TY - THES A1 - Dufner, Vera Christine T1 - Effektivität und Sicherheit von Blinatumomab im Long-term Follow-up bei Non-Hodgkin-Lymphom-Patienten T1 - Long-term Follow-up of safety and efficacy of Blinatumomab in Non-Hodgkin-Lymphoma patients N2 - Das Non-Hodgkin-Lymphom (NHL) steht an siebter Stelle der Inzidenzen aller Krebserkrankungen, mit jährlich steigender Tendenz. Wie kann einer so gefährlichen und heterogenen Krankheitsentität in der heutigen Medizin angemessen begegnet werden? Neben etablierten Therapien, die geraden bei rezidivierten oder refraktären NHL an ihre Grenzen stoßen, bieten experimentelle Therapieansätze neue Hoffnung: Blinatumomab ist ein bispezifischer Antikörper, der durch seine beiden Domänen als Adapter für die T-Zelle und die Tumor-Zelle fungiert und eine Zytolyse der malignen B-Zelle induziert. Bei der ALL fand Blinatumomab schon Anwendung in mehreren klinischen Studien und wurde im Dezember 2014 von der FDA in den USA zur Behandlung von Philadelphia-Chromosom-negativer rezidivierten/ refraktären B-Zell Vorläufer-ALL zugelassen. Als erste klinische Studie an NHL-Patienten wurde von 2004-2011 die MT103/104-Studie veranlasst. Im Zuge dieser unverblindeten, multizentrischen Phase I/II Studie wurden 76 Patienten mit refraktärem und rezidiviertem NHL vier bis acht Wochen mit Blinatumomab als Dauerinfusion behandelt und hierbei Informationen zu Toxizität und Tolerabilität gesammelt. Mit der Langzeitbeobachtung der Würzburger Kohorte aus dieser Studie befasst sich die vorliegende Arbeit. Ziel ist es zunächst, festzustellen, wie lange die Patienten nach Blinatumomab-Therapie im Zuge der MT103/104 Studie gesamt, rezidiv- oder therapiefrei überlebten und ob bei einem bestimmten Patientensubkollektiv ein besonders vorteilhaftes Langzeitüberleben gezeigt werden kann. Die Frage nach der Sicherheit von Blinatumomab beantwortet die Erfassung des Langzeitnebenwirkungsspektrums: Somit werden als zweiter Endpunkt die häufigsten Gründe für Krankenhausaufenthalte nach Blinatumomabtherapie, eventuelle Häufungen einer spezifischen Nebenwirkungsentität und die Reversibilität der unter der Therapie aufgetretenen Nebenwirkungen mit einem selbst entwickelten Fragebogen erfasst. Der MoCA-Test soll neurokognitive Langzeittoxizitäten ausschließen. Die Arbeit konnte nicht nur zeigen, dass Patienten, die auf Blinatumomab ansprachen gegenüber den Patienten ohne Ansprechen ein deutlich längeres Überleben zeigten, sie bestätigte die Wichtigkeit des Erhalts der effektiven Dosis von 60 µg/m²/24h für das Erreichen und den Erhalt der Progressionsfreiheit. Sechs Patienten waren bei Beobachtungsende noch in Remission. Die unterschiedlichen Eindosierungsmodi hatten keinen Effekt auf das Langzeitüberleben, können aber nebenwirkungsbedingte Therapieabbrüche während der Therapie minimieren. Alle während der Therapie aufgetretenen Nebenwirkungen waren in der Langzeitnachbeobachtung vollständig reversibel. Am häufigsten mussten Patienten auf Grund von Infektionen im Verlauf hospitalisiert werden, bei zwei Patienten traten zusätzliche Tumorerkrankungen auf, die allerdings nicht mit der Blinatumomab-Therapie assoziiert waren. Die Rate der Transformationen von indolenten in aggressive NHL war nicht erhöht. Im MoCA-Test lassen sich keine Häufungen von neurokognitiven Defiziten finden. Blinatumomab zeigt sich auch in der Langzeitbeobachtung als ein für die Behandlung von rezidivierten und refraktären NHLs effektives und sicheres Medikament. N2 - The incidence of NHL ranks on seventh position of all cancer types with a tendency to increase year by year. How can we face such a dangerous and heterogenous entity in today’s medicine? Besides established therapy options, which find their boundaries in relapsed or refractory NHL, new, experimental approaches raise new hope: Blinatumomab is a bispecific antibody, which is able to link T-cells to tumor cells, and thus induces cytolysis of the malign B-cell. Blinatumomab was applied in ALL patients in multiple clinical trials and was admitted by the FDA for treatment of Philadelphia-chromosome negative, relapsed or refractory B-cell precursor ALL in December 2014 in the U.S.. The first clinical trial in NHL patients (MT103/104) was initiated 2004-2011. During this open-labeled, multicenter, phase I/II study, 76 patients with relapsed or refractory NHL received Blinatumomab for four to eight weeks as a continous intravenous infusion, whilst data about tolerability and toxicity were collected. The aim of this work is the long-term follow-up of the patients, who were treated in Wuerzburg. First and foremost, the goal is to determine overall, progression-free and therapy-free survival of the patients, who received Blinatumomab during the MT103/104 trial, and if a certain subgroup shows an outstanding long-term survival. The second goal is to acquire long-term safety data and collect the possible spectrum of side-effects after Blinatumomab treatment. Therefore, the most frequent reasons for hospitalization after Blinatumomab administration, potential accumulation of certain side-effects and the reversibility of the witnessed adverse events were recorded by a self-generated questionnaire. The MoCA-test is to exclude long-term neurotoxicity. This work shows, that patients who responded to blinatumomab had a significantly longer OS, PFS and TFS in comparison to patients who did not respond to blinatumomab. The work also confirmed the importance of treatment on a target dose (60 µg/m²/d) in order to achieve and preserve PFS. Six patients were still in remission at the end of observation. The different steps of dosing (single, double, flat) couldn’t show any effect on the long-term survival, but where able to minimize side-effect-related treatment dropouts. Every single witnessed adverse-event during therapy is fully reversible. The most common reason for hospitalization after treatment cessation were infections, two patients experienced other malignancies, however not associated with Blinatumomab treatment. The number of transformations from indolent to aggressive lymphomas was not elevated. The MoCA-test doesn’t show any accumulation of neurocognitive impairment. Thus, Blinatumomab is safe and effective in the treatment of relapsed and refractory NHL. KW - Non-Hodgkin-Lymphom KW - Blinatumomab Y1 - 2020 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-184762 ER - TY - JOUR A1 - Dufner, Vera A1 - Kessler, Almuth Friederike A1 - Just, Larissa A1 - Hau, Peter A1 - Bumes, Elisabeth A1 - Pels, Hendrik Johannes A1 - Grauer, Oliver Martin A1 - Wiese, Bettina A1 - Löhr, Mario A1 - Jordan, Karin A1 - Strik, Herwig T1 - The emesis trial: depressive glioma patients are more affected by chemotherapy-induced nausea and vomiting JF - Frontiers in Neurology N2 - Purpose Glioma patients face a limited life expectancy and at the same time, they suffer from afflicting symptoms and undesired effects of tumor treatment. Apart from bone marrow suppression, standard chemotherapy with temozolomide causes nausea, emesis and loss of appetite. In this pilot study, we investigated how chemotherapy-induced nausea and vomiting (CINV) affects the patients' levels of depression and their quality of life. Methods In this prospective observational multicentre study (n = 87), nausea, emesis and loss of appetite were evaluated with an expanded MASCC questionnaire, covering 10 days during the first and the second cycle of chemotherapy. Quality of life was assessed with the EORTC QLQ-C30 and BN 20 questionnaire and levels of depression with the PHQ-9 inventory before and after the first and second cycle of chemotherapy. Results CINV affected a minor part of patients. If present, it reached its maximum at day 3 and decreased to baseline level not before day 8. Levels of depression increased significantly after the first cycle of chemotherapy, but decreased during the further course of treatment. Patients with higher levels of depression were more severely affected by CINV and showed a lower quality of life through all time-points. Conclusion We conclude that symptoms of depression should be perceived in advance and treated in order to avoid more severe side effects of tumor treatment. Additionally, in affected patients, delayed nausea was most prominent, pointing toward an activation of the NK1 receptor. We conclude that long acting antiemetics are necessary totreat temozolomide-induced nausea. KW - glioblastoma KW - chemotherapy KW - depression KW - nausea and emesis KW - quality of life Y1 - 2022 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-262859 SN - 1664-2295 VL - 13 ER - TY - JOUR A1 - Linsenmann, Thomas A1 - März, Alexander A1 - Dufner, Vera A1 - Stetter, Christian A1 - Weiland, Judith A1 - Westermaier, Thomas T1 - Optimization of radiation settings for angiography using 3D fluoroscopy for imaging of intracranial aneurysms JF - Computer Assisted Surgery N2 - Mobile 3D fluoroscopes have become increasingly available in neurosurgical operating rooms. We recently reported its use for imaging cerebral vascular malformations and aneurysms. This study was conducted to evaluate various radiation settings for the imaging of cerebral aneurysms before and after surgical occlusion. Eighteen patients with cerebral aneurysms with the indication for surgical clipping were included in this prospective analysis. Before surgery the patients were randomized into one of three different scan protocols according (default settings of the 3D fluoroscope): Group 1: 110 kV, 80 mA (enhanced cranial mode), group 2: 120 kV, 64 mA (lumbar spine mode), group 3: 120 kV, 25 mA (head/neck settings). Prior to surgery, a rotational fluoroscopy scan (duration 24 s) was performed without contrast agent followed by another scan with 50 ml of intravenous iodine contrast agent. The image files of both scans were transferred to an Apple PowerMac(R) workstation, subtracted and reconstructed using OsiriX(R) MD 10.0 software. The procedure was repeated after clip placement. The image quality regarding preoperative aneurysm configuration and postoperative assessment of aneurysm occlusion and vessel patency was analyzed by 2 independent reviewers using a 6-grade scale. This technique quickly supplies images of adequate quality to depict intracranial aneurysms and distal vessel patency after aneurysm clipping. Regarding these features, a further optimization to our previous protocol seems possible lowering the voltage and increasing tube current. For quick intraoperative assessment, image subtraction seems not necessary. Thus, a native scan without a contrast agent is not necessary. Further optimization may be possible using a different contrast injection protocol. KW - 3D fluoroscopy KW - aneurysm KW - fluoroscopy KW - intraoperative imaging Y1 - 2021 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-259251 VL - 26 IS - 1 ER -