children n=86, 35%, p<0,001). Children with viral mono-infection (n=499, 71.7% of 696 virus-positive children, median age: 23 (11-49) months) were older than children with viral co-detection (n=197, 28,3%, median age: 19 (11-31) months, p=0,006; 2 viruses: 23.6%, 3 viruses: 3.1%, >3 viruses 1.7%; p=0,006), but presented with similar clinical severity. The viral distribution among viral monoinfections was as follows: rhinovirus (RhV) (34.9% of 499 mono-infections), respiratory syncytial virus (RSV) (14.6%), influenzavirus (IV) A(H1)/A(H3)/B (10.6%), parainfluenzavirus (PIV) 1-4 (8.4%) and adenovirus (AV) (8.0%), human metapneumovirus (hMPV) (7,4%), human coronavirus (hCoV) NL63/OC43/ HKU1/229E (5%), human bocavirus (hBoV) (4,4%), enterovirus (EV) (3,2%) and parechovirus (PV) (0,4%). Clinical severity was highest in children infected with RSV: bronchitis (59%), oxygen therapy (43%), high viral load (81%)) and hMPV: pneumonia (38%). Viral co-detection was not associated with a significant difference concerning the frequency of a specific clinical diagnosis in children infected with RSV, PIV, hCoV, hBoV or hMPV. However, RhV-co-detection was associated with a higher frequency of bronchitis (n=48, 45% vs. n=56 (32%), p=0,042) and respiratory insufficiency (n=28, 26% vs. n=25, 14%, p=0,018). Among the detected respiratory viral pathogens, RhV was the most frequent, whereas RSV and hMPV were associated with higher disease severity in hospitalised children with ARI. KW - Atemwegsinfektion KW - Kinderkrankheit KW - RS-Virus KW - acute respiratory infection KW - respiratory virus KW - Virale Koinfektion KW - Virale Monoinfektion Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-181605 ER - TY - THES A1 - Horn, Stephan T1 - Resistenzentwicklung von \(Pseudomonas\) \(aeruginosa\) gegen Tobramycin und Colistin bei Patienten mit Mukoviszidose unter Suppressionstherapie T1 - Resistance to tobramycin and colistin in isolates of \(Pseudomonas\) \(aeruginosa\) from chronically colonized patients with cystic fibrosis under antimicrobial treatment N2 - Tobramycin und Colistin sind zwei Standardantibiotika bei der inhalativen Behandlung von Patienten mit zystischer Fibrose (CF), die chronisch mit Pseudomonas aeruginosa besiedelt sind. In dieser Arbeit wurde die Resistenzentwicklung von Pseudomonas aeruginosa gegen Tobramycin und Colistin bei 1844 Isolaten beobachtet. Die Pseudomonas-aeruginosa-Isolate wurden von 22 Patienten mit CF gewonnen, die eine alternierende Inhalationstherapie mit Tobramycin und Colistin erhalten hatten. Eine Tobramycinresistenz wurde bei 30,4% der Isolate und bei 72,7% der Patienten beobachtet. Im Gegensatz hierzu waren alle Isolate sensibel gegenüber Colistin, und es entwickelte auch kein Patient eine Colistin-Resistenz. In molekulargenetischen Analysen ausgewählter Pseudomonas-aeruginosa-Isolate hatte es den Anschein, dass die Patienten im Verlauf der Erkrankung jeweils nur mit einem Genotyp besiedelt waren. Zusammenfassend kann gesagt werden, dass eine Resistenzentwicklung gegen Tobramycin unter Inhalationstherapie stattfindet, während eine Resistenzentwicklung gegen Colistin die Ausnahme zu bleiben scheint. N2 - Tobramycin and colistin represent two standard antimicrobial agents in the treatment of cystic fibrosis (CF) patients who are chronically colonized with Pseudomonas aeruginosa. In this study, we determined the rate of resistance to tobramycin and colistin in 1844 isolates of P. aeruginosa obtained from 22 CF patients under alternate therapy with inhaled tobramycin and colistin. Resistance to tobramycin was observed in 30,4% of isolates and in 72,7% of patients. In contrast, all isolates were susceptible to colistin and no patient developed resistance to colistin. Molecular typing of selected isolates suggested that only one clone occurred over time in each patient. To conclude, resistance to tobramycin in P. aeruginosa isolates from CF patients under antimicrobial therapy may occur while colistin resistance remains uncommon. KW - Pseudomonas aeruginosa KW - tobramycin KW - colistin KW - Resistenz KW - Mukoviszidose KW - Colistin KW - Tobramycin KW - resistance KW - cystic fibrosis Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-174159 ER - TY - JOUR A1 - Hetzer, Benjamin A1 - Orth-Höller, Dorothea A1 - Würzner, Reinhard A1 - Kreidl, Peter A1 - Lackner, Michaela A1 - Müller, Thomas A1 - Knabl, Ludwig A1 - Geisler-Moroder, Daniel Rudolf A1 - Mellmann, Alexander A1 - Sesli, Özcan A1 - Holzknecht, Jeanett A1 - Noce, Damia A1 - Akarathum, Noppadon A1 - Chotinaruemol, Somporn A1 - Prelog, Martina A1 - Oberdorfer, Peninnah T1 - “Enhanced acquisition of antibiotic-resistant intestinal E. coli during the first year of life assessed in a prospective cohort study” JF - Antimicrobial Resistance & Infection Control N2 - Background Increasing bacterial resistance to antibiotics is a serious problem worldwide. We sought to record the acquisition of antibiotic-resistant Escherichia coli (E. coli) in healthy infants in Northern Thailand and investigated potential determinants. Methods Stool samples from 142 infants after birth, at ages 2wk, 2mo, 4 to 6mo, and 1y, and parent stool samples were screened for E. coli resistance to tetracycline, ampicillin, co-trimoxazole, and cefazoline by culture, and isolates were further investigated for multiresistance by disc diffusion method. Pulsed-field gel electrophoresis was performed to identify persistent and transmitted strains. Genetic comparison of resistant and transmitted strains was done by multilocus sequence typing (MLST) and strains were further investigated for extra- and intra-intestinal virulence factors by multiplex PCR. Results Forty-seven (33%) neonatal meconium samples contained resistant E. coli. Prevalence increased continuously: After 1y, resistance proportion (tetracycline 80%, ampicillin 72%, co-trimoxazole 66%, cefazoline 35%) almost matched those in parents. In 8 infants (6%), identical E. coli strains were found in at least 3 sampling time points (suggesting persistence). Transmission of resistant E. coli from parents to child was observed in only 8 families. MLST showed high diversity. We could not identify any virulence genes or factors associated with persistence, or transmission of resistant E. coli. Full-term, vaginal birth and birth in rural hospital were identified as risk factors for early childhood colonization with resistant E. coli. Conclusion One third of healthy Thai neonates harboured antibiotic-resistant E. coli in meconium. The proportion of resistant E. coli increased during the first year of life almost reaching the value in adults. We hypothesize that enhancement of infection control measures and cautious use of antibiotics may help to control further increase of resistance. KW - Escherichia coli KW - antibiotic resistance KW - multiresistance KW - transmission KW - persistence KW - children KW - neonates Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-320284 VL - 8 ER - TY - THES A1 - Hempel, Katharina T1 - Vergleichende Analyse von Antigenexpressionsmustern kindlicher cALL-Blasten und gesunden B-Zellvorstufen – Nutzen für die MRD Diagnostik T1 - Comparative analysis of antigen expression on cALL blasts and healthy B cell progenitors – Use for MRD diagnostics N2 - Die MRD Diagnostik ist von erheblicher Bedeutung für die Risikostratifizierung kindlicher Leukämien. Um aber gesunde, sich regenerierende Vorstufen von blastären Zellen unterscheiden zu können ist die genaue Kenntnis des Antigenverlaufs sowohl der Vorstufen der B-Zellreihe als auch der Blasten notwendig. In dieser Arbeit wird eine Vergleichende Analyse von B-Zellvorstufen und Blasten mittels Durchflusszytometrie durchgeführt. Von besonders diskriminativem Wert waren die Vorläufermarker CD10, CD34, sowie die lymphatischen Marker CD19, CD20, CD22, CD45, cyCD79a und cyTdT. Zur Beschreibung des individuellen LAIP eigneten sich vor allem die Marker CD11b, CD38, CD58, CD123 und CD133, sowie die myeloischen Marker CD13 und CD33. Die Bessere Unterscheidung zwischen gesunden und kranken Zellen zusammen mit neuen Entwicklungen in Diagnostik und Therapie muss in Zukunft zur weiteren Verbesserung der Überlebensraten, auch im Rezidiv führen. N2 - MRD diagnostic is important for the ongoing therapy of cALL in children. For better discrimination between blasts and b-cell progenitors we used flow cytometry to analyse the antigen expression on b cell progenitors with those on cALL blasts. KW - residual KW - minimal KW - disease KW - Durchflusszytometrie KW - Akute Leukämie KW - MRD KW - kindliche Leukämie KW - cALL Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-179203 ER - TY - JOUR A1 - Hagemann, Carsten A1 - Neuhaus, Nikolas A1 - Dahlmann, Mathias A1 - Kessler, Almuth F. A1 - Kobelt, Dennis A1 - Herrmann, Pia A1 - Eyrich, Matthias A1 - Freitag, Benjamin A1 - Linsenmann, Thomas A1 - Monoranu, Camelia M. A1 - Ernestus, Ralf-Ingo A1 - Löhr, Mario A1 - Stein, Ulrike T1 - Circulating MACC1 transcripts in glioblastoma patients predict prognosis and treatment response JF - Cancers N2 - Glioblastoma multiforme is the most aggressive primary brain tumor of adults, but lacksreliable and liquid biomarkers. We evaluated circulating plasma transcripts of metastasis-associatedin colon cancer-1 (MACC1), a prognostic biomarker for solid cancer entities, for prediction of clinicaloutcome and therapy response in glioblastomas. MACC1 transcripts were significantly higher inpatients compared to controls. Low MACC1 levels clustered together with other prognosticallyfavorable markers. It was associated with patients’ prognosis in conjunction with the isocitratedehydrogenase (IDH) mutation status: IDH1 R132H mutation and low MACC1 was most favorable(median overall survival (OS) not yet reached), IDH1 wildtype and high MACC1 was worst (medianOS 8.1 months), while IDH1 wildtype and low MACC1 was intermediate (median OS 9.1 months).No patients displayed IDH1 R132H mutation and high MACC1. Patients with low MACC1 levelsreceiving standard therapy survived longer (median OS 22.6 months) than patients with high MACC1levels (median OS 8.1 months). Patients not receiving the standard regimen showed the worstprognosis, independent of MACC1 levels (low: 6.8 months, high: 4.4 months). Addition of circulatingMACC1 transcript levels to the existing prognostic workup may improve the accuracy of outcomeprediction and help define more precise risk categories of glioblastoma patients. KW - metastasis-associated in colon cancer 1 (MACC1) KW - glioblastoma multiforme KW - liquid biopsy KW - therapy response KW - prognostic marker Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-197327 SN - 2072-6694 VL - 11 IS - 6 ER - TY - JOUR A1 - Haarmann, Axel A1 - Schuhmann, Michael K. A1 - Silwedel, Christine A1 - Monoranu, Camelia-Maria A1 - Stoll, Guido A1 - Buttmann, Mathias T1 - Human brain endothelial CXCR2 is inflammation-inducible and mediates CXCL5- and CXCL8-triggered paraendothelial barrier breakdown JF - International Journal of Molecular Science N2 - Chemokines (C-X-C) motif ligand (CXCL) 5 and 8 are overexpressed in patients with multiple sclerosis, where CXCL5 serum levels were shown to correlate with blood–brain barrier dysfunction as evidenced by gadolinium-enhanced magnetic resonance imaging. Here, we studied the potential role of CXCL5/CXCL8 receptor 2 (CXCR2) as a regulator of paraendothelial brain barrier function, using the well-characterized human cerebral microvascular endothelial cell line hCMEC/D3. Low basal CXCR2 mRNA and protein expression levels in hCMEC/D3 were found to strongly increase under inflammatory conditions. Correspondingly, immunohistochemistry of brain biopsies from two patients with active multiple sclerosis revealed upregulation of endothelial CXCR2 compared to healthy control tissue. Recombinant CXCL5 or CXCL8 rapidly and transiently activated Akt/protein kinase B in hCMEC/D3. This was followed by a redistribution of tight junction-associated protein zonula occludens-1 (ZO-1) and by the formation of actin stress fibers. Functionally, these morphological changes corresponded to a decrease of paracellular barrier function, as measured by a real-time electrical impedance-sensing system. Importantly, preincubation with the selective CXCR2 antagonist SB332235 partially prevented chemokine-induced disturbance of both tight junction morphology and function. We conclude that human brain endothelial CXCR2 may contribute to blood–brain barrier disturbance under inflammatory conditions with increased CXCL5 and CXCL8 expression, where CXCR2 may also represent a novel pharmacological target for blood–brain barrier stabilization. KW - blood–brain barrier KW - multiple sclerosis KW - human cerebral endothelial cells KW - CXCR2 KW - CXCL5 KW - CXCL8 KW - interleukin-8 KW - SB332235 Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-201297 SN - 1422-0067 VL - 20 IS - 3 ER - TY - JOUR A1 - Glaser, Kirsten A1 - Gradzka-Luczewska, Anna A1 - Szymankiewicz-Breborowicz, Marta A1 - Kawczynska-Leda, Natalia A1 - Henrich, Birgit A1 - Waaga-Gasser, Ana Maria A1 - Speer, Christian P. T1 - Perinatal ureaplasma exposure is associated with increased risk of late onset sepsis and imbalanced inflammation in preterm infants and may add to lung injury JF - Frontiers in Cellular and Infection Microbiology N2 - Background: Controversy remains concerning the impact of Ureaplasma on preterm neonatal morbidity. Methods: Prospective single-center study in very low birth weight infants <30 weeks' gestation. Cord blood and initial nasopharyngeal swabs were screened for Ureaplasma parvum and U. urealyticum using culture technique and polymerase chain reaction. Neonatal outcomes were followed until death or discharge. Multi-analyte immunoassay provided cord blood levels of inflammatory markers. Using multivariate regression analyses, perinatal Ureaplasma exposure was evaluated as risk factor for the development of bronchopulmonary dysplasia (BPD), other neonatal morbidities until discharge and systemic inflammation at admission. Results: 40/103 (39%) infants were positive for Ureaplasma in one or both specimens, with U. parvum being the predominant species. While exposure to Ureaplasma alone was not associated with BPD, we found an increased risk of BPD in Ureaplasma-positive infants ventilated ≥5 days (OR 1.64; 95% CI 0.12–22.98; p = 0.009). Presence of Ureaplasma was associated with a 7-fold risk of late onset sepsis (LOS) (95% CI 1.80–27.39; p = 0.014). Moreover, Ureaplasma-positive infants had higher I/T ratios (b 0.39; 95% CI 0.08–0.71; p = 0.014), increased levels of interleukin (IL)-17 (b 0.16; 95% CI 0.02–0.30; p = 0.025) and matrix metalloproteinase 8 (b 0.77; 95% CI 0.10–1.44; p = 0.020), decreased levels of IL-10 (b −0.77; 95% CI −1.58 to −0.01; p = 0.043) and increased ratios of Tumor necrosis factor-α, IL-8, and IL-17 to anti-inflammatory IL-10 (p = 0.003, p = 0.012, p < 0.001). Conclusions: Positive Ureaplasma screening was not associated with BPD. However, exposure contributed to BPD in infants ventilated ≥5 days and conferred an increased risk of LOS and imbalanced inflammatory cytokine responses. KW - Ureaplasma parvum KW - Ureaplasma urealyticum KW - preterm infants KW - VLBW KW - bronchopulmonary dysplasia KW - late onset sepsis KW - neonatal outcome KW - inflammation Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-201270 VL - 9 IS - 68 ER - TY - THES A1 - Gierlich, Philipp T1 - 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 T1 - 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 N2 - 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. N2 - 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. KW - Reifung KW - Dendritische Zelle KW - Toll-like-Rezeptoren KW - Tumor KW - Impfstoff KW - Glioblastom KW - Poly(I:C) KW - TLR3 KW - R848 KW - TLR8 KW - Kostimulation KW - Zytokine KW - Migration KW - Homing KW - Priming Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-188756 ER - TY - THES A1 - Demerath, Antonia T1 - Evaluation der Wertigkeit des Schweißtestes nach Gibson und Cooke zur Diagnose einer Mukoviszidose bei Patienten mit Trisomie 21 T1 - Evaluation valency of sweat testing after Gibson and Cooke for diagnosis of cystic fibrosis in patients with down syndrome N2 - Menschen mit Trisomie 21 weisen häufig eine Gedeihstörung und eine erhöhte Infektanfälligkeit auf, weswegen im klinischen Alltag nicht selten ein Schweißtest zum Ausschluss einer Mukoviszidose (CF) durchgeführt werden muss. In der Literatur gibt es Hinweise, dass bei Patienten mit Trisomie 21 eine erhöhte Schweißosmolalität vorliegt, was zu falsch positiven Schweißtestuntersuchungen führen könnte. Bisher gab es keine Studie darüber, ob die Chlorid(Cl)-Messung im Schweiß bei Patienten mit Trisomie 21 zum Ausschluss einer CF herangezogen werden kann. Diese Studie stellt nun die Schweißsekretionsrate, sowie die Chlorid-Konzentration in Schweißproben von Probanden mit Trisomie 21 der von Kontrollpersonen gegenüber. N2 - Recurrent airway infections are common in patients with Down’s syndrome (DS). Hence, ruling out Cystic Fibrosis (CF) in these patients is often required. In the past, the value of sweat testing–the gold standard to diagnose CF–has been questioned in DS as false positive results have been reported. However, these reports are based on measurements of sweat osmolality or sodium concentrations, not chloride concentrations. This study analyses sweat secretion rate and chloride concentration in sweat samples of patients with DS in comparison to healthy controls KW - Down-Syndrom KW - Mukoviszidose KW - Schweißosmolalität KW - Trisomie 21 KW - Mukoviszidose KW - Schweißsekretionsrate KW - Thermoregulation KW - gender gap KW - non-responder KW - sweat osmolality KW - sweat secretion rate KW - thermoregulation Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-188988 ER - TY - THES A1 - Böhm, Marie-Luise T1 - Erregerspektrum und Resistenzlage bakterieller Sepsis im Kindes- und Jugendalter – statistische Auswertung von Blutkultur-positiven Sepsisfällen im Department für Pädiatrie der Medizinischen Universität Innsbruck in den Jahren 2000 bis 2008 – T1 - Pathogen spectrum and resistance situation of bacterial sepsis in children and adolescents – statistical evaluation of blood culture-positive sepsis in the Department of Pediatrics of the Medical University Innsbruck from 2000 to 2008 – N2 - Diese Arbeit ist eine epidemiologische, deskriptive Beobachtungsstudie mit retrospektiver Datenerhebung. Sie stellt das bakterielle Erreger- und Resistenzspektrum von pädiatrischen Patienten mit Blutkultur-positiver Sepsis in Innsbruck dar. Dazu wurden 797 positive Blutkulturen von pädiatrischen Patienten des Departments für Pädiatrie der Medizinischen Universität Innsbruck, bei denen gemäß Patientenakte eine Sepsis diagnostiziert wurde, im Zeitraum von Januar 2000 bis Dezember 2008 an der Sektion für Hygiene und Medizinische Mikrobiologie der Medizinischen Universität Innsbruck bezüglich der Erregerverteilung und des Resistenzspektrums untersucht. In einem weiteren Schritt wurde im Rahmen einer statistischen Auswertung überprüft, inwieweit patientenbezogene Daten (Geschlecht, Alter, Begleiterkrankung) sowie der Infektionsort (nosokomial oder ambulant erworben), die Entnahmestelle der Blutkultur und der Zeitraum das Erreger- und Resistenzspektrum beeinflussen. N2 - This is an epidemiological, descriptive, observational study with retrospective data collection. It shows the bacterial pathogen spectrum and the resistance situation of pediatric patients with blood culture-positive sepsis in Innsbruck. Therefore, 797 positive blood cultures of pediatric patients from the Department of Pediatrics of the Medical University Innsbruck, who were suffering from sepsis according to patient file, were analyzed from January 2000 to December 2008 at the Division of Hygiene and Medical Microbiology of the Medical University Innsbruck regarding the pathogen spectrum and the resistance situation. Furthermore a statistical evaluation was conducted, to examine to what extent patient-related data (gender, age, accompanying illness), site of infection (nosocomial or community acquired), sampling point of the blood culture and time period affect the pathogen spectrum and resistance situation. KW - Sepsis KW - Kinderheilkunde KW - Antibiotikum KW - Antibiotikaresistenz KW - Erregerspektrum Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-179774 ER - TY - JOUR A1 - Bonig, Halvard A1 - Kuçi, Zyrafete A1 - Kuçi, Selim A1 - Bakhtiar, Shahrzad A1 - Basu, Oliver A1 - Bug, Gesine A1 - Dennis, Mike A1 - Greil, Johann A1 - Barta, Aniko A1 - Kállay, Krisztián M. A1 - Lang, Peter A1 - Lucchini, Giovanna A1 - Pol, Raj A1 - Schulz, Ansgar A1 - Sykora, Karl-Walter A1 - Teichert von Luettichau, Irene A1 - Herter-Sprie, Grit A1 - Ashab Uddin, Mohammad A1 - Jenkin, Phil A1 - Alsultan, Abdulrahman A1 - Buechner, Jochen A1 - Stein, Jerry A1 - Kelemen, Agnes A1 - Jarisch, Andrea A1 - Soerensen, Jan A1 - Salzmann-Manrique, Emilia A1 - Hutter, Martin A1 - Schäfer, Richard A1 - Seifried, Erhard A1 - Paneesha, Shankara A1 - Novitzky-Basso, Igor A1 - Gefen, Aharon A1 - Nevo, Neta A1 - Beutel, Gernot A1 - Schlegel, Paul-Gerhardt A1 - Klingebiel, Thomas A1 - Bader, Peter T1 - Children and adults with Refractory acute Graft-versus-Host Disease respond to treatment with the Mesenchymal Stromal cell preparation “MSC-FFM”—Outcome report of 92 patients JF - Cells N2 - (1) Background: Refractory acute graft-versus-host disease (R-aGvHD) remains a leading cause of death after allogeneic stem cell transplantation. Survival rates of 15% after four years are currently achieved; deaths are only in part due to aGvHD itself, but mostly due to adverse effects of R-aGvHD treatment with immunosuppressive agents as these predispose patients to opportunistic infections and loss of graft-versus-leukemia surveillance resulting in relapse. Mesenchymal stromal cells (MSC) from different tissues and those generated by various protocols have been proposed as a remedy for R-aGvHD but the enthusiasm raised by initial reports has not been ubiquitously reproduced. (2) Methods: We previously reported on a unique MSC product, which was generated from pooled bone marrow mononuclear cells of multiple third-party donors. The products showed dose-to-dose equipotency and greater immunosuppressive capacity than individually expanded MSCs from the same donors. This product, MSC-FFM, has entered clinical routine in Germany where it is licensed with a national hospital exemption authorization. We previously reported satisfying initial clinical outcomes, which we are now updating. The data were collected in our post-approval pharmacovigilance program, i.e., this is not a clinical study and the data is high-level and non-monitored. (3) Results: Follow-up for 92 recipients of MSC-FFM was reported, 88 with GvHD ≥°III, one-third only steroid-refractory and two-thirds therapy resistant (refractory to steroids plus ≥2 additional lines of treatment). A median of three doses of MSC-FFM was administered without apparent toxicity. Overall response rates were 82% and 81% at the first and last evaluation, respectively. At six months, the estimated overall survival was 64%, while the cumulative incidence of death from underlying disease was 3%. (4) Conclusions: MSC-FFM promises to be a safe and efficient treatment for severe R-aGvHD. KW - graft-versus host KW - transplantation KW - mesenchymal stromal cell KW - cell therapy KW - hospital exemption KW - steroid-resistant aGvHD KW - refractory aGvHD Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-193878 SN - 2073-4409 VL - 8 IS - 12 ER -