TY - THES A1 - Aehnlich, Flora T1 - Untersuchungen zur Präsentation kryptischer und kanonischer Peptide über den MHC-Klasse-I-Komplex in Patienten mit akuter myeloischer Leukämie T1 - Investigation about the presentation of cryptic and canonical peptides on the MHC-class-I-complex in patients with acute myeloid leukemia N2 - Die AML stellt mit einem Anteil von 80 % an den akuten Leukämien bei Erwachsenen eine bedeutende Erkrankung für die Gesellschaft dar. Aufgrund fehlender durchbrechender Erfolge in der Therapieentwicklung liegt die durchschnittliche Fünfjahresüberlebensrate dennoch nur bei etwa 25 %. Der Blick auf die Kraft des Graft-versus-Leukämie-Effekts nach allogener Stammzelltransplantation, eine Langzeitremission der AML erzielen zu können, weist jedoch auf die Immunogenität und Eignung der Erkrankung für neue immuntherapeutische Ansätze hin. Anhand der Kartierung der in-vivo präsentierten MHC-Klasse-I-Peptidome auf AML-Blasten sollten in dieser Arbeit potenziell geeignete Therapietargets identifiziert werden, um eine breitere Anwendung immuntherapeutischer Strategien bei AML-Patienten zu ermöglichen. Auf primären Patientenmaterialien, Zelllinien und benignen Zellen wurden hierzu über eine Immunoaffinitätschromatographie mit nachfolgenden Purifizierungsschritten die MHC-präsentierten Peptide massenspekrometrisch-basiert identifiziert. Zusätzlich erfolgte eine Quantifizierung der Oberflächen- und intrazellulären MHC-Klasse-I-Moleküle der verwendeten Proben durch einen indirekten Immunfluoreszenz-Assay. Unter der Gesamtheit von 17.750 identifizierten nicht-redundanten MHC-Klasse- I-präsentierten Peptiden konnte eine Vielzahl von 5.626 Peptiden mit Präsentationsfrequenzen bis zu 72 % als AML-exklusiv beschrieben werden. Hierunter wurden 240 kryptische Peptide vermeintlich nicht-codierenden Ursprungs identifiziert. Zudem wurden mehrere potenziell CMV-kreuzreaktive AML-Peptide erfasst, die zu der reduzierten Rezidivrate bei CMV-Infektion nach allogener Stammzelltransplantation führen könnten. Bei der MHC-Quantifizierung wiesen die AML-Blasten keine verminderte MHC-Expression auf und stellten sich somit als geeignete Target-Zellen für eine T-Zell-Immuntherapie dar. N2 - AML is a disease with huge society impacts since it represents 80 % of all acute leukemia in adults. However, due to the lack of breakthroughs in the development of new therapies, the average five-year survival rate is only around 25%. The Graft-versus-Leukemia-Effect after allogeneic stem cell transplantation, which can achieve long-term remission in AML-patients, provides evidence for the immunogenicity and therefore suitability of the disease for new immunotherapeutic approaches. The aim of this these is to enable a broader application of immunotherapeutic strategies in AML patients by mapping the in-vivo presented peptidomes of the MHC-class-I-pathway. For this purpose, primary patient materials, cell lines and benign cells were analyzed using immunoaffinity chromatography with several subsequential purification steps and mass-spectrometric-based identification. In addition, the surface and intracellular MHC-class-I-molecules of the samples used were quantified by an indirect immunofluorescence assay. Among the total of 17,750 identified non-redundant MHC-class-I-presented peptides, a large number of 5,626 peptides with presentation frequencies of up to 72% could be described as AML-exclusive. Among them, 240 cryptic peptides of supposedly non-coding origin were identified. In addition, several potentially CMV-cross-reactive AML-peptides were identified. Such a cross reactivity could explain the reduced recurrence rate through CMV infection after allogeneic stem cell transplantation. The MHC-class-I-quantification of the AML-blasts did not show any reduced MHC-expression and would therefore be suitable target cells for T-cell-immunotherapy. KW - Akute myeloische Leukämie KW - Immuntherapie KW - MHC KW - Cytomegalie-Virus KW - Kreuzreaktion KW - Kartierung KW - MHC-Klasse-I-Peptidom Y1 - 2022 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-270036 ER - TY - JOUR A1 - Aghai, Fatemeh A1 - Zimmermann, Sebastian A1 - Kurlbaum, Max A1 - Jung, Pius A1 - Pelzer, Theo A1 - Klinker, Hartwig A1 - Isberner, Nora A1 - Scherf-Clavel, Oliver T1 - Development and validation of a sensitive liquid chromatography tandem mass spectrometry assay for the simultaneous determination of ten kinase inhibitors in human serum and plasma JF - Analytical and Bioanalytical Chemistry N2 - A liquid chromatography tandem mass spectrometry method for the analysis of ten kinase inhibitors (afatinib, axitinib, bosutinib,cabozantinib, dabrafenib, lenvatinib, nilotinib, osimertinib, ruxolitinib, and trametinib) in human serum and plasma for theapplication in daily clinical routine has been developed and validated according to the US Food and Drug Administration andEuropean Medicines Agency validation guidelines for bioanalytical methods. After protein precipitation of plasma samples withacetonitrile, chromatographic separation was performed at ambient temperature using a Waters XBridge® Phenyl 3.5μm(2.1×50 mm) column. The mobile phases consisted of water-methanol (9:1, v/v) with 10 mM ammonium bicarbonate as phase A andmethanol-water (9:1, v/v) with 10 mM ammonium bicarbonate as phase B. Gradient elution was applied at a flow rate of 400μL/min. Analytes were detected and quantified using multiple reaction monitoring in electrospray ionization positive mode. Stableisotopically labeled compounds of each kinase inhibitor were used as internal standards. The acquisition time was 7.0 min perrun. All analytes and internal standards eluted within 3.0 min. The calibration curves were linear over the range of 2–500 ng/mLfor afatinib, axitinib, bosutinib, lenvatinib, ruxolitinib, and trametinib, and 6–1500 ng/mL for cabozantinib, dabrafenib, nilotinib,and osimertinib (coefficients of correlation≥0.99). Validation assays for accuracy and precision, matrix effect, recovery,carryover, and stability were appropriate according to regulatory agencies. The rapid and sensitive assay ensures high throughputand was successfully applied to monitor concentrations of kinase inhibitors in patients. KW - kinase inhibitors KW - therapeutic drug monitoring KW - liquid chromatography tandem mass spectrometry (LC-MS/MS KW - afatinib KW - osimertinib Y1 - 2021 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-231925 SN - 1618-2642 VL - 413 ER - TY - THES A1 - Aichholzer, Mareike T1 - Veränderungen im intestinalen Mikrobiom bei Patienten mit akuter Leukämie im longitudinalen Verlauf T1 - Comprehensive monitoring of gut microbiota during therapy for acute leukemia N2 - In der vorliegenden Studie wurden Veränderungen des Darmmikrobioms anhand von Stuhlproben von Patienten mit akuter Leukämie longitudinal untersucht. Die Patienten wurden mit intensiver Chemotherapie behandelt. Die Therapie als auch die Erkrankung selbst führte zu einer erheblichen Immunsuppression der Patienten. Prophylaktisch und therapeutisch wurden intensive Antibiotikatherapien bei allen Patienten durchgeführt. Das Mikrobiom wurde quantitativ und qualitativ analysiert. Die Bakterienmenge der Stuhlproben wurde mittels quantitativer Polymerase-Kettenreaktion und die Diversität des Mikrobioms mittels 16s rDNA Sequenzierung aufgezeigt. Zusätzlich dazu fand eine mikrobiologische Kultivierung von Bakterien in Rektalabstrichen statt, um multiresistente Keime nachzuweisen. Ebenso wurde der klinische Verlauf der Patienten dokumentiert. Insgesamt wurde das Mikrobiom von drei verschiedenen Studiengruppen untersucht: Patienten mit akuter Leukämie, Patienten, die mit multiresistenten Keimen besiedelt waren und sich in der Nachsorge der Würzburger interdisziplinären onkologischen Tagesklinik befanden sowie gesunde Probanden. Im Mikrobiom der Patienten mit akuter Leukämie war eine deutlich geringere Diversität sowie eine deutlich geringere Bakterienmenge im Vergleich zu beiden anderen Studiengruppen festzustellen. Das Mikrobiom änderte sich während des Therapieverlaufs erheblich und am Beispiel von einigen Patienten konnte gezeigt werden, dass einzelne Bakterien das Mikrobiom dominierten. Des Weiteren waren im Mikrobiom der Patienten mit akuter Leukämie mehr potenziell pathogene sowie weniger potenziell protektive Bakterien im Vergleich zur Kontrollgruppe vorhanden. Zusammenfassend lässt sich sagen, dass sich das Mikrobiom der Patienten mit akuter Leukämie deutlich von dem der anderen Studiengruppen unterscheidet. Um die Daten zu validieren und einen eventuellen Einfluss des Mikrobioms auf das Überleben der Patienten zu identifizieren, sollten die Untersuchungen an einer deutlich größeren Studienpopulation wiederholt werden. N2 - In the present study changes in the intestinal microbiome were examined longitudinally using stool samples from patients with acute leukemia. The patients were treated with intensive chemotherapy. The therapy as well as the disease itself led to a considerable immunosuppression of the patients. Prophylactic and therapeutic intensive antibiotic therapies were performed in all patients. The microbiome was analyzed quantitatively and qualitatively. The amount of bacteria in the stool samples was determined by a quantitative polymerase chain reaction and the diversity of the microbiome by 16s rDNA sequencing. In addition, a microbiological cultivation of bacteria in analswabs was performed to detect multiresistant bacteria. The clinical course of the patients was also documented. In total the microbiome was examined by three different study groups: patients with acute leukaemia, patients colonised with multi-resistant germs and undergoing follow-up treatment at the Würzburg interdisciplinary oncological day clinic, and healthy volunteers. In the microbiome of the patients with acute leukaemia, a significantly lower diversity as well as a significantly lower amount of bacteria was found in comparison to the two other study groups. The microbiome changed considerably during the course of therapy and it could be shown in the cases of some patients that individual bacteria dominated the microbiome. In addition, the microbiome of patients with acute leukaemia contained more potentially pathogenic and less potentially protective bacteria compared to the control group. In summary, the microbiome of patients with acute leukaemia differed significantly from that of the other study groups. In order to validate the data and identify a possible influence of the microbiome on the survival rates of the patients, the investigations should be repeated in a significantly larger study population. KW - Akute Leukämie KW - Mikrobiom KW - acute leukemia KW - microbiota Y1 - 2020 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-199213 ER - TY - JOUR A1 - Almanzar, Giovanni A1 - Klein, Matthias A1 - Schmalzing, Marc A1 - Hilligardt, Deborah A1 - El Hajj, Nady A1 - Kneitz, Hermann A1 - Wild, Vanessa A1 - Rosenwald, Andreas A1 - Benoit, Sandrine A1 - Hamm, Henning A1 - Tony, Hans-Peter A1 - Haaf, Thomas A1 - Goebeler, Matthias A1 - Prelog, Martina T1 - Disease Manifestation and Inflammatory Activity as Modulators of Th17/Treg Balance and RORC/FoxP3 Methylation in Systemic Sclerosis JF - International Archives of Allergy and Immunology N2 - Background: There is much evidence that T cells are strongly involved in the pathogenesis of localized and systemic forms of scleroderma (SSc). A dysbalance between FoxP3+ regulatory CD4+ T cells (Tregs) and inflammatory T-helper (Th) 17 cells has been suggested. Methods: The study aimed (1) to investigate the phenotypical and functional characteristics of Th17 and Tregs in SSc patients depending on disease manifestation (limited vs. diffuse cutaneous SSc, dcSSc) and activity, and (2) the transcriptional level and methylation status of Th17- and Treg-specific transcription factors. Results: There was a concurrent accumulation of circulating peripheral IL-17-producing CCR6+ Th cells and FoxP3+ Tregs in patients with dcSSc. At the transcriptional level, Th17- and Treg-associated transcription factors were elevated in SSc. A strong association with high circulating Th17 and Tregs was seen with early, active, and severe disease presentation. However, a diminished suppressive function on autologous lymphocytes was found in SSc-derived Tregs. Significant relative hypermethylation was seen at the gene level for RORC1 and RORC2 in SSc, particularly in patients with high inflammatory activity. Conclusions: Besides the high transcriptional activity of T cells, attributed to Treg or Th17 phenotype, in active SSc disease, Tregs may be insufficient to produce high amounts of IL-10 or to control proliferative activity of effector T cells in SSc. Our results suggest a high plasticity of Tregs strongly associated with the Th17 phenotype. Future directions may focus on enhancing Treg functions and stabilization of the Treg phenotype. KW - methylation KW - systemic sclerosis KW - suppression KW - Tregs KW - Th17 Y1 - 2016 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-196577 SN - 1018-2438 SN - 1423-0097 N1 - This publication is with permission of the rights owner freely accessible due to an Alliance licence and a national licence (funded by the DFG, German Research Foundation) respectively. VL - 171 IS - 2 ER - TY - JOUR A1 - Anany, Mohamed A. A1 - Kreckel, Jennifer A1 - Füllsack, Simone A1 - Rosenthal, Alevtina A1 - Otto, Christoph A1 - Siegmund, Daniela A1 - Wajant, Harald T1 - Soluble TNF-like weak inducer of apoptosis (TWEAK) enhances poly(I:C)-induced RIPK1-mediated necroptosis JF - Cell Death & Disease N2 - TNF-like weak inducer of apoptosis (TWEAK) and inhibition of protein synthesis with cycloheximide (CHX) sensitize for poly(I:C)-induced cell death. Notably, although CHX preferentially enhanced poly(I:C)-induced apoptosis, TWEAK enhanced primarily poly(I:C)-induced necroptosis. Both sensitizers of poly(I:C)-induced cell death, however, showed no major effect on proinflammatory poly(I:C) signaling. Analysis of a panel of HeLa-RIPK3 variants lacking TRADD, RIPK1, FADD, or caspase-8 expression revealed furthermore similarities and differences in the way how poly(I:C)/TWEAK, TNF, and TRAIL utilize these molecules for signaling. RIPK1 turned out to be essential for poly(I:C)/TWEAK-induced caspase-8-mediated apoptosis but was dispensable for this response in TNF and TRAIL signaling. TRADD-RIPK1-double deficiency differentially affected poly(I:C)-triggered gene induction but abrogated gene induction by TNF completely. FADD deficiency abrogated TRAIL- but not TNF- and poly(I:C)-induced necroptosis, whereas TRADD elicited protective activity against all three death inducers. A general protective activity against poly(I:C)-, TRAIL-, and TNF-induced cell death was also observed in FLIPL and FLIPS transfectrants. Y1 - 2018 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-221104 VL - 9 ER - TY - JOUR A1 - Andersen, Jens Peter A1 - Bøgsted, Martin A1 - Dybkær, Karen A1 - Mellqvist, Ulf-Henrik A1 - Morgan, Gareth J. A1 - Goldschmidt, Hartmut A1 - Dimopoulos, Meletios A. A1 - Einsele, Hermann A1 - San Miguel, Jesús A1 - Palumbo, Antonio A1 - Sonneveld, Pieter A1 - Johnsen, Hans Erik T1 - Global myeloma research clusters, output, and citations: a bibliometric mapping and clustering analysis JF - PLoS ONE N2 - Background International collaborative research is a mechanism for improving the development of disease-specific therapies and for improving health at the population level. However, limited data are available to assess the trends in research output related to orphan diseases. Methods and Findings We used bibliometric mapping and clustering methods to illustrate the level of fragmentation in myeloma research and the development of collaborative efforts. Publication data from Thomson Reuters Web of Science were retrieved for 2005-2009 and followed until 2013. We created a database of multiple myeloma publications, and we analysed impact and co-authorship density to identify scientific collaborations, developments, and international key players over time. The global annual publication volume for studies on multiple myeloma increased from 1,144 in 2005 to 1,628 in 2009, which represents a 43% increase. This increase is high compared to the 24% and 14% increases observed for lymphoma and leukaemia. The major proportion (> 90% of publications) was from the US and EU over the study period. The output and impact in terms of citations, identified several successful groups with a large number of intra-cluster collaborations in the US and EU. The US-based myeloma clusters clearly stand out as the most productive and highly cited, and the European Myeloma Network members exhibited a doubling of collaborative publications from 2005 to 2009, still increasing up to 2013. Conclusion and Perspective Multiple myeloma research output has increased substantially in the past decade. The fragmented European myeloma research activities based on national or regional groups are progressing, but they require a broad range of targeted research investments to improve multiple myeloma health care. KW - multiparametric flow cytometry KW - multiple myeloma KW - consensus statement KW - European experts KW - disorders KW - therapy KW - network Y1 - 2015 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-144214 VL - 10 IS - 1 ER - TY - JOUR A1 - Anger, Friedrich A1 - Döring, Anna A1 - van Dam, Jacob A1 - Lock, Johann Frisco A1 - Klein, Ingo A1 - Bittrich, Max A1 - Germer, Christoph-Thomas A1 - Wiegering, Armin A1 - Kunzmann, Volker A1 - van Eijck, Casper A1 - Löb, Stefan T1 - Impact of Borderline Resectability in Pancreatic Head Cancer on Patient Survival: Biology Matters According to the New International Consensus Criteria JF - Annals of Surgical Oncology N2 - Background International consensus criteria (ICC) have redefined borderline resectability for pancreatic ductal adenocarcinoma (PDAC) according to three dimensions: anatomical (BR-A), biological (BR-B), and conditional (BR-C). The present definition acknowledges that resectability is not just about the anatomic relationship between the tumour and vessels but that biological and conditional dimensions also are important. Methods Patients’ tumours were retrospectively defined borderline resectable according to ICC. The study cohort was grouped into either BR-A or BR-B and compared with patients considered primarily resectable (R). Differences in postoperative complications, pathological reports, overall (OS), and disease-free survival were assessed. Results A total of 345 patients underwent resection for PDAC. By applying ICC in routine preoperative assessment, 30 patients were classified as stage BR-A and 62 patients as stage BR-B. In total, 253 patients were considered R. The cohort did not contain BR-C patients. No differences in postoperative complications were detected. Median OS was significantly shorter in BR-A (15 months) and BR-B (12 months) compared with R (20 months) patients (BR-A vs. R: p = 0.09 and BR-B vs. R: p < 0.001). CA19-9, as the determining factor of BR-B patients, turned out to be an independent prognostic risk factor for OS. Conclusions Preoperative staging defining surgical resectability in PDAC according to ICC is crucial for patient survival. Patients with PDAC BR-B should be considered for multimodal neoadjuvant therapy even if considered anatomically resectable. KW - pancreatic head cancer Y1 - 2021 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-235251 SN - 1068-9265 VL - 28 IS - 4 ER - TY - JOUR A1 - Anger, Friedrich A1 - Lock, Johan Friso A1 - Klein, Ingo A1 - Hartlapp, Ingo A1 - Wiegering, Armin A1 - Germer, Christoph-Thomas A1 - Kunzmann, Volker A1 - Löb, Stefan T1 - Does concurrent cholestasis alter the prognostic value of preoperatively elevated CA19-9 serum levels in patients with pancreatic head adenocarcinoma? JF - Annals of Surgical Oncology N2 - Background Pancreatic adenocarcinoma (PDAC) patients with preoperative carbohydrate antigen 19-9 (CA19-9) serum levels higher than 500 U/ml are classified as biologically borderline resectable (BR-B). To date, the impact of cholestasis on preoperative CA19-9 serum levels in these patients has remained unquantified. Methods Data on 3079 oncologic pancreatic resections due to PDAC that were prospectively acquired by the German Study, Documentation and Quality (StuDoQ) registry were analyzed in relation to preoperative CA19-9 and bilirubin serum values. Preoperative CA19-9 values were adjusted according to the results of a multivariable linear regression analysis of pathologic parameters, bilirubin, and CA19-9 values. Results Of 1703 PDAC patients with tumor located in the pancreatic head, 420 (24.5 %) presented with a preoperative CA19-9 level higher than 500 U/ml. Although receiver operating characteristics (ROC) analysis failed to determine exact CA19-9 cut-off values for prognostic indicators (R and N status), the T, N, and G status; the UICC stage; and the number of simultaneous vein resections increased with the level of preoperative CA19-9, independently of concurrent cholestasis. After adjustment of preoperative CA19-9 values, 18.5 % of patients initially staged as BR-B showed CA19-9 values below 500 U/ml. However, the postoperative pathologic results for these patients did not change compared with the patients who had CA19-9 levels higher than 500 U/ml after bilirubin adjustment. Conclusions In this multicenter dataset of PDAC patients, elevation of preoperative CA19-9 correlated with well-defined prognostic pathologic parameters. Bilirubin adjustment of CA19-9 is feasible but does not affect the prognostic value of CA19-9 in jaundiced patients. KW - pancreatic adenocarcinoma (PDAC) KW - CA19-9 KW - cholestasis Y1 - 2022 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-323854 VL - 29 IS - 13 ER - TY - THES A1 - Attinger, Hannah Marie T1 - Bedeutung der nukleären Lokalisationssequenz (NLS) des Proteins p8 für die Kerntranslokation und seine Proliferation induzierende Wirkung T1 - The role of the nuclear localisation sequence (NLS) of the protein p8 concerning nuclear translocation and its proliferation inducing effect N2 - p8 ist ein erstmals im Zusammenhang mit akuter Pankreatitis beschriebenes Protein, das im exokrinen und endokrinen Pankreas mit vermehrtem Zellwachstum assoziiert ist. Bei der Analyse seiner Primärstruktur wurde ein speziesübergreifend hoch konservierter Abschnitt, eine sogenannte NLS, ausgemacht, der HMG-Y/I-Proteinen ähnelt. Da HMG-Proteine oft als Transkriptionsfaktoren wirken, wurde die Hypothese formuliert, auch p8 sei ein HMG-Y/I-Protein und wirke als Transkriptionsfaktor im Nukleus. Um die Bedeutung der rp8-NLS näher zu charakterisieren, wurde in INS-1 beta-Zellen ein rp8(NLS-)-EGFP Fusionsprotein ektopisch exprimiert, um dessen subzelluläre Lokalisation zu untersuchen. Es zeigte sich, ähnlich wie bei Kontrollzellen mit ektoper Expression von EGFP allein, eine gleichmäßige Verteilung von rp8(NLS-)-EGFP zwischen Zytoplasma und Nukleus. Da rp8(NLS-) trotz fehlender NLS dennoch in den Kern translozieren kann, scheint die NLS für diesen Vorgang nicht essentiell zu sein. Diese Annahme wird gestützt durch die Beobachtung, dass einzeln exprimiertes rp8(NLS-) seine Proliferation induzierende Wirkung nicht verliert. In Zellzählungsexperimenten zeigte sich, dass ein rp8- bzw. p8(NLS-)-EGFP Fusionsprotein keinen proliferationsfördernden Einfluss in INS-1 und hMSC-TERT Zellen hat. Bei ektoper Expression von rp8 bzw. rp8(NLS-) und hrGFP als Einzelproteine konnte jedoch eine zwischen beiden rp8-Varianten ähnliche und insgesamt signifikante Stimulation der Zellvermehrung beobachtet werden. Dies belegt, dass die Fusion von rp8 an EGFP dessen biologische Funktion inhibiert, während die Deletion der NLS keinen Einfluß darauf hat. Da der proliferative Stimulus von p8 in menschlichen hMSC-TERT Zellen unabhängig von der Herkunft von p8 aus Ratte oder Mensch ist, scheint p8 bei Säugern hoch konserviert zu sein und speziesübergreifend zu wirken. Aus der hier vorgestellten Arbeit geht hervor, dass der molekulare Mechanismus, über den p8 glukoseabhängig proliferationsinduzierend in INS-1 beta-Zellen wirkt, nicht über die NLS vermittelt wird. Weitere Untersuchungen der Wirkungsweise von p8 auf molekularer Ebene könnten in Zukunft einen Ansatz zur in vitro-Generierung ausreichender Mengen an beta-Zellen zur Zelltherapie des Diabetes mellitus bilden. N2 - The protein p8 was first described as a proliferative factor in the exocrine and endocrine pancreas during an acute pancreatitis. An analysis of the amino acid sequence showed a highly conserved area with strong similarities to a nuclear localisation sequence (NLS) of HMG-Y/I proteins. These proteins act very often as transcription factors and therefore it was hypothesized that p8 also acts as transcription factor. In order to explore the functionality of the rat p8 NLS sequence, an rp8(NLS-)-EGFP fusion protein was transfected into INS1 beta cells and the sub cellular localisation of the protein analyzed. This experiment showed an equal distribution of the fusion protein between nucleus and cytoplasm as it was also observed for control cells which were only transfected with EGFP. It seems that the NLS sequence is not essential for the translocation of rp8 to the nucleus. This is also supported by the observation that rp8(NLS-) still has its proliferative function. Cell counting experiments showed that rp8 and rp8(NLS-)-EGFP fusion proteins had no proliferative effect in INS-1 or hMSC-TERT cells whereas the expression of rp8 and rp8(NLS-) as single proteins caused a significant proliferation augmentation. This led to the conclusion that the fusion protein of p8 and EGFP has lost its biological function whereas the NLS is not essential for the function of p8 as a single protein. The independence of the proliferative effect in hMSC-TERT cells from rat or human p8 may indicate a highly conserved role for p8 in mammals. This work showed that the proliferative effect of p8 in glucose stimulated INS-1 beta cells is independent of its supposed nuclear localisation sequence. The molecular mechanisms of p8 function has still to be revealed by further experiments but once elucidated it may lead to in-vitro generation of beta cells for a cell therapy of diabetes mellitus. KW - Diabetes mellitus KW - Proliferation KW - Transkriptionsfaktor KW - Kernproteine KW - Protein p8 KW - subzelluläre Lokalisation KW - nukleäre Lokalisationssequenz KW - beta-Zellproliferation KW - protein p8 KW - subcellular localisation KW - nuclear localisation sequence KW - proliferation of beta-cells Y1 - 2010 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-47534 ER - TY - THES A1 - Austein, Kristof T1 - Entwicklung und Charakterisierung von 4-1BB-spezifischen Agonisten T1 - Development and characterization of 4-1BB specific agonists N2 - Um eine Signaltransduktion mittels agnostischer Antikörper an Rezeptoren der TNFRSF zu bewirken, ist eine vorherige Immobilisation über des Fc Anteil des Antikörpers Grundvorraussetzung. In dieser Arbeit sollte die Möglichkeit der Verankerung über eine andere Bindungsdomäne untersucht werden. Es konnte gezeigt werden, dass eine Immobilisation mittels scFv:CD70 zu einer starken Signalaktivierung führt. N2 - In order to effect signal transduction by means of agnostic antibodies at receptors of TNFRSF, prior immobilization via the Fc part of the antibody is a basic requirement. In this thesis the possibility of anchoring via a different binding domain should be investigated. It could be shown that immobilization by means of scFv: CD70 leads to strong signal activation. KW - Monoklonaler Antikörper KW - Monoklonaler bispezifischer Antikörper KW - Antikörper-Fusionsproteine KW - TNRSF KW - antibody KW - 4-1BB Agonist Y1 - 2021 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-234285 ER - TY - JOUR A1 - Bachmann, Friederike A1 - Schreder, Martin A1 - Engelhardt, Monika A1 - Langer, Christian A1 - Wolleschak, Denise A1 - Mügge, Lars Olof A1 - Dürk, Heinz A1 - Schäfer-Eckart, Kerstin A1 - Blau, Igor Wolfgang A1 - Gramatzki, Martin A1 - Liebisch, Peter A1 - Grube, Matthias A1 - Metzler, Ivana v. A1 - Bassermann, Florian A1 - Metzner, Bernd A1 - Röllig, Christoph A1 - Hertenstein, Bernd A1 - Khandanpour, Cyrus A1 - Dechow, Tobias A1 - Hebart, Holger A1 - Jung, Wolfram A1 - Theurich, Sebastian A1 - Maschmeyer, Georg A1 - Salwender, Hans A1 - Hess, Georg A1 - Bittrich, Max A1 - Rasche, Leo A1 - Brioli, Annamaria A1 - Eckardt, Kai-Uwe A1 - Straka, Christian A1 - Held, Swantje A1 - Einsele, Hermann A1 - Knop, Stefan T1 - Kinetics of renal function during induction in newly diagnosed multiple myeloma: results of two prospective studies by the German Myeloma Study Group DSMM JF - Cancers N2 - Background: Preservation of kidney function in newly diagnosed (ND) multiple myeloma (MM) helps to prevent excess toxicity. Patients (pts) from two prospective trials were analyzed, provided postinduction (PInd) restaging was performed. Pts received three cycles with bortezomib (btz), cyclophosphamide, and dexamethasone (dex; VCD) or btz, lenalidomide (len), and dex (VRd) or len, adriamycin, and dex (RAD). The minimum required estimated glomerular filtration rate (eGFR) was >30 mL/min. We analyzed the percent change of the renal function using the International Myeloma Working Group (IMWG) criteria and Kidney Disease: Improving Global Outcomes (KDIGO)-defined categories. Results: Seven hundred and seventy-two patients were eligible. Three hundred and fifty-six received VCD, 214 VRd, and 202 RAD. VCD patients had the best baseline eGFR. The proportion of pts with eGFR <45 mL/min decreased from 7.3% at baseline to 1.9% PInd (p < 0.0001). Thirty-seven point one percent of VCD versus 49% of VRd patients had a decrease of GFR (p = 0.0872). IMWG-defined “renal complete response (CRrenal)” was achieved in 17/25 (68%) pts after VCD, 12/19 (63%) after RAD, and 14/27 (52%) after VRd (p = 0.4747). Conclusions: Analyzing a large and representative newly diagnosed myeloma (NDMM) group, we found no difference in CRrenal that occurred independently from the myeloma response across the three regimens. A trend towards deterioration of the renal function with VRd versus VCD may be explained by a better pretreatment “renal fitness” in the latter group. KW - multiple myeloma KW - renal failure KW - kidney KW - bortezomib KW - lenalidomide KW - induction regimen Y1 - 2021 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-234139 SN - 2072-6694 VL - 13 IS - 6 ER - TY - JOUR A1 - Banales, Jesus M. A1 - Cardinale, Vincenzo A1 - Carpino, Guido A1 - Marzioni, Marco A1 - Andersen, Jesper B. A1 - Invernizzi, Pietro A1 - Lind, Guro E. A1 - Folseraas, Trine A1 - Forbes, Stuart J. A1 - Fouassier, Laura A1 - Geier, Andreas A1 - Calvisi, Diego F. A1 - Mertens, Joachim C. A1 - Trauner, Michael A1 - Benedetti, Antonio A1 - Maroni, Luca A1 - Vaquero, Javier A1 - Macias, Rocio I. R. A1 - Raggi, Chiara A1 - Perugorria, Maria J. A1 - Gaudio, Eugenio A1 - Boberg, Kirsten M. A1 - Marin, Jose J. G. A1 - Alvaro, Domenico T1 - Cholangiocarcinoma: current knowledge and future perspectives consensus statement from the European Network for the Study of Cholangiocarcinoma (ENS-CCA) JF - Nature Reviews Gastroenterology & Hepatology N2 - Cholangiocarcinoma (CCA) is a heterogeneous group of malignancies with features of biliary tract differentiation. CCA is the second most common primary liver tumour and the incidence is increasing worldwide. CCA has high mortality owing to its aggressiveness, late diagnosis and refractory nature. In May 2015, the "European Network for the Study of Cholangiocarcinoma" (ENS-CCA: www.enscca.org or www.cholangiocarcinoma.eu) was created to promote and boost international research collaboration on the study of CCA at basic, translational and clinical level. In this Consensus Statement, we aim to provide valuable information on classifications, pathological features, risk factors, cells of origin, genetic and epigenetic modifications and current therapies available for this cancer. Moreover, future directions on basic and clinical investigations and plans for the ENS-CCA are highlighted. KW - primary sclerosing cholangitis KW - growth-factor-receptor KW - biliary-tract cancer KW - epithelial-mesenchymal transition KW - fine-needle-aspiration KW - human intrahepatic cholangiocarcinoma KW - induce cyclooxygenase-2 expression KW - human cholangiocellular carcinoma KW - nucleoside transporter KW - hepatic stellate cells Y1 - 2016 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-189077 VL - 13 IS - 5 ER - TY - JOUR A1 - Bankoglu, Ezgi Eyluel A1 - Tschopp, Oliver A1 - Schmitt, Johannes A1 - Burkard, Philipp A1 - Jahn, Daniel A1 - Geier, Andreas A1 - Stopper, Helga T1 - Role of PTEN in Oxidative Stress and DNA Damage in the Liver of Whole-Body Pten Haplodeficient Mice JF - PLoS One N2 - Type 2 diabetes (T2DM) and obesity are frequently associated with non-alcoholic fatty liver disease (NAFLD) and with an elevated cancer incidence. The molecular mechanisms of carcinogenesis in this context are only partially understood. High blood insulin levels are typical in early T2DM and excessive insulin can cause elevated reactive oxygen species (ROS) production and genomic instability. ROS are important for various cellular functions in signaling and host defense. However, elevated ROS formation is thought to be involved in cancer induction. In the molecular events from insulin receptor binding to genomic damage, some signaling steps have been identified, pointing at the PI3K/AKT pathway. For further elucidation Phosphatase and Tensin homolog (Pten), a tumour suppressor phosphatase that plays a role in insulin signaling by negative regulation of PI3K/AKT and its downstream targets, was investigated here. Dihydroethidium (DHE) staining was used to detect ROS formation in immortalized human hepatocytes. Comet assay and micronucleus test were performed to investigate genomic damage in vitro. In liver samples, DHE staining and western blot detection of HSP70 and HO-1 were performed to evaluate oxidative stress response. DNA double strand breaks (DSBs) were detected by immunohistostaining. Inhibition of PTEN with the pharmacologic inhibitor VO-OHpic resulted in increased ROS production and genomic damage in a liver cell line. Knockdown of Pten in a mouse model yielded increased oxidative stress levels, detected by ROS levels and expression of the two stress-proteins HSP70 and HO-1 and elevated genomic damage in the liver, which was significant in mice fed with a high fat diet. We conclude that PTEN is involved in oxidative stress and genomic damage induction in vitro and that this may also explain the in vivo observations. This further supports the hypothesis that the PI3K/AKT pathway is responsible for damaging effects of high levels of insulin. KW - insulin KW - mouse models DNA damage KW - oxidative stress KW - mammalian genomics KW - fatty liver KW - micronuclei KW - insulin signaling Y1 - 2016 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-146970 VL - 11 IS - 11 ER - TY - JOUR A1 - Bannasch, Johannes H. A1 - Berger, Benjamin A1 - Schwartkopp, Claus-Peter A1 - Berning, Marco A1 - Goetze, Oliver A1 - Panning, Marcus A1 - Fritz-Weltin, Miriam A1 - Trendelenburg, George A1 - Gelderblom, Mathias A1 - Lütgehetmann, Marc A1 - Stute, Fridrike A1 - Horvatits, Thomas A1 - Dirks, Meike A1 - Antoni, Christoph A1 - Behrendt, Patrick A1 - Pischke, Sven T1 - HEV-associated neuralgic amyotrophy: a multicentric case series JF - Pathogens N2 - Background: Neuralgic amyotrophy (NA) has been described as a possible extrahepatic manifestation of hepatitis E virus (HEV) infection. Usually, HEV-associated NA occurs bilaterally. The clinical characteristics determining the course of HEV-associated NA have still not been defined. Methods: In this retrospective multicentric case series, 16 patients with HEV-associated NA were studied and compared to 176 HEV patients without NA in terms of their age, sex, and ALT levels. Results: Neither gender distribution (75% vs. 67% male) nor age (47 vs. 48 years median) differed significantly between the NA patients and controls. Eight NA patients (50%) presented with bilateral involvement — seven of these had right-side dominance and one had left-side dominance. Thirteen cases (81%) were hospitalized. Eight of these patients stayed in hospital for five to seven days, and five patients stayed for up to two weeks. The time from the onset of NA to the HEV diagnosis, as well as the diagnostic and therapeutic proceedings, showed a large variability. In total, 13 (81%) patients received treatment: 1/13 (8%) received intravenous immunoglobulins, 8/13 (62%) received glucocorticoids, 3/13 (23%) received ribavirin, and 6/13 (46%) received pregabalin/gabapentin. Patients with ages above the median (47 years) were more likely to be treated (p = 0.001). Conclusion: HEV-associated NA causes a relevant morbidity. In our case series neither the type of treatment nor the time of initiation of therapy had a significant effect on the duration of hospitalization or the course of the disease. The clinical presentation, the common diagnostic and therapeutic procedures, and the patients' characteristics showed large variability, demonstrating the necessity of standardized protocols for this rare but relevant disease. KW - Hepatitis E KW - HEV KW - neuralgic amyotrophy KW - NA Y1 - 2021 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-239691 SN - 2076-0817 VL - 10 IS - 6 ER - TY - JOUR A1 - Barej, Michael F. A1 - Schmitz, Andreas A1 - Penner, Johannes A1 - Doumbia, Joseph A1 - Sandberger-Loua, Laura A1 - Hirschfeld, Mareike A1 - Brede, Christian A1 - Emmrich, Mike A1 - Kouamé, N'Goran Germain A1 - Hillers, Annika A1 - Gonwouo, Nono L. A1 - Nopper, Joachim A1 - Adeba, Patrick Joël A1 - Bangoura, Mohamed A. A1 - Gage, Ceri A1 - Anderson, Gail A1 - Rödel, Mark-Oliver T1 - Life in the spray zone - overlooked diversity in West African torrent-frogs (Anura, Odontobatrachidae, Odontobatrachus) JF - Zoosystematics and Evolution N2 - West African torrent-frogs of the genus Odontobatrachus currently belong to a single species: Odontobatrachus natator (Boulenger, 1905). Recently, molecular results and biogeographic separation led to the recognition of five Operational Taxonomic Units (OTUs) thus identifying a species-complex. Based on these insights, morphological analyses on more than 150 adult specimens, covering the entire distribution of the family and all OTUs, were carried out. Despite strong morphological congruence, combinations of morphological characters made the differentiation of OTUs successful and allowed the recognition of five distinct species: Odontobatrachus natator, and four species new to science: Odontobatrachus arndti sp. n., O. fouta sp. n., O. smithi sp. n. and O. ziama sp. n. All species occur in parapatry: Odontobatrachus natator is known from western Guinea to eastern Liberia, O. ziama sp. n. from eastern Guinea, O. smithi sp. n. and O. fouta sp. n. from western Guinea, O. arndti sp. n. from the border triangle Guinea-Liberia-Cote d'Ivoire. In addition, for the first time the advertisement call of a West African torrent-frog (O. arndti sp. n.) is described. KW - Guinean rain forest KW - molecular data KW - conservation KW - Upper Guinea KW - new species KW - Phrynobatrachus amphibia KW - Arthroleptis amphibia KW - ivory coast KW - genus KW - biodiversity KW - Ranidae KW - Petropedetidae KW - biodiversity hotspot KW - rainforest KW - taxonomy KW - Amphibia Y1 - 2015 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-144254 VL - 91 IS - 2 ER - TY - THES A1 - Bauer, Jonas T1 - Bedeutung eines spezifischen Genpolymorphismus (IL28B) für die Verträglichkeit einer Interferontherapie bei Patienten mit chronischer Hepatitis-C-Infektion T1 - Importance of a specific gene polymorphism (IL28B) for the tolerability of interferon therapy in patients with chronic hepatitis C infection N2 - Vor Einführung der direkt antiviralen Kombinationstherapien war die Kombination aus pegyliertem Interferon plus Ribavirin die Standardbehandlung für Patienten mit chronischer Hepatitis-C-Infektion. Bei 30% der Patienten zeigten sich neurokognitive sowie depressive Nebenwirkungen, die das dauerhafte Therapieansprechen negativ beeinflussen können. Vor diesem Hintergrund untersuchten wir in unserer Arbeit bei 93 Patienten mit chronischer Hepatitis-C-Infektion den Zusammenhang zwischen drei Single Nucleotide Polymorphismen im Bereich des IL28B-Gens und der Verträglichkeit sowie dem Therapieerfolg einer interferonbasierten Behandlung. Der Vergleich zwischen den Ergebnissen im HADS-(Hospital Anxiety and Depression Scale) sowie TAPS- (Testbatterie zur Aufmerksamkeitsprüfung) Testverfahren mit den Genotypen der drei SNPs zeigte im Studienkollektiv keinen signifikanten Zusammenhang. Hinsichtlich des Therapieerfolges konnten wir bei einem der drei SNPs das C-Allel als positiven Prognosefaktor für das dauerhafte Therapieansprechen nachweisen. N2 - Prior to the introduction of direct antiviral combination therapies, the combination of pegylated interferon plus ribavirin was the standard treatment for patients with chronic hepatitis C infection. In 30% of the patients, neurocognitive and depressive side effects were observed, which could negatively influence the sustained virological response. Against this background, the central question that motivates our work was to investigate the association between three single nucleotide polymorphisms in the IL28B gene and the tolerability and therapeutic outcome of interferon-based treatment in 93 patients with chronic hepatitis C infection. The comparison between two test procedures, the HADS (hospital anxiety and depression scale) and TAPS (test battery for attention testing), with the genotypes of the three SNPs showed no significant association in the study population. In terms of therapeutic success, we were able to demonstrate the C allele in one of the three SNPs as a positive prognostic factor for the sustained virological response. KW - Interferon alpha KW - Verträglichkeit Interferon alpha KW - Nebenwirkungen interferonbasierte Hepatitis-C-Therapie KW - Neuropsychiatrische Nebenwirkungen Interferon alpha KW - Single Nucleotid Polymorphismus IL28B Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-178519 ER - TY - THES A1 - Bauer, Katja T1 - Langzeit-Nachbeobachtung von Patienten aus einer Phase III-Studie zum Vergleich zweier Hochdosischemotherapie-Protokolle bei Patienten mit multiplem Myelom im Stadium II/III („DSMM I“-Studie) T1 - A long-term survey of patients suffering from multiple myeloma in stage II/III in a phase III study to compare two forms of high dose chemotherapy (“DSMM I”-study) N2 - Das multiple Myelom ist trotz intensiver Forschung eine bisher unheilbare maligne Plasmazellerkrankung. Für jüngere Patienten ohne relevante Komorbiditäten ist die Behandlung mit einer Hochdosistherapie gefolgt von einer autologen Stammzelltransplantation der Goldstandard. Bei einer geringen Rate an therapiebedingter Mortalität erzielt diese eine hohe Rate an kompletten Remissionen und damit die Wahrscheinlichkeit für ein längeres Überleben. Um die optimale Konditionierungstherapie zu finden, wurde eine Vielzahl von Chemotherapeutika, teilweise gekoppelt mit Ganzkörperbestrahlung, getestet. In dem in dieser Dissertation schwerpunktmäßig analysierten Langzeit-Datensatzes der „DSMM I“-Studie erfolgte der prospektive Vergleich einer Doppelhochdosis-Chemotherapie mit Melphalan und zweimaliger autologer Stammzelltransplantation und einer Einfachhochdosis-Therapie mit modifizierter Ganzkörperbestrahlung, Busulfan und Cyclophosphamid und einfacher autologer Stammzelltransplantation. Es wurde untersucht, ob sich eines der beiden Konditionierungsschemata hinsichtlich des ereignisfreien Überlebens, des Gesamtüberlebens, des maximalen Ansprechens auf die Therapie oder der Toxizität überlegen zeigte. Bisher publizierte Studien wiesen einen Vorteil der Tandem-Hochdosistherapie gegenüber der Einfachhochdosis-Therapie nach. In dieser Studie hatten beide Therapiegruppen ein exzellentes Gesamtüberleben. Es zeigte sich jedoch keine Überlegenheit einer der Therapien für das ereignisfreie und Gesamtüberleben, trotz signifikant höherer Ansprechrate unter Melphalan. Nach modifizierter Ganzkörperbestrahlung war, wie bereits in anderen Studien beschrieben, die Rate an Nebenwirkungen signifikant erhöht. Die Patienten litten vor allem unter Mukositis, Schmerzen und Pneumonitis. Somit ist die Doppelhochdosistherapie mit Melphalan Therapie der Wahl. Die mediane Nachbeobachtungszeit von knapp 7 Jahren ist im Gegensatz zu vielen anderen Publikationen sehr viel länger als das mediane ereignisfreie Überleben. Dies spricht für die Validität der Daten. N2 - Despite of intensive research multiple myeloma is still an incurable malignant plasma cell disorder. Treatment with high dose chemotherapy followed by autologous stem cell transplantation is the standard of care for younger patients without relevant comorbidities. With a low rate of therapy-related mortality this form of treatment achieves a high rate of complete remissions und thus the possibility of a longer survival. To find the optimal conditioning therapy many different chemotherapeutics, partly with total body irradiation, have been tested. In the long-term data of the ”DSMM I”-study, which have been analyzed in this dissertation, a double high-dose chemotherapy with melphalan and double autologous stem cell transplantation and a single high-dose chemotherapy including total marrow irradiation, busulfan und cyclophosphamide were compared prospectively. It was analyzed whether one of the conditioning regimes was superior according to event-free survival, overall survival and maximal response to therapy or toxicity. Published studies to date proved an advantage of tandem high-dose chemotherapy. In this study both therapy groups had an excellent overall survival. There was no superiority of one therapy concerning event-free or overall survival, despite of a higher rate of response after melphalan. As reported previously, after modified total marrow irradiation significantly more patients had adverse effects. Patients suffered from mucositis, pain and pneumonitis. Thus, double high dose chemotherapy with melphalan is the therapy of choice. The median follow-up of almost seven years is - in contrast to many other publications - much longer than the median event-free survival. This concedes confirms the validity of the data. KW - Multiples Myelom KW - Hochdosischemotherapie KW - Ganzkörperbestrahlung KW - DSMMI-Studie Y1 - 2013 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-105716 ER - TY - THES A1 - Bauer, Nikolaus Johannes T1 - Drug Monitoring von Lopinavir, Efavirenz und Nevirapin im Rahmen der antiretroviralen Kombinationstherapie bei Kindern und Jugendlichen mit HIV-Infektion in Kapstadt, Südafrika T1 - Drug Monitoring of Lopinavir, Efavirenz and Nevirapine in antiretroviral combination therapy of HIV-positive children and adolescents in Cape Town, South Africa N2 - Der Nutzen von Therapeutischem Drug Monitoring (TDM) bei der Behandlung von HIV-infizierten Kindern in Ländern mit geringen finanziellen Ressourcen ist bisher nicht gründlich erforscht worden. Pharmakokinetische Studien antiretroviraler Medikamente haben bei Kindern eine hohe intra- und interpersonale Varianz gezeigt. Dies könnte den kontinuierlichen Prozessen von Reifung, Wachstum und Körperzusammensetzung geschuldet sein. Deswegen könnte TDM zu einer sichereren und erfolgreicheren Behandlung von HIV bei Kindern in Südafrika beitragen. Diese Untersuchung einer pädiatrischen HIV-Kohorte zeigte, dass 73,5 % der Patienten innerhalb des empfohlenen therapeutischen Bereichs ihrer Medikamentenkonzentration waren. Aufgrund einer hohen interpersonalen Varianz antiretroviraler Medikamentenkonzentrationen, eine großen Zahl an Komedikationen mit Interaktionspotential, das Risiko für Non-Adhärenz und Zeichen möglicher Arzneimittelnebenwirkungen, kann TDM die Effizienz und Sicherheit der antiretroviralen Kombinationstherapie von Kindern und Jugendlichen mit HIV verbessern. N2 - The utility of therapeutic drug monitoring (TDM) in HIV-infected children in low resource settings is not thoroughly investigated. Pharmacokinetic studies of antiretroviral drugs (ARVs) in children have shown a wide intra- and interpersonal range. This could be due to continuous processes of maturation, growth and changes in body composition. Therefore, TDM could contribute to a safe and efficient treatment of paediatric HIV in South Africa. This investigation of a paediatric HIV cohort in routine clinical care illustrated 73,5 % of the patients within the recommended therapeutic range of their drug serum concentration. Due to high interpatient variability of antiretroviral drug concentrations, a large number of concomitant medication with potential drug-drug interactions, the risk for non-adherence as well as the presence of possible ART specific adverse events, Therapeutic Drug Monitoring can improve the efficacy and safety of cART of children and adolescents. KW - HIV KW - Südafrika KW - Arzneimittelüberwachung KW - Kinderheilkunde KW - Infektiologie KW - Therapeutisches Drug Monitoring KW - Therapeutic Drug Monitoring KW - Lopinavir KW - Efavirenz KW - Nevirapin Y1 - 2020 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-214647 ER - TY - THES A1 - Bauer, Ruth T1 - Interaktionen von humanen Immuneffektorzellpopulationen mit dem humanpathogenen Pilz Aspergillus fumigatus, sowie der Einfluss von40-0-[2-Hydroxyethyl]rapamycin (RAD) auf deren Funktionen T1 - Interaction of human immune effector cell populations with the pathogenic mold Aspergillus fumigatus, and influence of 40-0-[2-hydroxy-ethyl]rapamycin (RAD) on their functions N2 - Durch die Immunsuppression bei Patienten nach Stammzell- oder Organtransplantation erhöht sich das Risiko für opportunistische Infektionen wie invasive Aspergillose (IA). IA wird hauptsächlich durch den Schimmelpilz Aspergillus fumigatus, der durch die Luft übertragen wird, verursacht. Deshalb haben Erkennung und Therapie von IA in den letzten Jahren eine immer größere Bedeutung erlangt. Für eine erfolgreiche Behandlung sind die Mechanismen des Immunsystems nach Kontaktaufnahme mit dem Pathogen von zentraler Bedeutung. Die Erstinfektion mit A. fumigatus findet in der Lunge statt. Als Bewohner der Alveolen wurden deshalb dendritische Zellen (DCs) auf ihre Fähigkeiten hin untersucht, das Immunsystem anzuregen. DCs besitzen vor allem die wichtigen Aufgaben, das Immunsystem zu modulieren und T-Lymphozyten zur Proliferation anzuregen. Ein Großteil dieser Arbeit befasst sich mit der Analyse des Einflusses des Immunsuppressivums 40-0-[2-Hydroxyethyl]rapamycin (RAD) auf neutrophile Granulozyten und auf die in vitro Generierung von moDCs sowie deren Fähigkeit mit dem Pathogen A. fumigatus zu interagieren. RAD bindet an das zytosolische FK506 bindende Protein (FKBP12), wodurch die Kinase mammalian target of rapamycin (mTOR) inhibiert und somit die T-Zellantwort unterdrückt wird. Klinische Anwendung findet RAD bereits, um eine Immunsuppression bei Patienten nach Stammzell- oder Organtransplantation zu erhalten. Der oxidative Burst neutrophiler Granulozyten war nach RAD-Behandlung und Konfrontation mit A. fumigatus signifikant verringert. Die Generierung der moDCs aus Monozyten erfolgte über 7 Tage, wobei ab dem Tag der Isolation der Monozyten 10 nM RAD oder EtOH zur Kontrolle hinzugegeben wurde. RAD zeigte vielfältige Effekte auf die Immunfunktion dendritischer Zellen. Obwohl sich keine Änderung in der Differenzierung der moDCs fand, was durch die Oberflächenmarker CD1a+, CD14- und HLA-DR+ überprüft wurde, zeigte sich eine signifikante Reduktion der Rezeptoren TLR4 und Dectin-1 sowie der kostimulatorischen Moleküle CD40, CD83 und CD86. Nach Konfrontation mit A. fumigatus verblieb CD40 unter RAD Behandlung signifikant reduziert, während CD83 genau dieses Schema als Trend aufwies. Ferner wies CD86 sowohl in der Kontrolle als auch mit RAD-Behandlung die gleiche Expression auf. Nach 6 h Konfrontation der moDCs mit A. fumigatus waren die Zytokine IL-12, TNF-α und CCL20 auf Genexpressionsebene unter RAD reduziert, was sich auf Proteinebene teilweise bestätigen ließ, da sich hier erst nach 12 h eine signifikante Reduktion von IL-12, TNF-α und CCL20 in RAD-behandelten Zellen im Vergleich zu Kontrollzellen zeigte. Des Weiteren war das anti-inflammatorische Zytokin IL-10 signifikant reduziert. Die Phagozytose sowohl von FITC-Dextran-Beads als auch von A. fumigatus Konidien und zugleich die Schädigung von A. fumigatus Keimschläuchen war in unreifen RAD-behandelten moDCs signifikant reduziert. Ob moDCs, die mit RAD behandelt wurden, schlechter in der Lage waren, CD8+-T-Lymphozyten zur Proliferation anzuregen, geht nicht mit Sicherheit aus dieser Studie hervor, da große spenderabhängige Unterschiede auftraten. Es wurde zudem ein Vergleich von in vitro aus Monozyten differenzierten DCs (moDCs) und myeloiden DCs (mDCs) angefertigt. Mittels eines home-made Microarrays, der vor allem Gene mit einschloss, die für Zytokine und Rezeptoren von Immunzellen kodieren, konnten in einem Modell der frühen IA in der Lunge differentiell regulierte Gene nach Konfrontation mit A. fumigatus identifiziert werden. Es wurden insgesamt 30 Gene mehr als 2-fach reguliert, wie zum Beispiel die Interleukine und Chemokine IL-1β, IL-8, CXCL2, CCL3, CCL4 und CCL20, der Immunrezeptor PTX3 und der Transkriptionsfaktor Nf-κB. Generell konnte beobachtet werden, dass moDCs mehr regulierte Gene aufwiesen als mDCs. Zuletzt wurde betrachtet, ob der Knock-down von CXCL10, dessen Fehlen ein erhöhtes Risiko für IA nach sich zieht, einen Einfluss auf moDCs hat, so dass sie schlechter auf A. fumigatus reagieren können. Diese Hypothese konnte in dieser Studie nicht bestätigt werden, da kein Unterschied in der Zytokinproduktion oder Expression kostimulatorischer Moleküle zwischen Kontroll-moDCs und moDCs, in denen das CXCL10-Gen ausgeschaltet wurde, festgestellt werden konnte. Zusammenfassend lässt sich sagen, dass durch die Microarray-Analyse wichtige Gene in moDCs und mDCs identifizierbar waren, die nach Konfrontation mit A. fumigatus reguliert wurden. Zudem fanden sich lediglich minimale Unterschiede zwischen artifiziellen DCs und myeloiden DCs, die direkt aus dem Körper isoliert wurden. Eine Behandlung mit RAD erhöht das Risiko eines Patienten an invasiver Aspergillose zu erkranken unabhängig von der Eigenschaft des RAD, die Proliferation von T-Lymphozyten zu inhibieren. N2 - Following a stem cell or solid organ transplant immunosuppressed patients have an increased risk of developing opportunistic infections such as invasive aspergillosis (IA), which is mainly caused by the most prevalent airborne mold, Aspergillus fumigatus. The diagnosis and therapy of IA have become increasingly relevant in recent years, making it essential to understand the mechanisms of the immune system. The infection generally spreads from the lung. Dendritic cells (DCs), whose major task is to activate T-lymphocytes, were therefore investigated for their ability to influence the immune system. 40-0-[2-Hydroxy-ethyl]rapamycin (RAD), a novel immunosuppressive drug, was analysed for its in vitro influence on the interaction of neutrophils and monocyte-derived dendritic cells (moDCs) with the pathogenic mould, A. fumigatus. RAD acts by bonding with the cytosolic FK506 binding protein (FKBP12) causing inhibition of the lipid kinase mammalian target of rapamycin (mTOR) which in turn results in the repression of T-cell activation. It is clinically used to prevent graft-versus-host disease or the rejection of solid organ and bone marrow transplants. RAD-treatment significantly decreased the oxidative burst of neutrophils after confrontation with A. fumigatus. moDCs were derived from monocytes through culture with granulocyte-macrophage colony-stimulating factor and interleukin-4 in the presence or absence of 10 nM RAD. Although there was no difference in the expression of the surface markers CD1a+, CD14- and HLA-DR+, RAD had various modulating effects on the immune function of moDCs. It reduced the expression of innate immunity receptors (TLR4 and dectin-1) and impaired the maturation capacity of moDCs as was observed in the reduction of co-stimulatory factors (CD40, CD83 and CD86). CD40 remained significantly reduced even after treatment with A. fumigatus, while CD83 only exhibit a downstream trend and CD86 did not stay reduced. RAD treatment significantly reduced the cytokine expression levels of IL-12, TNF-α, and CCL20 after 6 h stimulation of the moDCs with the mold. This was to some extent confirmed at protein level, where the same cytokines as well as IL-10 were significantly reduced in RAD-treated moDCs by comparison with reference cells after 12 h of stimulation with A. fumigatus. The phagocytosis and binding rate of dextran beads and conidia as well as the damage to A. fumigatus germ tubes were significantly reduced in DCs treated with the agent. It cannot be determined for certain whether moDCs under RAD-treatment were also less able to activate CD8+-Tlymphocytes because of the wide donor related discrepancies that they displayed. A home-made RNA microarray, which included genes coding for cytokines and receptors of immune cells, was used to identify several differentially regulated genes after confrontation with A. fumigatus. Furthermore, a comparison between monocyte-derived dendritic cells (moDCs) and myeloid dendritic cells (mDCs) was performed, revealing that only a few genes were regulated more than 2-fold and that fewer of these genes occured in mDCs than in moDCs. Among them were genes, such as the cytokines IL-1β, IL-8, CXCL2, CCL3, CCL4 and CCL20, the immune receptor PTX3 and the transcription factor Nf-κB. Finally, it was investigated whether the knock-down of the CXCL10-gene in moDCs potentially impaired the response of the immune cells to A. fumigatus. It is proven that the lack of CXCL10 results in a higher risk of IA. However, there was no difference in the cytokine production or the expression of co-stimulatory factors in control moDCs compared to moDCs treated with CXCL10 siRNA. In conclusion, important genes which had been up-regulated after confrontation with A. fumigatus in moDCs and mDCs, were successfully identified. Moreover, treatment with RAD during the generation of moDCs had a considerable effect on the ability of these cells to kill A. fumigatus and modulate the immune response. RAD treatment could thus increase the patient's risk of contracting invasive aspergillosis regardless of the drug's capacity to inhibit T-cell activation. KW - Aspergillus fumigatus KW - Dendritische Zellen KW - Immunsuppression KW - RAD KW - Aspergillus fumigatus KW - RAD KW - dendritiric cells Y1 - 2011 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-65499 ER - TY - JOUR A1 - Becker, Philip P. A1 - Rau, Monika A1 - Schmitt, Johannes A1 - Malsch, Carolin A1 - Hammer, Christian A1 - Bantel, Heike A1 - Müllhaupt, Beat A1 - Geier, Andreas T1 - Performance of serum microRNAs -122, -192 and -21 as biomarkers in patients with non-alcoholic steatohepatitis JF - PLoS ONE N2 - Objectives Liver biopsies are the current gold standard in non-alcoholic steatohepatitis (NASH) diagnosis. Their invasive nature, however, still carries an increased risk for patients' health. The development of non-invasive diagnostic tools to differentiate between bland steatosis (NAFL) and NASH remains crucial. The aim of this study is the evaluation of investigated circulating microRNAs in combination with new targets in order to optimize the discrimination of NASH patients by non-invasive serum biomarkers. Methods Serum profiles of four microRNAs were evaluated in two cohorts consisting of 137 NAFLD patients and 61 healthy controls. In a binary logistic regression model microRNAs of relevance were detected. Correlation of microRNA appearance with known biomarkers like ALT and CK18-Asp396 was evaluated. A simplified scoring model was developed, combining the levels of microRNA in circulation and CK18-Asp396 fragments. Receiver operating characteristics were used to evaluate the potential of discriminating NASH. Results The new finding of our study is the different profile of circulating miR-21 in NASH patients (p<0.0001). Also, it validates recently published results of miR-122 and miR-192 to be differentially regulated in NAFL and NASH. Combined microRNA expression profiles with CK18-Asp396 fragment level scoring model had a higher potential of NASH prediction compared to other risk biomarkers (AUROC = 0.83, 95% CI = 0.754-0.908; p<0.001). Evaluation of score model for NAFL (Score = 0) and NASH (Score = 4) had shown high rates of sensitivity (91%) and specificity (83%). Conclusions Our study defines candidates for a combined model of miRNAs and CK18-Asp396 levels relevant as a promising expansion for diagnosis and in turn treatment of NASH. KW - fatty liver disease KW - independent marker KW - expression KW - injury KW - NAFLD KW - circulating micrornas KW - caspase activation KW - fibrosis KW - miR-122 KW - apoptosis Y1 - 2015 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-145147 VL - 10 IS - 11 ER -