TY - THES A1 - Stadler, David T1 - Studien zur Inflammation und neuronalem Schaden in genetischen Modellen von progredienter Multipler Sklerose T1 - Studies in inflammation and neuronal damage in genetic models of progressive multiple sclerosis N2 - Multiple Sklerose ist eine der häufigsten neurologischen Erkrankungen, die zu motorischen, sensiblen und vegetativen Einschränkungen führt. Häufig beginnt die Erkrankung mit einem schubförmigen Verlauf, dem eine progrediente Verschlechterung folgt. Trotzdem leiden ca. 15% der Patienten bereits von Beginn an, an einer primär progressiven Variante der MS, die bereits mit der progredienten Phase beginnt. Bis jetzt ist die Pathophysiologie nicht vollständig verstanden. Lange Zeit dachte man, dass MS primär eine reine Autoimmun-Erkrankung darstellt, aber in den letzten Jahren ergab sich die Frage, ob es vor allem in den progressiven Formen, eine zytodegenerative Komponente gibt, auf die eine sekundäre Inflammation folgt. Eine mögliche Ursache stellen hier Mutationen des PLP 1 Gens dar, die normalerweise mit leukodystrophischen Erkrankungen assoziiert sind. Es gab zwei Fallberichte, in denen von Patienten berichtet wurde, die unterschiedliche Mutationen in diesem Gen hatten und den klinischen Phänotyp einer MS zeigten. Diese Arbeit sollte nun die Auswirkungen der Mutationen, beziehungsweise einer Nullmutation des PLP 1 Gens in 18- und zum Teil 12-Monate alten Mausmutanten untersuchen. Hier konnten Myelin-Veränderungen und axonaler Schaden in immunhistochemischen Untersuchungen sowie mittels Elektronenmikroskopie und optischer Kohärenztomographie gezeigt werden. Weiter konnte eine Neuroinflammation und damit einhergehend eine zunehmende Anzahl CD8+ T-Zellen sowie einer erhöhten Anzahl an Mikroglia/Makrophagen gefunden werden. Dies ging mit vergleichsweise reduzierten Leistungen der Mutanten bei der motorischen Rotarod-Analyse einher. Interessanterweise wurde weniger neuraler Schaden in den heterozygoten Varianten gefunden, obwohl das Ausmaß der Entzündung gleichblieb. Dies könnte für eine zielgerichtete immunvermittelte Schädigung der Oligodendrozyten sprechen, die zu neuronalem Schaden führt. So konnte gezeigt werden, dass es durch Punktmutationen in einem Myelinprotein-codierendem Gen zu einer sekundären Entzündung kommen kann, die mit dem klinischen Phänotyp einer progressiven MS einhergeht. Weiter sind diese Mausmodelle ein Beispiel für eine genetische Erkrankung des ZNS, in denen die Klinik maßgeblich durch die begleitende Inflammation und nicht allein durch den genetischen Schaden verursacht wird. N2 - Multiple sclerosis (MS) is one of the most common neurological diseases, leading to motor, sensory and vegetative impairment. Frequently, the disease begins as a relapsing remitting form, which is followed by a progressive stage. Nevertheless about 15% of the patients suffer under a primary progressive multiple sclerosis, which starts with the progressive stage. Until now the pathophysiology is not completely understood. For a long time, multiple sclerosis was thought to be an autoimmune disease, but in the last years the question arose if the underlying cause, especially in the progressive forms (PMS), could be a cytodegenerative component, followed by secondary inflammation. A possible candidate here could be point mutations in the PLP 1 gene, which are usually associated with leukodystrophic disorders. There were two case reports about patients carrying distinct point mutations in this gene, leading to the clinical phenotype of multiple sclerosis. This thesis examines 18- and in part 12-month-old mice, carrying these point mutations or having a Plp 1 null mutation. Here myelin alterations and axonal damage in immunohistochemical stainings could be shown, as well as in the optical coherence tomography and electron microscopy. Furthermore, the occurrence of neuroinflammation comprising recruitment of microglia/macrophages and CD8 positive T-cells could be demonstrated. Also, typical clinical symptoms in the Rotarod test were found. Interestingly, there was less neural damage found in heterozygous females than in homozygous mutant mice, while the extent of inflammation was the same. This could indicate a targeted immune-mediated injury of oligodendrocytes leading to neuronal damage. In summary, this thesis shows that a point mutation of a gene coding for a myelin protein of oligodendrocytes can lead to secondary neuroinflammation and a neurological phenotype comparable to PMS. In addition, the generated mouse models are an example for genetic diseases of the CNS, in which the clinical outcome could be driven by inflammation and not only by the primary gene mutation. KW - Multiple Sklerose KW - Maus KW - Genetik KW - Immunsystem KW - Glia KW - Sekundäre Inflammation KW - Neuroinflammation KW - Neurodegeneration KW - Mikroglia KW - Mausmodell Y1 - 2021 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-236923 ER - TY - JOUR A1 - Holzmann-Littig, Christopher A1 - Stadler, David A1 - Popp, Maria A1 - Kranke, Peter A1 - Fichtner, Falk A1 - Schmaderer, Christoph A1 - Renders, Lutz A1 - Braunisch, Matthias Christoph A1 - Assali, Tarek A1 - Platen, Louise A1 - Wijnen-Meijer, Marjo A1 - Lühnen, Julia A1 - Steckelberg, Anke A1 - Pfadenhauer, Lisa A1 - Haller, Bernhard A1 - Fuetterer, Cornelia A1 - Seeber, Christian A1 - Schaaf, Christian T1 - Locating medical information during an infodemic: information seeking behavior and strategies of health-care workers in Germany JF - Healthcare N2 - Background: The COVID-19 pandemic has led to a flood of — often contradictory — evidence. HCWs had to develop strategies to locate information that supported their work. We investigated the information-seeking of different HCW groups in Germany. Methods: In December 2020, we conducted online surveys on COVID-19 information sources, strategies, assigned trustworthiness, and barriers — and in February 2021, on COVID-19 vaccination information sources. Results were analyzed descriptively; group comparisons were performed using χ\(^2\)-tests. Results: For general COVID-19-related medical information (413 participants), non-physicians most often selected official websites (57%), TV (57%), and e-mail/newsletters (46%) as preferred information sources — physicians chose official websites (63%), e-mail/newsletters (56%), and professional journals (55%). Non-physician HCWs used Facebook/YouTube more frequently. The main barriers were insufficient time and access issues. Non-physicians chose abstracts (66%), videos (45%), and webinars (40%) as preferred information strategy; physicians: overviews with algorithms (66%), abstracts (62%), webinars (48%). Information seeking on COVID-19 vaccination (2700 participants) was quite similar, however, with newspapers being more often used by non-physicians (63%) vs. physician HCWs (70%). Conclusion: Non-physician HCWs more often consulted public information sources. Employers/institutions should ensure the supply of professional, targeted COVID-19 information for different HCW groups. KW - COVID-19 KW - infodemic KW - health-care workers KW - HCW KW - information strategies KW - emergency information Y1 - 2023 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-319306 SN - 2227-9032 VL - 11 IS - 11 ER - TY - JOUR A1 - Groh, Janos A1 - Stadler, David A1 - Buttmann, Mathias A1 - Martini, Rudolf T1 - Non-invasive assessment of retinal alterations in mouse models of infantile and juvenile neuronal ceroid lipofuscinosis by spectral domain optical coherence tomography N2 - Introduction The neuronal ceroid lipofuscinoses constitute a group of fatal inherited lysosomal storage diseases that manifest in profound neurodegeneration in the CNS. Visual impairment usually is an early symptom and selective degeneration of retinal neurons has been described in patients suffering from distinct disease subtypes. We have previously demonstrated that palmitoyl protein thioesterase 1 deficient (Ppt1-/-) mice, a model of the infantile disease subtype, exhibit progressive axonal degeneration in the optic nerve and loss of retinal ganglion cells, faithfully reflecting disease severity in the CNS. Here we performed spectral domain optical coherence tomography (OCT) in Ppt1-/- and ceroid lipofuscinosis neuronal 3 deficient (Cln3-/-) mice, which are models of infantile and juvenile neuronal ceroid lipofuscinosis, respectively, in order to establish a non-invasive method to assess retinal alterations and monitor disease severity in vivo. Results Blue laser autofluorescence imaging revealed increased accumulation of autofluorescent storage material in the inner retinae of 7-month-old Ppt1-/- and of 16-month-old Cln3-/- mice in comparison with age-matched control littermates. Additionally, optical coherence tomography demonstrated reduced thickness of retinae in knockout mice in comparison with age-matched control littermates. High resolution scans and manual measurements allowed for separation of different retinal composite layers and revealed a thinning of layers in the inner retinae of both mouse models at distinct ages. OCT measurements correlated well with subsequent histological analysis of the same retinae. Conclusions These results demonstrate the feasibility of OCT to assess neurodegenerative disease severity in mouse models of neuronal ceroid lipofuscinosis and might have important implications for diagnostic evaluation of disease progression and therapeutic efficacy in patients. Moreover, the non-invasive method allows for longitudinal studies in experimental models, reducing the number of animals used for research. KW - Optical coherence tomography KW - Neuronal ceroid lipofuscinosis KW - Neurodegeneration KW - Retinal degeneration KW - Lysosomal storage disease Y1 - 2014 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-110566 ER -