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Gastroesophageal junction (GEJ), demarcating the region where the distal esophagus meets with the proximal stomach region, is known for developing pathological conditions, including metaplasia and esophageal adenocarcinoma (EAC). It is essential to understand the mechanisms of developmental stages which lead to EAC since the incidence rate of EAC increased over 7-fold during the past four decades, and the overall five years survival rate is 18.4%. In most cases, patients are diagnosed in the advanced stage without prior symptoms. The main precursor for the development of EAC is a pre-malignant condition called Barrett's esophagus (BE). BE is the metaplastic condition where the multilayered squamous epithelium of the native esophagus is replaced by specialized single-layered columnar epithelium, which shows the molecular characteristics of the gastric as well as intestinal epithelium. The main risk factors for BE development include chronic gastro-esophageal acid reflux disease (GERD), altered microbiota, and altered retinoic acid signaling (RA). The cell of origin of BE is under debate due to a lack of clear evidence demonstrating the process of BE initiation. Here, I investigated how GEJ homeostasis is maintained in healthy tissue by stem cell regulatory morphogens, the role of vitamin A (RA signaling), and how its alteration contributes to BE development.
In the first part of my thesis, I showed the presence of two types of epithelial cells, the squamous type in the esophagus and the columnar type in the stomach region in the GEJ, using single-molecule RNA in situ hybridization (smRNA-ISH) and immunohistochemistry. Employing lineage tracing in the mouse model, I have demonstrated that the esophageal epithelial and stomach epithelial cells derived from two distinct epithelial stem cell lineages in the GEJ. The border between squamous and columnar epithelial cells in the Squamo-columnar junction (SCJ) of GEJ is regulated by opposing Wnt microenvironments. The regeneration of stomach columnar epithelial stem cells is maintained by Wnt activating signal from the stromal compartment while squamous epithelial stem cells of the esophagus are maintained by the Wnt inhibitory signals. I recapitulated the in vivo GEJ epithelial stem cell maintenance by using in vitro epithelial 3D organoid culture model. The growth and propagation of stomach columnar epithelial organoids depend on Wnt growth factors, while squamous epithelial organoids' development needs Wnt-deficient culture conditions.
Further, single-cell RNA sequence (scRNA-seq) analysis of organoid-derived epithelial cells revealed the non-canonical Wnt/ planar cell polarity (PCP) pathway involvement in regulating the squamous epithelial cells. In contrast, columnar stomach epithelial cells are regulated by the canonical Wnt/ beta-catenin and non-canonical Wnt/Ca2+ pathways. My data indicate that the SCJ epithelial cells that merge at the GEJ are regulated by opposing stromal Wnt factors and distinct Wnt pathway signaling in the epithelial cells.
In the second part of the thesis, I investigated the role of Vitamin A-derived bioactive compound RA on esophageal and stomach epithelial stem cells. In vitro treatment of esophageal and stomach, epithelial organoids with RA or its pharmacological inhibitor BMS 493 revealed that each cell type was regulated distinctly. I observed that enhanced RA promoted esophageal stem cell differentiation and loss of stratification, while RA inhibition led to enhanced stemness and regeneration of the esophagus stratified epithelium. As opposed to the esophagus, RA signaling is active in the stomach organoids, and inhibition of RA reduces the growth of stomach organoids. Global transcriptomic data and scRNA-seq data revealed that RA signaling induces dormancy phenotype in the esophageal cells. In contrast, the absence of RA in stomach epithelial cells induces the expression of genes associated with BE. Thus, spatially defined regulation of Wnt and RA signaling at GEJ is critical for healthy homeostasis, and its perturbation leads to disease development.
This compilation focuses on adolescent mental disorders and their prevention. It comprises three distinct studies, each contributing to a deeper understanding of this critical topic. This work addresses a critical gap in the understanding of, and approach to, adolescent mental health, and as a result reveals a critically important and urgently needed policy implication for action. The thematic structure of these studies begins with an examination of the epidemiology of child and adolescent mental disorders. Baseline data were collected from N = 877 adolescents with a mean age of 12.43 years (SD = 0.65). Mental health problems, such as depressive symptoms, non-suicidal self-injury, suicidal ideation, symptoms of eating disorders, and gender differences, are thoroughly examined. Results revealed a significant portion of our sample displaying mental health problems as early as the 6th and 7th grades, with girls generally being more affected than boys. The findings underscore the importance of early adolescence in the emergence of mental health problems and thereby emphasize the need for preventive measures. Moving beyond prevalence estimates, the compilation delves into the etiology of these disorders, exploring their potential correlation with a COVID-19 infection. Understanding the early signs and risk factors is crucial for timely support. While numerous studies have investigated potential risk and protective factors during the pandemic, our focus shifts to adolescents’ coping when an infection with the virus was involved (N = 2,154, M = 12.31, SD = 0.67). We hypothesized that students infected or with close family members infected, would exhibit an increased psychopathology and a decreased functioning of protective factors such as self-efficacy or self-esteem. We found no connection between infection and the mental health status within our sample, but protective factors and mental well-being were positively associated. Thus, universal primary prevention appears to be the preferred approach for promoting mental health. Lastly, the compilation introduces LessStress, a noteworthy contribution to more evidence-based prevention programs. This universal approach is designed to reduce stress in schools, accompanied by a cluster-randomized trial to evaluate its effectiveness (estimated sample size N = 1,894). Existing studies have demonstrated the effectiveness of stress prevention, leading us to introduce a short and easy-to-implement prevention program. There is positive evidence for one-lesson interventions in schools for promoting well-being and health behaviors among adolescents. LessStress is designed based on a life skills approach that not only imparts psychoeducational content but also teaches skills relevant to everyday life and directly applicable. Throughout these studies, a common thread emerges: the pressing need to address mental disorders during childhood and adolescence. These formative years play a pivotal role in the development of mental health problems. These formative years play a crucial role in the development of mental health problems. They highlight the importance of epidemiological data collection and analysis based on the latest models to develop prevention interventions that are not only effective but also reach young people on a global level.
Background
Healthcare workers and medical students faced new challenges during the COVID-19 pandemic. Processes within many hospitals were completely disrupted. In addition, the face to face teaching of medical students was drastically reduced. Those at risk of developing mental health problems appear to be younger health care workers and women.
Objective
To investigate potential COVID-19 pandemic-related gender differences in psychological distress among medical students and physicians in their first years of practice.
Design and setting
An anonymous survey was carried out online between December 1, 2021, and March 31, 2022, at the Mannheim Medical Faculty and the Würzburg Medical Faculty, Germany, after obtaining informed consent. Primary outcome measures were changes in anxiety and depression symptoms using the Hospital Anxiety and Depression Scale (HADS), and changes in participants' current quality of life using the WHO Quality of Life BREF.
Results
The results show wave-like courses for perceived anxiety and burden overlapping with the course of the COVID-19 incidence. In comparison to men, women showed a significant higher increase in HADS (p = 0.005) and a reduced life quality (p = 0.007) after COVID-19. Both sexes showed different frequencies of the factors influencing quality of life, with the presence of a previous mental illness and mean anxiety having a significant higher negative impact in women.
Conclusion
Future and young female physicians reported a disproportionate higher burden during COVID-19 compared to their male colleges. These observations suggest an increased need for support and prevention efforts especially in this vulnerable population.
Background
Haemophilus influenzae (Hi) is a Gram-negative bacterium that may cause sepsis or meningitis, treatment of which mainly includes β-lactam antibiotics. Since 2019 EUCAST breakpoints for piperacillin/tazobactam have been available. Little is known about the prevalence and mechanisms of piperacillin/tazobactam resistance in Hi.
Objectives
To provide reliable prevalence data for piperacillin/tazobactam resistance in Hi in Germany, to evaluate different antibiotic susceptibility testing methods and to examine possible resistance mechanisms.
Methods
According to EUCAST breakpoints, the MIC for piperacillin/tazobactam resistance is >0.25 mg/L. All invasive Hi in Germany from 2019 were examined by gradient agar diffusion (GAD) for piperacillin/tazobactam susceptibility. Piperacillin/tazobactam broth microdilution (BMD), piperacillin GAD on tazobactam-containing agar [piperacillin GAD on Mueller–Hinton agar with horse blood (MH-F)/tazobactam) and piperacillin/tazobactam agar dilution (AD) were used for confirmation. Phenotypic testing was complemented by ftsI sequencing.
Results
Piperacillin/tazobactam GAD resulted in 2.9% (21/726) resistant Hi. BMD did not confirm piperacillin/tazobactam resistance. Two strains were found resistant by AD, of which one was also resistant using piperacillin GAD on MH-F/tazobactam. Overall, we found two strains with a piperacillin/tazobactam MIC >0.25 mg/L in at least two different tests (0.3%). Both were β-lactamase-producing amoxicillin/clavulanate-resistant with PBP3 mutations characterized as group III-like+. Relevant PBP3 mutations occurred in six strains without phenotypic piperacillin/tazobactam resistance. These mutations suggest a reduced efficacy of β-lactam antibiotics in these isolates.
Conclusions
Piperacillin/tazobactam resistance prevalence in invasive Hi is low in Germany. Reduced susceptibility was correlated with PBP3 mutations, in particular with group III mutations.
The reprogramming of metabolic pathways is a hallmark of cancer: Tumour cells are dependent on the supply with metabolites and building blocks to fulfil their increased need as highly proliferating cells. Especially de novo synthesis pathways are upregulated when the cells of the growing tumours are not able to satisfy the required metabolic levels by uptake from the environment.
De novo synthesis pathways are often under the control of master transcription factors which regulate the gene expression of enzymes involved in the synthesis process. The master regulators for de novo fatty acid synthesis and cholesterogenesis are sterol regulatory element-binding proteins (SREBPs). While SREBP1 preferably controls the expression of enzymes involved in fatty acid synthesis, SREBP2 regulates the transcription of the enzymes of the mevalonate pathway and downstream processes namely cholesterol, isoprenoids and building blocks for ubiquinone synthesis.
SREBP activity is tightly regulated at different levels: The post-translational modification by ubiquitination decreases the stability of active SREBPs. The attachment of K48-linked ubiquitin chains marks the transcription factors for the proteasomal degradation. In tumour cells, high levels of active SREBPs are essential for the upregulation of the respective metabolic pathways. The increased stability and activity of SREBPs were investigated in this thesis.
SREBPs are ubiquitinated by the E3 ligase Fbw7 which leads to the subsequential proteolysis of the transcription factors. The work conducted in this thesis identified the counteracting deubiquitination enzyme USP28 which removes the ubiquitin chains from SREBPs and prevents their proteasomal degradation.
It further revealed that the stabilization of SREBP2 by USP28 plays an important role in the context of squamous cancers. Increased USP28 levels are associated with a poor survival in patients with squamous tumour subtypes. It was shown that reduced USP28 levels in cell lines and in vivo result in a decrease of SREBP2 activity and downregulation of the mevalonate pathway. This manipulation led to reduced proliferation and tumour growth.
A direct comparison of adenocarcinomas and squamous cell carcinomas in lung cancer patients revealed an upregulation of USP28 as well as SREBP2 and its target genes. Targeting the USP28-SREBP2 regulatory axis in squamous cell lines by inhibitors also reduced cell viability and proliferation.
In conclusion, this study reports evidence for the importance of the mevalonate pathway regulated by the USP28-SREBP2 axis in tumour initiation and progression of squamous cancer. The combinatorial inhibitor treatment of USP28 and HMGCR, the rate limiting enzyme of the mevalonate pathway, by statins opens the possibility for a targeted therapeutic treatment of squamous cancer patients.
Gegenstand dieser Arbeit war die Ermittlung der Scherfestigkeit von Kompositreparaturen auf unterschiedlichen Materialien und der Einfluss künstlicher Probenalterung auf den Haftverbund. Ziel war es hierüber ein möglichst einfaches Reparaturprotokoll für die klinische Anwendung zu prüfen. In der Versuchsreihe wurden neun verschiedene Materialien (SR Nexco®, Gradia® Plus, Estenia™ C&B®, Grandio Blocs®, Tetric® CAD, Brilliant Crios®, VITA Enamic®, VITABLOCS® Mark II, IPS e.max® CAD) nach einem festgelegten Konditionierungsprotokoll (Sandstrahlen vs. Flusssäureätzung und Monobond® Plus-Applikation, anschließend 3M™ Scotchbond™ Universal Plus Adhäsiv) mit Kompositzylindern (3M™ Filtek™ Supreme XTE Universal Komposit) verklebt. In einem Scherversuch wurden die Haftwerte des Klebeverbundes ermittelt sowie die vorkommenden Versagensmuster untersucht. Werden alle 216 untersuchten Prüfkörper betrachtet, so ist hervorzuheben, dass alle Prüfzylinder Scherkräften von über 21 MPa standhielten. Dennoch zeigten sich Unterschiede unter den Materialgruppen. In den Kontrollgruppen zeigte Estenia™ C&B® mit ±34,5 MPa die höchste Scherfestigkeit. Die modellierbaren Verblend-komposite erreichten mit ±29,6 MPa höhere Haftwerte als die CAD/CAM Komposite (±24,1 MPa) und die keramischen Werkstoffe (±26,7 MPa). Eine künstliche Probenalterung wirkte sich signifikant auf die Verbundfestigkeit aus. Im gesamten Probenkorpus war zwischen den Kontrollgruppen und den Gruppen mit Temperaturwechselbehandlung vor und nach Verklebung eine Reduktion der Scherkraft um ±10,6 MPa zu beobachten. Insgesamt hatte eine Temperaturwechselbehandlung einzig vor Verklebung der Proben zumeist eine geringere Auswirkung auf den Haftverbund verglichen mit Alterung vor und nach Verklebung. Mit einer Inzidenz von 74,5 % war ein kohäsiver Bruch im Ausgangsmaterial das dominierende Versagensmuster. Daraus lässt sich ableiten, dass ein adäquates Konditionierungsprotokoll gewählt wurde. Auch auf das Versagensmuster hatte die Temperaturwechselbehandlung einen signifikanten Einfluss, wobei kohäsive Brüche zunahmen. Die vorliegende Arbeit konnte zeigen, dass Reparaturen in vitro auch zwischen unterschiedlichen Materialklassen suffiziente Haftverbunde erzielen können, obgleich der Verbund bei Kompositen verlässlicher erscheint. Die ermittelten hohen Scherkräfte verdeutlichen, dass die Möglichkeit einer Reparatur am Patienten in jedem Fall in Erwägung gezogen werden sollte, bevor eine Restauration vollständig ausgetauscht wird.
Die vorliegende Arbeit befasst sich mit der Beschreibung des Status quo der Versorgungsrealität von BARMER Patient*innen, welche nach operativem inguinalen- oder femoralen Hernienverschluss an Schmerzen litten und geht in weiterer Folge dessen Hinweisen auf CPIP nach. Es fand die Sekundärdatenanlyse von Routinedaten der BARMER Krankenkasse Anwendung. Die Stichprobe umfasste 11221 Patient*innen, von denen 77.7% unter keinen Leistenschmerzen im prä- oder postoperativen Zusammenhang mit dem Eingriff litten, bezeichnet als Gruppe „Pain 0“. 4.2% litten sowohl innerhalb von 365 Tagen vor- als auch nach dem Krankenhausaufenthalt an Schmerzen, was als chronisch zu bezeichnen war und unter Gruppe „Pain 2“ geführt wurde. 8.5% der Patient*innen litten nur innerhalb von 365 Tagen nach Entlassung an Schmerzen, was nur im erweiterten Sinne auf CPIP hinwies, da der Ausschluss der ersten 90 Tage postoperativ nicht in der Definition der Gruppe enthalten war. Diese Patient*innen gehörten der Gruppe „Pain 1“ an. Die Gruppe „Pain 3“ umfasste diejenigen 9.6% der Patient*innen, welche innerhalb von 365 Tagen präoperativ an Schmerzen litten. Obwohl keine postoperativen Leistenschmerzen für diese Patient*innen codiert worden sind, stellte sich eine bessere Versorgung als die der Gruppe „Pain 0“ dar.
Patient*innen der Gruppe „Pain 2“ mit der längsten Schmerzerfahrung wurden signifikant besser versorgt. Diese Gruppe, welche an chronischen, postoperativen, inguinalen Schmerzen litt, zeichnete sich durch eine signifikant jüngere Patient*innenklientel aus. Der Anteil an Frauen war signifikant höher. Begleitende psychiatrische Komorbiditäten traten signifikant häufiger auf. Die Versorgung dieser Patient*innengruppe war signifikant besser, allerdings vor allem hinsichtlich der psychologischen und psychiatrischen Betreuung nicht ausreichend gut. Die Mehrzahl der Analysen war hochsignifikant, deren Effektstärke fiel klein aus.
Human-environment interaction has significantly altered the pedosphere since the Neolithic, if not since the early Holocene. In the course of clearance, agriculture, and (wood) pasture soils have been deeply modified or eroded. These types of land use practices but above all forms of sedentariness spread alongside floodplains and trajectories were oriented towards loess covered areas where fertile soils could develop. Besides this, also peripheral / marginal regions were settled due to population pressure or other factors. Evidence for landscape history and development can be found within archeological sites but also overbank deposits and anthropogenic slope deposits document vast transformation processes.
The presented investigations took place within the natural region of the Windsheimer Bucht which is locat-ed in the district of Middle Franconia in northern Bavaria, Germany. In this area, Holocene soils predomi-nantly developed within mudstones of the Middle to Upper Triassic. The soil texture is extremely clay-rich which renders the soils problematic with regard to cultivation management. As a peculiarity, the gypsum underlying the mudstones is prone to karstification processes and resulting proceeding geomorphological processes shape the surface of the landscape. In the course of gypsum mining the karst forms are being exposed and archeological findings are being documented. The latter mainly date back to a span from the Neolithic to the Iron Age, but partly are of Younger Paleolithic origin. Especially subsidence sinkholes are capable of storing pedosediments of several meters in thickness. Despite the high clay content and connect-ed pedoturbation processes, the excavated sequences are stratigraphically and pedologically well-differentiated. The archives occur in the context of settlement structures such as pits and postholes; there-fore, they developed at the interface of natural developments and human impact on their surroundings.
The main original research questions that were formulated within the general frame of a project funded by the Deutsche Forschungsgemeinschaft (DFG-projects Te295/15-1 and -2 and Fa390/9-1 and -2) focused on the attractors of the peripheral region for early settlers, the pedological conditions before land use, but also the impact of humans on soils and karst dynamics through time. In the course of the in hand study, the pedosedimentary archives have been approached with a multimethodological toolset which consisted of field analyses, soil morphological analyses from micro- to macro-scale, spectrophotometric (color), (laser) granulometric, and (iron-) pedochemical analyses. The numerical chronological frame was spanned by radiocarbon dating of different organic remains and bulk material if soil organic carbon was supposed-ly high. The result is a multi-dimensional data set that consists of analyses on different spatial scales but also on different levels of measurement. Thus, qualitative, semi-quantitative, and quantitative data consti-tute the basis for discussion. While the grain-size analyses underline the general sedimentological differen-tiation of the records and further affirm the high clay content within the pedosedimentary layers, iron-pedochemical analyses indicate an interplay between oxidation of iron and its chemical reduction. This is also manifested within the spectrophotometric record. Especially the versatile pedogenic characteristics that have been identified by field analyses are confirmed within the thin sections and, by considering all different analyses, the polygenic character of the pedosediments is emphasized.
After stressing the general pedological specificities among the different investigated sites within the re-search area, for the collected data, the research further branches into the subjects of general notions on pedogenesis in clayey material and the classification of the respective pedosediments according to paleo-pedological concepts but also recent schemes. Concerning the latter, it becomes evident that established principles cannot be applied to the studied pedosediments without major adaptions. This underlines the specific characteristics of the material.
The basis for further interpretations is the evaluation of the multi-level data set for the single records with regard to profile development and pedogenic processes. Hereby, the main drivers of pedogenesis could be identified, which are karst dynamics, land use, and subtle changes in parent material due to the admixture of slope deposits that contain allochthonous eolian material. The latter underlines the importance of Pleis-tocene preconditioning for understanding Holocene landscape dynamics. At the same time, a differentia-tion between the mentioned factors and Holocene climate development is difficult. The following compila-tion of record and localities within the given time frame unveils synchronous as well as asynchronous de-velopments; however, a clear connection between phases of Holocene climate and pedogenesis within the pedosediments cannot be established. Instead, it becomes evident that site specific factors or those that act on the scale of the micro-catchment of the investigated records are decisive.
The aforementioned main topics of the project are also considered in the in hand study from a soil-geographic perspective: it is possible that before land use, there was an insular or thin cover by loess sedi-ments or at least upper layers (according to the concept of periglacial cover beds) which constituted the parent material for Holocene soil formation. The according soils, which were superior for agricultural purposes compared to those developed on the autochthonous mudstones, were eroded which exposed the clayey Upper to Middle Triassic beds. Erosion was aggravated due to the impermeable mudstones which enhanced overland flow and interflow within the overlying silty (loessic) material. This is further support-ed by the notions on erodibility of the clayey material that are derived from the comparison of conven-tional and laser granulometric analyses: probably, the clayey pedosediments are capable of forming micro-aggregates that can easily be eroded during heavy rainfall events despite the general consent that material with heavy texture should be rather resistant.
The study presents a comprehensive view on clay-rich pedosediments and the complex effects of human-environment interaction on pedogenic as well as sedimentary processes through time that have not been investigated in such detail before. In this context, the multi-level soil morphological analyses and their necessity for a genetic interpretation with regard to the influence of natural versus anthropogenic factors need to be emphasized. Based on quantitative laboratory analytical data only, a respective differentiation would not be possible. This underlines the importance of the chosen soil-geographic multi-methodological approach for answering questions with regard to human-environment interaction but also geoarcheology in general.
Glycine receptor β–targeting autoantibodies contribute to the pathology of autoimmune diseases
(2024)
Background and Objectives
Stiff-person syndrome (SPS) and progressive encephalomyelitis with rigidity and myoclonus (PERM) are rare neurologic disorders of the CNS. Until now, exclusive GlyRα subunit–binding autoantibodies with subsequent changes in function and surface numbers were reported. GlyR autoantibodies have also been described in patients with focal epilepsy. Autoimmune reactivity against the GlyRβ subunits has not yet been shown. Autoantibodies against GlyRα1 target the large extracellular N-terminal domain. This domain shares a high degree of sequence homology with GlyRβ making it not unlikely that GlyRβ-specific autoantibody (aAb) exist and contribute to the disease pathology.
Methods
In this study, we investigated serum samples from 58 patients for aAb specifically detecting GlyRβ. Studies in microarray format, cell-based assays, and primary spinal cord neurons and spinal cord tissue immunohistochemistry were performed to determine specific GlyRβ binding and define aAb binding to distinct protein regions. Preadsorption approaches of aAbs using living cells and the purified extracellular receptor domain were further used. Finally, functional consequences for inhibitory neurotransmission upon GlyRβ aAb binding were resolved by whole-cell patch-clamp recordings.
Results
Among 58 samples investigated, cell-based assays, tissue analysis, and preadsorption approaches revealed 2 patients with high specificity for GlyRβ aAb. Quantitative protein cluster analysis demonstrated aAb binding to synaptic GlyRβ colocalized with the scaffold protein gephyrin independent of the presence of GlyRα1. At the functional level, binding of GlyRβ aAb from both patients to its target impair glycine efficacy.
Discussion
Our study establishes GlyRβ as novel target of aAb in patients with SPS/PERM. In contrast to exclusively GlyRα1-positive sera, which alter glycine potency, aAbs against GlyRβ impair receptor efficacy for the neurotransmitter glycine. Imaging and functional analyses showed that GlyRβ aAbs antagonize inhibitory neurotransmission by affecting receptor function rather than localization.
Highlights
• The GLA variant S126G is not associated with Fabry symptoms in the presented case
• S126G has no effect on α-GAL A activity or Gb3 levels in this patient
• S126G sensory neurons show no electrophysiological abnormalities
Abstract
Fabry disease (FD) is a life-limiting disorder characterized by intracellular globotriaosylceramide (Gb3) accumulations. The underlying α-galactosidase A (α-GAL A) deficiency is caused by variants in the gene GLA. Variants of unknown significance (VUS) are frequently found in GLA and challenge clinical management. Here, we investigated a 49-year old man with cryptogenic lacunar cerebral stroke and the chance finding of the VUS S126G, who was sent to our center for diagnosis and initiation of a costly and life-long FD-specific treatment. We combined clinical examination with in vitro investigations of dermal fibroblasts (HDF), induced pluripotent stem cells (iPSC), and iPSC-derived sensory neurons. We analyzed α-GAL A activity in iPSC, Gb3 accumulation in all three cell types, and action potential firing in sensory neurons. Neurological examination and small nerve fiber assessment was normal except for reduced distal skin innervation. S126G iPSC showed normal α-GAL A activity compared to controls and no Gb3 deposits were found in all three cell types. Baseline electrophysiological characteristics of S126G neurons showed no difference compared to healthy controls as investigated by patch-clamp recordings. We pioneer multi-level cellular characterization of the VUS S126G using three cell types derived from a patient and provide further evidence for the benign nature of S126G in GLA, which is of great importance in the management of such cases in clinical practice.