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Die Dissertation ,Spuren des Religiösen´ im Werk der deutsch-jüdischen Schriftstellerin Barbara Honigmann – eine literaturwissenschaftlich-theologische Werkanalyse – analysiert und interpretiert das literarische Frühwerk der deutsch-jüdischen Schriftstellerin Barbara Honigmann (geb. 12. Februar 1949 in Ostberlin). Die Schriftstellerin verlässt Mitte der achtziger Jahre mit ihrer Familie die ehemalige DDR und findet in Straßburg (Frankreich) eine neue Heimat. In der Dissertation werden der Erzählband Roman von einem Kinde (1986) und die Romane Eine Liebe aus nichts (1991) und Soharas Reise (1996) aus der Sicht verschiedener Fachwissenschaften beleuchtet. Die meisten Texte sind nach ihrer Emigration in Frankreich entstanden. Methodisch werden die Texte nach der Erzähltextanalyse von Sönke Finnern analysiert. Das Judentum und jüdische Religiosität bilden dabei das gemeinsame Zentrum der literarischen Werke Barbara Honigmanns (Hans Otto Horch). In differenzierter Weise werden unterschiedliche jüdisch-theologische Aspekte wie Gottesfrage, Bedeutung der jüdischen Feste, Riten und Exilerfahrung anhand der Werke herausgearbeitet. Aus literaturwissenschaftlicher Sicht wird der Aspekt des exterritorialen Schreibens betont (Andreas Kilcher). Dabei wird die besondere Perspektive als Autorin der sogenannten zweiten Generation nach der Shoah hervorgehoben (Hartmut Steinecke). Georg Langenhorst macht auf die Bedeutung Honigmanns im Kontext des religionspädagogischen Diskurses unter interkultureller und interreligiöser Fragestellung aufmerksam. Die Erzählte Religion bildet das Zentrum der literarisch-theologischen Werkanalyse. Die Kategorie der Grenzerfahrung bzw. der Liminalität rückt dabei in das Zentrum der Verhältnisbestimmung (Victor Turner und Dirk Hohnsträter). Auf der theologischen Ebene werden die jüdischen Konzepte von makom (hebr. Ort), galut (hebr. Exil) und jetzirat (hebr. Schöpfung) herausgearbeitet. Die jüdische Erfahrung von Heimat und Heimatlosigkeit wird hervorgehoben (Yannif Feller). Die Arbeit schließt mit einer Einordnung der Werkinterpretation in den Bereich Literatur und Ritual (Wolfgang Braungart).
Growth, ageing and atherosclerotic plaque development alter the biomechanical forces acting on the vessel wall. However, monitoring the detailed local changes in wall shear stress (WSS) at distinct sites of the murine aortic arch over time has been challenging. Here, we studied the temporal and spatial changes in flow, WSS, oscillatory shear index (OSI) and elastic properties of healthy wildtype (WT, n = 5) and atherosclerotic apolipoprotein E-deficient (Apoe−/−, n = 6) mice during ageing and atherosclerosis using high-resolution 4D flow magnetic resonance imaging (MRI). Spatially resolved 2D projection maps of WSS and OSI of the complete aortic arch were generated, allowing the pixel-wise statistical analysis of inter- and intragroup hemodynamic changes over time and local correlations between WSS, pulse wave velocity (PWV), plaque and vessel wall characteristics. The study revealed converse differences of local hemodynamic profiles in healthy WT and atherosclerotic Apoe−/− mice, and we identified the circumferential WSS as potential marker of plaque size and composition in advanced atherosclerosis and the radial strain as a potential marker for vascular elasticity. Two-dimensional (2D) projection maps of WSS and OSI, including statistical analysis provide a powerful tool to monitor local aortic hemodynamics during ageing and atherosclerosis. The correlation of spatially resolved hemodynamics and plaque characteristics could significantly improve our understanding of the impact of hemodynamics on atherosclerosis, which may be key to understand plaque progression towards vulnerability.
Abstract
Amphidiploid fungal Verticillium longisporum strains Vl43 and Vl32 colonize the plant host Brassica napus but differ in their ability to cause disease symptoms. These strains represent two V. longisporum lineages derived from different hybridization events of haploid parental Verticillium strains. Vl32 and Vl43 carry same‐sex mating‐type genes derived from both parental lineages. Vl32 and Vl43 similarly colonize and penetrate plant roots, but asymptomatic Vl32 proliferation in planta is lower than virulent Vl43. The highly conserved Vl43 and Vl32 genomes include less than 1% unique genes, and the karyotypes of 15 or 16 chromosomes display changed genetic synteny due to substantial genomic reshuffling. A 20 kb Vl43 lineage‐specific (LS) region apparently originating from the Verticillium dahliae‐related ancestor is specific for symptomatic Vl43 and encodes seven genes, including two putative transcription factors. Either partial or complete deletion of this LS region in Vl43 did not reduce virulence but led to induction of even more severe disease symptoms in rapeseed. This suggests that the LS insertion in the genome of symptomatic V. longisporum Vl43 mediates virulence‐reducing functions, limits damage on the host plant, and therefore tames Vl43 from being even more virulent.
A Brief History of APIs
(2021)
Online platforms such as Facebook, YouTube and Twitter offer a wide range of data for scientific research. Since many of the social media providers have set up application programming interfaces (APIs), extensive volumes of data can be collected automatically (Jünger, 2018; Keyling & Jünger, 2016). Social media data are attractive, inter alia, because they not only include already available communication, such as that from public media, but they also make organisational and interpersonal communication visible (Ledford, 2020). In addition, these data are process-generated (Baur, 2011, p. 1234), meaning that they are generated independently of scientific research and thus promise an authentic insight into human behaviour. 1 A wide range of studies in the social sciences exploit APIs for data collection and analysis. Thus, the establishment and development of APIs has significant implications for science.
Our goal was to provide a comprehensive overview of the antibody response to Staphylococcus aureus antigens in the general population as a basis for defining disease-specific profiles and diagnostic signatures. We tested the specific IgG and IgA responses to 79 staphylococcal antigens in 996 individuals from the population-based Study of Health in Pomerania. Using a dilution-based multiplex suspension array, we extended the dynamic range of specific antibody detection to seven orders of magnitude, allowing the precise quantification of high and low abundant antibody specificities in the same sample. The observed IgG and IgA antibody responses were highly heterogeneous with differences between individuals as well as between bacterial antigens that spanned several orders of magnitude. Some antigens elicited significantly more IgG than IgA and vice versa. We confirmed a strong influence of colonization on the antibody response and quantified the influence of sex, smoking, age, body mass index, and serum glucose on anti-staphylococcal IgG and IgA. However, all host parameters tested explain only a small part of the extensive variability in individual response to the different antigens of S. aureus.
A lot of research data has become available since the outbreak of the COVID-19
pandemic in 2019. Connecting this data is essential for the understanding of the
SARS-CoV-2 virus and the fight against the pandemic.
Amongst biological and biomedical research data, computational models targeting
COVID-19 have been emerging and their number is growing constantly. They are a
central part of the field of Systems Biology, which aims to understand the mechanisms
and behaviour of biological systems. Model predictions help to understand the
mechanisms of the novel coronavirus and the life-threatening disease it is causing.
Both biomedical research data and modelling data regarding COVID-19 have
previously been stored in separated domain-specific graph databases. MaSyMoS,
short for Management System for Models and Simulations, is a graph database for
storing simulation studies of biological and biochemical systems. The CovidGraph
project integrates research data regarding COVID-19 and the coronavirus family
from various data resources in a knowledge graph.
In this thesis, we integrate simulation models from MaSyMoS, including models
targeting COVID-19, into the CovidGraph. Therefore, we present a concept for
the integration of simulation studies and the linkage through ontology terms and
reference publications in the CovidGraph. Ultimately, we connect data from the field
of systems biology and biomedical research data in a graph database.
Background: Previous studies suggest that blood donation impacts blood donors’ psychological state, with either positive or negative effects, such as feeling more energetic or more exhausted. It has not yet been described how long these effects last. Materials and Methods: This prospective cohort study consisted of a qualitative and a quantitative part: (1) Psychological characteristics which changed after blood donation were identified by structured interviews of regular whole blood donors (n = 42). Based on this, a questionnaire addressing 7 psychological dimensions was established. (2) The psychological state of 100 blood donors was assessed after blood donation by applying the questionnaire 15–30 min before and during donation, as well as 15–30 min, 6 h, 24 h, 72 h, 1 week, and 8 weeks after donation. The resulting changes were summarized to a score. Furthermore, potential correlations of the score with pre-donation blood pressure, hemoglobin, or body mass index were calculated. Results: Seven items were identified which changed in at least 25% of blood donors (mood, concentration, satisfaction, resilience, spirit of initiative, physical well-being, energy level). In the 100 blood donors, the well-being score increased (positive effects, n = 23), showed minor changes (n = 53), or decreased (negative effects, n = 24). The positive effects lasted for about 1 week and the negative effects for 3 days. Conclusion: While the frequency of psychological effects following blood donation identified by our study was comparable to others, the changes of the psychological state in our donors were traceable for a longer period than previously acknowledged.
We introduce PVSC-DTM (Parallel Vectorized Stencil Code for Dirac and Topological Materials), a library and code generator based on a domain-specific language tailored to implement the specific stencil-like algorithms that can describe Dirac and topological materials such as graphene and topological insulators in a matrix-free way. The generated hybrid-parallel (MPI+OpenMP) code is fully vectorized using Single Instruction Multiple Data (SIMD) extensions. It is significantly faster than matrix-based approaches on the node level and performs in accordance with the roofline model. We demonstrate the chip-level performance and distributed-memory scalability of basic building blocks such as sparse matrix-(multiple-) vector multiplication on modern multicore CPUs. As an application example, we use the PVSC-DTM scheme to (i) explore the scattering of a Dirac wave on an array of gate-defined quantum dots, to (ii) calculate a bunch of interior eigenvalues for strong topological insulators, and to (iii) discuss the photoemission spectra of a disordered Weyl semimetal.
Abstract
Background
Twenty five‐hydroxy vitamin D (25OHD) levels have been proposed to protect against periodontitis based on in vitro and observational studies but evidence from long‐term randomized controlled trials (RCTs) is lacking. This study tested whether genetically proxied 25OHD is associated with periodontitis using Mendelian randomization (MR).
Methods
Genetic variants strongly associated with 25OHD in a genome‐wide association study (GWAS) of 417,580 participants of European ancestry were used as instrumental variables, and linked to GWAS summary data of 17,353 periodontitis cases and 28,210 controls. In addition to the main analysis using an inverse variance weighted (IVW) model, we applied additional robust methods to control for pleiotropy. We also undertook sensitivity analyses excluding single nucleotide polymorphisms (SNPs) used as instruments with potential pleiotropic effects and used a second 25OHD GWAS for replication. We identified 288 SNPs to be genome‐wide significant for 25OHD, explaining 7.0% of the variance of 25OHD levels and providing ≥90% power to detect an odds ratio (OR) of ≤ 0.97.
Results
MR analysis suggested that a 1 standard deviation increase in natural log‐transformed 25OHD was not associated with periodontitis risk (IVW OR = 1.04; 95% confidence interval (CI): 0.97–1.12; P‐value = 0.297). The robust models, replication, and sensitivity analyses were coherent with the primary analysis.
Conclusions
Collectively, our findings suggest that 25OHD levels are unlikely to have a substantial effect on the risk of periodontitis, but large long‐term RCTs are needed to derive definitive evidence on the causal role of 25OHD in periodontitis.
Terrestrial surface waters and submarine ground water discharge (SGD) act as a source of dissolved substances for coastal systems. Solute fluxes of SGD depend on the ground water composition and the water-solid-microbe interactions close to the sediment-water interface. Thus, this study aims to characterize and evaluate the hydrogeochemical gradients developing in the fresh-salt water mixing zone of the Wismar Bay (WB), southern Baltic Sea, Germany. Sampling campaigns covering the WB, the fresh-salt water mixing zone at the beach of the WB shoreline, terrestrial surface and ground waters near the WB as well sediments pore water were carried out. In these different waters, the distribution of dissolved inorganic carbon, nutrients, major ions, trace elements, stable isotopes (H, O, C, S), and radium isotopes have been investigated. Enhanced concentrations of radium isotopes together with dissolved manganese, barium in the surface waters of the eastern WB indicated benthic-pelagic coupling via the exchange between pore water and the water column. Salinity, stable isotopes, and major ions in sediment pore water profiles identified the presence of fresh ground water below about 40 cmbsf in the central part of the bay. Geophysical acoustic techniques revealed the local impact of anthropogenic sediment excavation, which reduced the thickness of a sediment layer between the coastal aquifer and the bottom water, causing, therefore, a ground water upward flow close to the top sediments. The fresh impacted pore water stable isotope composition (δ18O, δ2H) plot close to the regional meteoric water line indicating a relatively modern ground water source. The calculated organic matter mineralization rates and the dissolved inorganic carbon sediment-water fluxes were much higher at the fresh impacted site when compared to other unimpacted sediments. Therefore, this study reveals that different fresh water sources contribute to the water balance of WB including a SGD source.
The human pathogen Clostridioides difficile has evolved into the leading cause of nosocomial diarrhea. The bacterium is capable of spore formation, which even allows survival of antibiotic treatment. Although C. difficile features an anaerobic lifestyle, we determined a remarkably high oxygen tolerance of the laboratory reference strain 630Δerm. A mutation of a single nucleotide (single nucleotide polymorphism [SNP]) in the DNA sequence (A to G) of the gene encoding the regulatory protein PerR results in an amino acid substitution (Thr to Ala) in one of the helices of the helix-turn-helix DNA binding domain of this transcriptional repressor in C. difficile 630Δerm. PerR is a sensor protein for hydrogen peroxide and controls the expression of genes involved in the oxidative stress response. We show that PerR of C. difficile 630Δerm has lost its ability to bind the promoter region of PerR-controlled genes. This results in a constitutive derepression of genes encoding oxidative stress proteins such as a rubrerythrin (rbr1) whose mRNA abundance under anaerobic conditions was increased by a factor of about 7 compared to its parental strain C. difficile 630. Rubrerythrin repression in strain 630Δerm could be restored by the introduction of PerR from strain 630. The permanent oxidative stress response of C. difficile 630Δerm observed here should be considered in physiological and pathophysiological investigations based on this widely used model strain.
IMPORTANCE The intestinal pathogen Clostridioides difficile is one of the major challenges in medical facilities nowadays. In order to better combat the bacterium, detailed knowledge of its physiology is mandatory. C. difficile strain 630Δerm was generated in a laboratory from the patient-isolated strain C. difficile 630 and represents a reference strain for many researchers in the field, serving as the basis for the construction of insertional gene knockout mutants. In our work, we demonstrate that this strain is characterized by an uncontrolled oxidative stress response as a result of a single-base-pair substitution in the sequence of a transcriptional regulator. C. difficile researchers working with model strain 630Δerm should be aware of this permanent stress response.
AbstractThe performance of a positively biased external ring anode in combination with a hollow cathode (HC) discharge or a magnetron sputtering (MS) discharge, both with a Ti cathode and with Ar as working gas, is investigated. Plasma and floating potential increase as function of anode voltage. Energy-resolved mass spectrometry reveals that the kinetic energy of argon and titanium ions is enhanced by a positive anode voltage allowing for an effective energy control of plasma ions.
Abstract
Individuals of the marine chelicerate lineage Pycnogonida (sea spiders) show considerable regenerative capabilities after appendage injury or loss. In their natural habitats, especially the long legs of sea spiders are commonly lost and regenerated, as is evidenced by the frequent encounter of specimens with missing or miniature legs. In contrast to this, the collection of individuals with abnormally developed appendages or trunk regions is comparably rare. Here, we studied a remarkable malformation in a postlarval instar of the species Phoxichilidium femoratum (Rathke, 1799) and describe the external morphology and internal organization of the specimen using a combination of fluorescent histochemistry and scanning electron microscopy. The individual completely lacks the last trunk segment with leg pair 4 and the normally penultimate trunk segment bears only a single aberrant appendage resembling an extension of the anteroposterior body axis. Externally, the proximal units of the articulated appendage are unpaired, but further distally a bifurcation into two equally developed leg‐like branches is found. Three‐dimensional reconstruction of the musculature reveals components of two regular leg muscle sets in several of the proximal articles. This confirms interpretation of the entire appendage as a malformed leg and reveals an externally hidden paired organization along its entire proximodistal axis. To explain the origin of this unique malformation, early pioneering studies on the regenerative potential of pycnogonids are evaluated and (a) an injury‐induced partial fusion of the developing limb buds of leg pair 3, as well as (b) irregular leg regeneration following near complete loss of trunk segments 3 and 4 are discussed. Which of the two hypotheses is more realistic remains to be tested by dedicated experimental approaches. These will have to rely on pycnogonid species with established laboratory husbandry in order to overcome the limitations of the few short‐term regeneration studies performed to date.
The Madden-Julian Oscillation (MJO) is a prominent feature of the intraseasonal variability of the atmosphere. The MJO strongly modulates tropical precipitation and has implications around the globe for weather, climate and basic atmospheric research. The time-dependent state of the MJO is described by MJO indices, which are calculated through sometimes complicated statistical approaches from meteorological variables. One of these indices is the OLR-based MJO Index (OMI; OLR stands for outgoing longwave radiation). The Python package mjoindices, which is described in this paper, provides the first open source implementation of the OMI algorithm, to our knowledge. The package meets state-of-the-art criteria for sustainable research software, like automated tests and a persistent archiving to aid the reproducibility of scientific results. The agreement of the OMI values calculated with this package and the original OMI values is also summarized here. There are several reuse scenarios; the most probable one is MJO-related research based on atmospheric models, since the index values have to be recalculated for each model run.
We decided to develop a short-form of the CHC-SUN/YHC-SUN, a questionnaire aiming at assessing health care satisfaction of children and adolescents with chronic health conditions. Data analysis was based on samples from three different studies. Item selection involved statistical analysis and expert consensus. For independent validation purposes, we calculated descriptive statistics on single-item and composite-scale levels and applied classic test theory, confirmatory factor analyses, and correlation analysis to investigate the psychometric properties of the final short-form by different types of reliability and validity. Internal consistency (Cronbach’s Alpha) reached values of a = 0.89 (self-report) and a = 0.92 (parents report), split-half reliability values reached 0.85 (self-report) and 0.91 (parents report). Confirmatory factor analysis indicated no sufficient fit for the single factor solution, whereas the solution with three factors and one higher order factor indicated the best overall fit amongst three competing models. Validity of the short-form measure can be assumed, e.g., as indicated by its association with a single-item measure on general health care satisfaction. The short-form measures of the CHC-SUN for parents (CHC-SUN-SF) and the YHC-SUN self-report version for adolescents (YHC-SUN-SF) feature excellent psychometric performances, provide economical assessments, and are easy-to-administer questionnaires. They should be used whenever brief measures are needed for economic reasons.
The function and mode of action of small regulatory RNAs is currently still understudied in archaea. In the halophilic archaeon Haloferax volcanii, a plethora of sRNAs have been identified; however, in-depth functional analysis is missing for most of them. We selected a small RNA (s479) from Haloferax volcanii for detailed characterization. The sRNA gene is encoded between a CRISPR RNA locus and the Cas protein gene cluster, and the s479 deletion strain is viable and was characterized in detail. Transcriptome studies of wild-type Haloferax cells and the deletion mutant revealed upregulation of six genes in the deletion strain, showing that this sRNA has a clearly defined function. Three of the six upregulated genes encode potential zinc transporter proteins (ZnuA1, ZnuB1, and ZnuC1) suggesting the involvement of s479 in the regulation of zinc transport. Upregulation of these genes in the deletion strain was confirmed by northern blot and proteome analyses. Furthermore, electrophoretic mobility shift assays demonstrate a direct interaction of s479 with the target znuC1 mRNA. Proteome comparison of wild-type and deletion strains further expanded the regulon of s479 deeply rooting this sRNA within the metabolism of H. volcanii especially the regulation of transporter abundance. Interestingly, s479 is not only encoded next to CRISPR–cas genes, but the mature s479 contains a crRNA-like 5′ handle, and experiments with Cas protein deletion strains indicate maturation by Cas6 and interaction with Cas proteins. Together, this might suggest that the CRISPR–Cas system is involved in s479 function.
Subterranean estuaries the, subsurface mixing zones of terrestrial groundwater and seawater, substantially influence solute fluxes to the oceans. Solutes brought by groundwater from land and solutes brought from the sea can undergo biogeochemical reactions. These are often mediated by microbes and controlled by reactions with coastal sediments, and determine the composition of fluids discharging from STEs (i.e., submarine groundwater discharge), which may have consequences showing in coastal ecosystems. While at the local scale (meters), processes have been intensively studied, the impact of subterranean estuary processes on solute fluxes to the coastal ocean remains poorly constrained at the regional scale (kilometers). In the present communication, we review the processes that occur in STEs, focusing mainly on fluid flow and biogeochemical transformations of nitrogen, phosphorus, carbon, sulfur and trace metals. We highlight the spatio-temporal dynamics and measurable manifestations of those processes. The objective of this contribution is to provide a perspective on how tracer studies, geophysical methods, remote sensing and hydrogeological modeling could exploit such manifestations to estimate the regional-scale impact of processes in STEs on solute fluxes to the coastal ocean.
The ubiquitin-proteasome system (UPS) and the autophagy-lysosomal pathway (ALP) are the main proteolytic systems involved in cellular homeostasis. Since cardiomyocytes, as terminally differentiated cells, lack the ability to share damaged proteins with their daughter cells, they are especially reliant on these protein degradation systems for their proper function. Alterations of the UPS and ALP have been reported in a wide range of cardiac diseases, including cardiomyopathies. In this study, we determined whether the UPS and ALP are altered in a mouse model of eccentric left ventricular (LV) hypertrophy expressing both cyclin T1 and Gαq under the control of the cardiac-specific α-myosin heavy chain promoter (double transgenic; DTG). Compared to wild-type (WT) littermates, DTG mice showed higher end-diastolic (ED) LV wall thicknesses and diameter with preserved ejection fraction (EF). The cardiomyopathic phenotype was further confirmed by an upregulation of the fetal gene program and genes associated with fibrosis as well as a downregulation of genes involved in Ca2+ handling. Likewise, higher NT-proBNP levels were detected in DTG mice. Investigation of the UPS showed elevated steady-state levels of (poly)ubiquitinated proteins without alterations of all proteasomal activities in DTG mice. Evaluation of ALP key marker revealed a mixed pattern with higher protein levels of microtubule-associated protein 1 light chain 3 beta (LC3)-I and lysosomal-associated membrane protein-2, lower protein levels of beclin-1 and FYVE and coiled-coil domain-containing protein 1 (FYCO1) and unchanged protein levels of p62/SQSTM1 in DTG mice when compared to WT. At transcriptional level, a > 1.2-fold expression was observed for Erbb2, Hdac6, Lamp2, Nrg1, and Sqstm1, while a < 0.8-fold expression was revealed for Fyco1 in DTG mice. The results related to the ALP suggested overall a repression of the ALP during the initiation process, but an induction of the ALP at the level of autophagosome-lysosome fusion and the delivery of ubiquitinated cargo to the ALP for degradation.
RationaleThe ubiquitin–proteasome system (UPS) is responsible for skeletal muscle atrophy. We showed earlier that the transcription factor EB (TFEB) plays a role by increasing E3 ubiquitin ligase muscle really interesting new gene-finger 1(MuRF1)/tripartite motif-containing 63 (TRIM63) expression. MuRF 1 ubiquitinates structural proteins and mediates their UPS-dependent degradation. We now investigated how TFEB-mediated TRIM63 expression is regulated.
ObjectiveBecause protein kinase D1 (PKD1), histone deacetylase 5 (HDAC5), and TFEB belong to respective families with close structural, regulatory, and functional properties, we hypothesized that these families comprise a network regulating TRIM63 expression.
Methods and ResultsWe found that TFEB and transcription factor for immunoglobulin heavy-chain enhancer 3 (TFE3) activate TRIM63 expression. The class IIa HDACs HDAC4, HDAC5, and HDAC7 inhibited this activity. Furthermore, we could map the HDAC5 and TFE3 physical interaction. PKD1, PKD2, and PKD3 reversed the inhibitory effect of all tested class IIa HDACs toward TFEB and TFE3. PKD1 mediated nuclear export of all HDACs and lifted TFEB and TFE3 repression. We also mapped the PKD2 and HDAC5 interaction. We found that the inhibitory effect of PKD1 and PKD2 toward HDAC4, HDAC5, and HDAC7 was mediated by their phosphorylation and 14-3-3 mediated nuclear export.
ConclusionTFEB and TFE3 activate TRIM63 expression. Both transcription factors are controlled by HDAC4, HDAC5, HDAC7, and all PKD-family members. We propose that the multilevel PKD/HDAC/TFEB/TFE3 network tightly controls TRIM63 expression.
BACKGROUND Acute disseminated encephalomyelitis (ADEM) is a rare, acquired demyelination syndrome that causes cognitive impairment and
focal neurological deficits and may be fatal. The potentially reversible disease mainly affects children, often after vaccination or viral infection, but may
be seen rarely in adults.
OBSERVATIONS A 50-year-old woman presented with loss of visual acuity of the left eye. Magnetic resonance imaging (MRI) revealed an intra- and
suprasellar mass, which was removed successfully. On postoperative day 1, MRI showed gross total resection of the lesion and no surgery-related
complications. On postoperative day 2, the patient presented with a progressive left-sided hemiparesis, hemineglect, and decline of cognitive
performance. MRI showed white matter edema in both hemispheres. Cerebrospinal fluid analysis revealed mixed pleocytosis (355/mL) without further
evidence of infection. In synopsis of the findings, ADEM was diagnosed and treated with intravenous immunoglobulins. Shortly thereafter, the patient
recovered, and no sensorimotor deficits were detected in the follow-up examination.
LESSONS Pituitary gland pathologies are commonly treated by transsphenoidal surgery, with only minor risks for complications. A case of ADEM after
craniopharyngioma resection has not been published before and should be considered in case of progressive neurological deterioration with multiple
white matter lesions.
Summary
The article discusses Adam Naruszewicz‘s famous Ode to Justice (1773) and the engagement of occasional poetry in contemporary discussions about the handling of justice in political trials. Looking at the trial of 1773 the Ode addresses the question of finding a just sentence for the abortive attempt two years earlier to abduct king Stanisław August. The article presents the pertinent aspects for such an analysis in three parts: 1) an introduction to the conceptualization of royal justice in European thought of the Enlightenment, 2) the known facts about the abduction and its historical contexts, 3) an overview of the occasional poetry written by Naruszewicz about the incident from 1771 to 1773 leading to an analysis of the Ode to Justice in regard to the political reasoning of its author.
Adaptation mechanisms within the B cell composition for successful human and murine pregnancies.
(2021)
Introduction
A well-balanced immune maternal status is essential for favourable outcome of pregnancy. Due to their complexities, not all immune adaptations that promote tolerance during pregnancy are known. To understand the adaptation of the B cell compartment, we analysed and compared B cell lymphopoiesis in different lymphoid tissues in a number of murine models.
Furthermore, we focused on the humoral immune response during pregnancy. We analysed immunoglobulin profiles in human subjects and mice during pregnancy.
These cellular alterations are subject to the influence of chemokines, among others. Therefore, we assessed serum levels of B cell activation factor to clarify its effects during pregnancy.
Methods
For analysis of the human peripheral B cell compartment, peripheral blood samples from age-matched non-pregnant and pregnant women without pregnancy complications, immunological disease or acute/chronic inflammation were collected and sub-classified into four different groups: non-pregnant, and first, second, or third trimester of pregnancy. The experiments, based on a mouse model, were performed with 8-week-old female mice: clinically healthy non-pregnant (CBA/J (H2k)), pregnant mice with normal gestation (BALB/c (H2d) x CBA/J (H2k)), and mice with pregnancy loss (DBA/2J (H2d) x CBA/J (H2k)). Subsequently, peripheral blood mononuclear cells from blood and lymphatic organs were isolated following standard protocols. The B cell analysis was performed by flow cytometry. The immunoglobulin serum levels of the human and murine subgroups were quantitated using Bio-Plex isotyping assay and analysed by a Bio-Plex reader. To quantify B cell activating factor (BAFF) in serum of pregnant and non-pregnant mice a BAFF enzyme-linked immunosorbent assay was used. The concentrations were determined by using a FLUOstar OPTIMA microplate reader. All statistical analyses were performed using the Kruskal–Wallis test with Dunn’s post-test in GraphPad Prism software. P values of < 0.05 were considered statistically significant.
Results
We were able to demonstrate B cell lymphopenia in mice bone marrow downstream of pre-pro B cells, irrespective of pregnancy outcome. The mature bone marrow B cells did not show this adjustment mechanism during normal gestation.
Closer inspection of the splenic tissue revealed expansion and activation of marginal zone B cells in mice with a normal pregnancy. However, this was not observed in mice suffering from pregnancy disturbances. Natural antibodies secreted from marginal zone B cells were also present at higher concentrations in serum of pregnant mice, compared to non-pregnant animals.
We also found significantly higher levels of natural antibodies in serum of pregnant women compared to non-pregnant age-matched controls. Analysis showed significantly lower levels of BAFF in mice with normal pregnancy as compared to non-pregnant mice.
Conclusions
We are able to show mechanisms within the B cell compartment as well as the change within the natural antibodies that might be crucial for successful pregnancy in both humans and mice. Furthermore, BAFF seems to play a central role as a mediator of peripheral B cell compartment and B cell lymphopoiesis in the bone marrow for successful pregnancy.
Rewetting is the most effective way to reduce greenhouse gas (GHG) emissions from drained peatlands and must significantly contribute to the implementation of the Paris Agreement on Climate within the land sector. In 2010–2013, more than 73 thousand hectares of fire-prone peatlands were rewetted in the Moscow Region (the hitherto largest rewetting program in the Northern Hemisphere). As the Russian Federation has no national accounting of rewetted areas yet, this paper presents an approach to detect them based on multispectral satellite data verified by ground truthing. We propose that effectively rewetted areas should minimally include areas with wet grasslands and those covered with water (cf. the IPCC categories “rewetted organic soils” and “flooded lands”). In 2020, these lands amounted in Moscow Region to more than 5.3 and 3.6 thousand hectares, respectively. Assuming that most rewetted areas were former peat extraction sites and using IPCC default GHG emission factors, an overall GHG emission reduction of over 36,000 tCO2-eq year−1 was calculated. We furthermore considered the uncertainty of calculations. With the example of a 1535 ha large rewetted peatland, we illustrate the estimation of GHG emission reductions for the period up to 2050. The approach presented can be used to estimate GHG emission reductions by peatland rewetting on the national, regional, and object level.
Ziel:
Diese populationsbasierte Studie untersucht sowohl die Prävalenz adipöser Schwangerer und deren Geburtsoutcome als auch den Einfluss der Adipositas auf das Outcome des Neugeborenen. Sie beschreibt die Bedeutung der Gewichtsentwicklung in der Schwangerschaft für Mutter und Kind.
Material/Methode:
Insgesamt wurden n=4593 Mütter und ihre Kinder in der populationsbasierten SNiP Studie, Survey of Neonates in Pomerania untersucht. Die Datenerhebung erfolgte im Zeitraum von März 2003 bis November 2008 in Universitäts- und Kreiskrankenhäusern im Nordosten von Mecklenburg-Vorpommern nach standardisierten Fragebögen, Erhebung von Laborparametern und klinischer Dokumentationen. Zur Beurteilung der Schwangerschaftskomplikationen und des Schwangerschaftsausganges wurden die Schwangeren in einzelne BMI Gruppen eingeteilt. Die individuelle Gewichtzunahme wurde ermittelt. Als Outcomeparameter wurden prä- und perinatale Erkrankungen, Pathologien und Risiken bei der Schwangeren und dem Neugeborenen ermittelt und ausgewertet. Hierbei wurden auch sozioökonomischen Faktoren erhoben und ausgewertet.
Ergebnis:
Adipositas ist eine Volkskrankheit. Die mit dieser Volkskrankheit im Zusammenhang stehenden gesundheitlichen Risiken treten nicht nur im Alter auf, sondern es entstehen auch zunehmend Gefährdungen junger Menschen. Hier sind besonders schwangere Frauen mit ihren Neugeborenen betroffen. Mehr als ¼ der schwangeren Frauen im Studiengebiet OVP sind präadipös (BMI 25-29,9) oder adipös (BMI ≥ 30).
Adipöse Schwangere finden sich dem weltweiten Trend entsprechend in der unteren sozialen Bevölkerungsschicht.
Eine Adipositas der Mutter beinhaltet Risiken für Mutter und Kind. Das Risiko einer adipösen Mutter (BMI ≥ 30) an einem Gestationsdiabetes zu erkranken gegenüber einer normalgewichtigen Mutter (BMI 19-24,9) steigt auf das 4,5fache. Das Risiko, eine Gestose auszubilden, steigt auf das 3fache.
Das Risiko des Auftretens mehr als einer Schwangerschaftskomplikation verdoppelt sich bei adipösen Müttern gegenüber normalgewichtigen Müttern. Dies kann unter der Geburt zu höheren Komplikationsraten führen. Häufiger ist bei adipösen Müttern eine primäre oder sekundäre Sectio indiziert. Für die Mütter beinhaltet eine Sectio die allgemeinen Risiken einer Operation (Thrombose/Embolie- Risiko, Blutungen, Wundinfektionen und Bildungen von Verwachsungen) bis hin zur Unfruchtbarkeit.
Zusätzlich stellt sich negativ heraus, dass die Fruchtwasserqualität mit zunehmender Adipositas schlechter wird. Es zeigt sich häufiger Mekonium im Fruchtwasser als Ausdruck einer Hypoxie mit Hyperperistaltik des kindlichen Darms. Durch die Sauerstoffunterernährung kann es vor oder während der Geburt zur Meconiumaspiration kommen, die Obstruktionen und chemische Schädigungen der Lunge verursachen können.
Bei der Betrachtung der Ergebnisse stellt sich allerdings immer wieder heraus, dass die Gewichtszunahme während der Schwangerschaft bei der Beurteilung des Geburtsoutcomes eine untergeordnete Rolle spielt. Allenfalls ist sie ein Parameter zur Abschätzung der Körpermaße des Kindes.
Der BMI eignet sich besser zur Abwägung von Risiken für Mutter und Kind.
Zuletzt ist zu vermerken:
Dennoch sollten untergewichtige Frauen auch nicht außer Acht gelassen werden.
Untergewichtige Frauen haben häufiger Fehlgeburten oder gebären häufiger Frühgeborene mit fehlenden Reifezeichen.
Schlussfolgerung:
Schwangerschaften von adipösen Schwangeren sind mit deutlich erhöhten prä- und perinatalen Schwangerschaftsrisiken für Mutter und Kind behaftet. Daher ist es sinnvoll, schon frühzeitig (am besten vor der Schwangerschaft bei Kinderwunsch) die werdende Mutter bei bestehender Disposition über die Folgen einer Adipositas aufzuklären und durch geeignete Maßnahmen (Diätberatung, Ernährungsumstellung) der Adipositas entgegen zu wirken. Die Beratung sollte jedoch nicht mit der Geburt des Kindes enden. So sollte nach der Geburt das Stillen des Kindes für einen gewissen Zeitraum empfohlen werden, um das spätere Adipositasrisiko des Neugeborenen zu verringern.
Der soziale Status spielt bei der Bekämpfung der Adipositas eine besondere Rolle.
Bildung kann zu einem großen Teil das Auftreten von Adipositas vermeiden.
Following the relational-developmental systems approach, this three-wave study examines whether acute stress (T2) mediates the relationship between the development of personality traits from the beginning of 8th grade (T1, Mage = 15.63, SD = 0.59; 22 girls) to the end of 9th grade (T3). Using the Montréal Imaging Stress Task, which is a task that provokes acute social stress by negative social feedback, this study combined the functional magnetic resonance imaging (fMRI), heart rate, and longitudinal survey data of 41 adolescents. Mediation analysis revealed that stress-induced left insula activation partially mediates the longitudinal stability of conscientiousness. These results highlight the impact of negative social feedback during stress on students’ personality development.
Technological advances in light microscopy have always gone hand in hand with unprecedented biological insight. For microbiology, light microscopy even played a founding role in the conception of the entire discipline. The ability to observe pathogens that would otherwise evade human observation makes it a critical necessity and an indispensable tool to infectious disease research. Thus, the aim of this thesis was to optimize, extend, and functionally apply advanced light microscopy techniques to elucidate spatio-temporal and spatio-morphological components of bacterial and viral infection in vitro and in vivo.
Pathogens are in a constant arms race with the host’s immune system. By finding ways to circumvent host-mediated immune responses, they try to evade elimination and facilitate their own propagation. The first study (publication I) demonstrated that the obligate intracellular pathogen Coxiella burnetii is not just able to infect natural killer (NK) cells, but is actually capable of surviving the harsh degradative conditions in the cytotoxic lymphocyte’s granules. Using live-cell imaging of reporter-expressing Coxiella burnetii, the transient NK cell passage was closely monitored to provide detailed spatio-temporal information on this dynamic process in support of a range of static analyses. Bacterial release from NK cells was pinpointed to a time frame between 24 to 48 hours post-infection and the duration of release to about 15 minutes.
The second approach (publications II-V) aimed at shedding light on the greater spatio-morphological context of virus infection. Thus far, most studies investigating the distribution or tropism of viruses in vivo have used conventional immunohistochemistry in thin sections. Omitting the native spatial context of the infection site in vivo inherently bears the risk of incomplete description. While the microscopic tools and sample preparation protocols needed for volumetric 3D immunofluorescence imaging have recently been made available, they had not gained a foothold in virus research yet. An integral part of this thesis was concerned with the assessment and optimization of available tissue optical clearing protocols to develop an immunofluorescence-compatible 3D imaging pipeline for the investigation of virus infection inside its intact spatio-morphological environment (publication II). This formed the basis for all subsequent volumetric analyses of virus infection in vivo presented here. Consequently, this thesis provided a valuable proof of concept and blueprints for future virus research on the mesoscopic scale of host-pathogen interactions in vivo (publications II-V), using rabies virus (RABV; publications II-IV) and the newly-emerged severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2; publication V) as infection models for the nervous system and the respiratory tract, respectively.
Applying and further improving this volumetric 3D imaging workflow enabled unprecedented insights into the comprehensive in vivo cell tropism of RABV in the central (CNS) (publication III) and peripheral nervous system (PNS) (publication IV). Accordingly, differential infection of CNS-resident astrocytes by pathogenic and lab-attenuated RABV was demonstrated (publication III). While either virus variant showed equal capacity to infect neurons, as demonstrated by quantitative image analysis, only pathogenic field RABVs were able to establish non-abortive infection of astrocytes via the natural intramuscular inoculation route. A combined 3D LSFM-CLSM workflow further identified peripheral Schwann cells as a relevant target cell population of pathogenic RABV in the PNS (publication IV). This suggested that non-abortive infection of central and peripheral neuroglia by pathogenic RABV impairs their immunomodulatory function and thus represents a key step in RABV pathogenesis, which may contribute significantly to the establishment of lethal rabies disease.
Finally, utilizing the full volumetric acquisition power of LSFM, a further refined version of the established 3D imaging pipeline facilitated a detailed mesoscopic investigation of the distribution of SARS-CoV-2 in the respiratory tract of the ferret animal model (publication V). Particularly for this newly-emerged pathogen of global concern, in-depth knowledge of host-pathogen interactions is critical. By preserving the complete spatio-morphological context of virus infection in the ferret respiratory tract, this thesis provided the first specific 3D reconstruction of SARS-CoV-2 infection and the first report of 3D visualization of respiratory virus infection in nasal turbinates altogether. 3D object segmentation of SARS-CoV-2 infection in large tissue volumes identified and emphasized a distinct oligofocal infection pattern in the upper respiratory tract (URT) of ferrets. Furthermore, it corroborated a preferential replication of SARS-CoV-2 in the ferret URT, as only debris-associated virus antigen was detected in the lower respiratory tract of ferrets, thus providing crucial information on the spatial distribution of SARS-CoV-2.
Endothelial dysfunction (ED) comes with age, even without overt vessel damage such as that which occurs in atherosclerosis and diabetic vasculopathy. We hypothesized that aging would affect the downstream signalling of the endothelial nitric oxide (NO) system in the vascular smooth muscle (VSM). With this in mind, resistance mesenteric arteries were isolated from 13-week (juvenile) and 40-week-old (aged) mice and tested under isometric conditions using wire myography. Acetylcholine (ACh)-induced relaxation was reduced in aged as compared to juvenile vessels. Pretreatment with L-NAME, which inhibits nitrix oxide synthases (NOS), decreased ACh-mediated vasorelaxation, whereby differences in vasorelaxation between groups disappeared. Endothelium-independent vasorelaxation by the NO donor sodium nitroprusside (SNP) was similar in both groups; however, SNP bolus application (10−6 mol L−1) as well as soluble guanylyl cyclase (sGC) activation by runcaciguat (10−6 mol L−1) caused faster responses in juvenile vessels. This was accompanied by higher cGMP concentrations and a stronger response to the PDE5 inhibitor sildenafil in juvenile vessels. Mesenteric arteries and aortas did not reveal apparent histological differences between groups (van Gieson staining). The mRNA expression of the α1 and α2 subunits of sGC was lower in aged animals, as was PDE5 mRNA expression. In conclusion, vasorelaxation is compromised at an early age in mice even in the absence of histopathological alterations. Vascular smooth muscle sGC is a key element in aged vessel dysfunction.
Aging is an independent risk factor for hypertension, cardiovascular morbidity, and mortality. However, detailed mechanisms linking aging to cardiovascular disease are unclear. We studied the aging effects on the role of perivascular adipose tissue and downstream vasoconstriction targets, voltage-dependent KV7 channels, and their pharmacological modulators (flupirtine, retigabine, QO58, and QO58-lysine) in a murine model. We assessed vascular function of young and old mesenteric arteries in vitro using wire myography and membrane potential measurements with sharp electrodes. We also performed bulk RNA sequencing and quantitative reverse transcription-polymerase chain reaction tests in mesenteric arteries and perivascular adipose tissue to elucidate molecular underpinnings of age-related phenotypes. Results revealed impaired perivascular adipose tissue-mediated control of vascular tone particularly via KV7.3–5 channels with increased age through metabolic and inflammatory processes and release of perivascular adipose tissue-derived relaxation factors. Moreover, QO58 was identified as novel pharmacological vasodilator to activate XE991-sensitive KCNQ channels in old mesenteric arteries. Our data suggest that targeting inflammation and metabolism in perivascular adipose tissue could represent novel approaches to restore vascular function during aging. Furthermore, KV7.3–5 channels represent a promising target in cardiovascular aging.
In dieser Dissertation wurden Transient Severe Motion (TSM) Artefakte in der mit Gadoxetat kontrastierten Magnetresonanztomographie (MRT) der Leber untersucht. Dieses Phänomen beeinträchtigt die Diagnostik erheblich. Erforscht wurde die Häufigkeit der TSM-Artefakte, der Einfluss des genauen Zeitabschnitts der bildlichen Erfassung der arteriellen Kontrastierungsphase auf ihr Auftreten sowie Risikofaktoren dafür. 354 Patienten, die von 2013 bis 2016 am Institut für Diagnostische Radiologie und Neuroradiologie der Universität Greifswald untersucht wurden, gingen in die retrospektive Studie ein. 69 dieser Patienten erhielten eine Folgeuntersuchung.
Aufnahmen der arteriellen Phase wurden hinsichtlich der TSM-Artefakte auf einer vierstufigen Skala nach Schweregrad eingeteilt (0=keine TSM, 1=leichte TSM, 2=mäßige TSM, 3=schwere TSM). Das Auftreten von TSM-Artefakten war erheblich vom genauen Zeitabschnitt der bildlichen Erfassung der arteriellen Phase (früharteriell, vollarteriell, spätarteriell) sowie eventueller TSM-Artefakte in Voruntersuchungen und verschiedenen Risikofaktoren abhängig.
TSM-Artefakte traten bei 48,59% der untersuchten Patienten auf (172/354). Bei 22,88% aller Patienten (n=81) traten TSM-Artefakte des Grades 1 auf. Bei 18,36% (n=65) wurden TSM-Artefakte des Grades 2 festgestellt. Bei 7,34% (n=26) kam es zu TSM-Artefakten des Grades 3.
In der vollarteriellen Phase kam es mit 58,8% der Untersuchungen am häufigsten zu TSM-Artefakten. In der früharteriellen Phase (51,6%) sowie der spätarteriellen Phase (42,1%) traten die Artefakte signifikant seltener auf (p=0,031). Das Auftreten von TSM-Artefakten korrelierte signifikant mit dem BMI (p=0,001) sowie grenzwertig mit Leberzirrhose (p=0,05). TSM-Artefakte der verschiedenen Schweregrade korrelierten signifikant mit Gewicht (p=0,03), Größe (p=0,033), BMI (p=0,003) sowie γ-GT (p=0,029). Bei Folgeuntersuchungen zeigte sich ein signifikanter Zusammenhang zwischen TSM-Artefakten in der Erstuntersuchung und TSM-Artefakten in Folgeuntersuchungen (p=0,041).
In dieser Studie konnte gezeigt werden, dass die geringste Wahrscheinlichkeit für TSM-Artefakte in der spätarteriellen Phase besteht. Daher ist bei der Diagnostik der mit Gadoxetat kontrastierten Leber-MRT die spätarterielle Phase zu empfehlen.
Hohe Aldosteron-Konzentrationen haben einen nicht zu unterschätzenden Einfluss auf kardiovaskuläre Risikofaktoren wie arterielle Hypertonie, Störungen des Glukosemetabolismus, eingeschränkte Nierenfunktion und Fettstoffwechselstörung. In vorausgehenden Studien an speziellen Patientenkollektiven aber auch in klinischepidemiologischen Studien wurde eine Assoziation zwischen der Plasma AldosteronKonzentration (PAC) und bestimmten Komponenten des Lipidmetabolismus beschrieben. Ob dieser Zusammenhang auch in der allgemeinen Bevölkerung, und innerhalb des Referenzbereiches für die PAC besteht ist unklar. Um dies zu beantworten, beschäftigte sich die vorliegende Arbeit mit der Assoziation zwischen der PAC und ausgewählten Lipoproteinen (High density lipoprotein cholesterol (HDL-C), Low density lipoprotein cholesterol (LDL-C), Triacylglyceride, gesamt Cholesterol, non-HDL-C) in der allgemeinen Bevölkerung. Hierfür wurden Daten von 793 Männern und 938 Frauen zwischen 25-86 Jahren genutzt die am ersten Follow-up der Study of Health in Pomerania (SHIP-1) teilnahmen. Die Assoziation zwischen der PAC und den oben genannten Lipoproteinen wurde anhand von multivariablen, linearen Regressionsmodellen erfasst. Diese wurden adjustiert für Geschlecht, Alter, BMI, geschätzter glomerulärer Filtrationsrate (eGFR) und HbA1c. Es zeigte sich, eine statistisch signifikante positive Assoziation von PAC mit LDL-C und non-HDL-C sowie eine inverse Assoziation mit HDL-C.
Erstmalig konnte in dieser Arbeit somit gezeigt werden, dass die PAC im physiologischen Bereich im engen Zusammenhang mit dem Lipidmetabolismus steht. Die beobachteten und bereits aus vorherigen Studien bekannten Assoziationen sind daher nicht auf ein bestimmtes Patientenkollektiv beschränkt, sondern auch in der allgemeinen Bevölkerung vorhanden. Weiterhin bestätigen die Ergebnisse aus SHIP-1 die bereits bekannte inverse Assoziation zwischen der PAC und HDL-C. Die hier beschriebene Assoziation zwischen der PAC und LDL-C sowie dem non-HDL-C wurde bis Dato noch nicht beschrieben.
Humans are exposed to a plethora of microorganisms that reside on outer and inner body surfaces. These are collectively referred to as the human microbiome. The evolutionary relationship between humans and their microbiome is very complex. It is now widely accepted that these microorganisms are not just passive spectators but play an important role in health. The presence or absence of certain microbes is also linked to various diseases, including inflammatory bowel disease, cardiovascular disease, obesity, cancer, and allergies.
Allergies are several conditions caused by a misguided immune response to foreign antigens that are typically harmless. Common allergic diseases include atopic dermatitis (AD), allergic asthma, hay fever, and anaphylaxis. The incidences of allergic diseases are continuously rising, with up to 40% of the human population thought to be sensitised to environmental antigens. This increased incidence is not simply the result of societies becoming more aware and better at diagnosing these diseases. It is believed that the increases in allergies and sensitisation have environmental causes and are related to Western lifestyles. It is known that the rate of allergies is less frequent in developing countries. They are also more likely to occur in urban than rural areas. The prevailing view of the involvement of bacteria in allergies is described by the hygiene hypothesis. The hypothesis claims that decreased exposure to diverse microbial communities early in life increases the risk of developing allergic diseases. There are numerous examples to support this claim. For example, children born and raised in close contact to farm animals or in the presence of pets, and who are thus in direct and constant contact with a complex microbial environment, are protected from allergic diseases. On the other hand, colonisation or infection with certain bacteria increases allergic disease risks. This seems to contradict the hygiene hypothesis.
It appears that the members of the microbiome have different effects on allergy, and the hygiene hypothesis may not apply to every player in the complex microbial diversity that humans are in contact with. Therefore, a better understanding of the host bacterial interaction is required on the level of bacterial species.
This work studies the interplay between bacteria and the immune system to identify and characterise bacterial components with allergenic properties. In this quest, Staphylococcus aureus (S. aureus) and Staphylococcus epidermidis (S. epidermidis) were investigated for their allergenic properties and involvement in different allergic diseases. In the case of S. aureus, evidence is presented on allergic implications for two different components; serine protease-like proteins (Spls) and superantigens (SAg). Furthermore, experimental support is provided on the allergenic properties of the extracellular serine protease (Esp) from S. epidermidis. We argue that stimulating allergic reactions by staphylococci is an immune evasion mechanism that increases the survival chances of the bacteria within the host.
In chapter 1, an introduction is given to both S. aureus and S. epidermidis and their interactions with the immune system. Also, the bacterial components with allergenic properties and allergic diseases with known bacterial involvement are presented. Finally, the question of why bacteria cause allergy is discussed.
Chapter 2 describes allergic reactions to the Spls of S. aureus in a cohort of cystic fibrosis patients. Chapter 3 focuses on the SAgs of S. aureus. SAgs were discovered more than 30 years ago, but their physiological function is still under discussion. In this chapter, the allergenic properties of SAgs and their possible immunological mechanisms are reviewed, and a possible link between SAgs and allergic diseases is discussed. In chapter 4, the focus shifts to S. epidermidis and its involvement in AD. The human immune response to the Esp from S. epidermidis is characterised in healthy and AD individuals. The allergenic properties of Esp imply a detrimental role of S. epidermidis in AD. Finally, chapter 5 summarises and discusses the results of this thesis. In this section, the pieces are put together, and attention is brought back to the question of why bacteria cause allergies.
In cystic fibrosis (CF) infectious and allergic airway inflammation cause pulmonary exacerbations that destroy the lungs. Staphylococcus aureus is a common long-term colonizer and cause of recurrent airway infections in CF. The pathogen is also associated with respiratory allergy; especially the staphylococcal serine protease-like proteins (Spls) can induce type 2 immune responses in humans and mice. We measured the serum IgE levels specific to 7 proteases of S. aureus by ELISA, targeting 5 Spls (76 CF patients and 46 controls) and the staphopains A and B (16 CF patients and 46 controls). Then we compared cytokine release and phenotype of T cells that had been stimulated with Spls between 5 CF patients and 5 controls. CF patients had strongly increased serum IgE binding to all Spls but not to the staphopains. Compared to healthy controls, their Spl-stimulated T cells released more type 2 cytokines (IL-4, IL-5, IL-13) and more IL-6 with no difference in the secretion of type 1- or type 3 cytokines (IFNγ, IL-17A, IL-17F). IL-10 production was low in CF T cells. The phenotype of the Spl-exposed T cells shifted towards a Th2 or Th17 profile in CF but to a Th1 profile in controls. Sensitization to S. aureus Spls is common in CF. This discovery could explain episodes of allergic inflammation of hitherto unknown causation in CF and extend the diagnostic and therapeutic portfolio.
Die Messung der endexspiratorischen Ammoniakkonzentration bei Patienten mit terminaler Niereninsuffizienz während der Dialyse stellt eine neue nicht-invasive Methode zur Evaluation des Dialyseerfolges dar.
Ziel dieser Studie ist es die endexspiratorische Ammoniakkonzentration von Patienten mit terminaler Niereninsuffizienz während der Dialyse zu messen, um einen signifikanten Abfall der endexspiratorischen Ammoniakkonzentration während des Dialysevorganges nachzuweisen. Des Weiteren gilt es Einflussfaktoren auf die endexspiratorische Ammoniakkonzentration vor der Dialyse zu finden sowie eine mögliche positive Korrelation zwischen der endexspiratorischen Ammoniakkonzentration und der Harnstoffkonzentration im Blut zu untersuchen.
Insgesamt wurden 45 Dialysepatienten (22 Frauen, 23 Männer) im Alter zwischen
dem 28. und dem 85. Lebensjahren für diese Studie rekrutiert. Es erfolgte eine standardisierte Befragung der Patienten bezüglich ihrer Vorerkrankungen und kardiovaskulären Risikofaktoren. Die restlichen relevanten Diagnosen wurden aus den Krankenunterlagen entnommen. Neben der Messung der endexspiratorischen Ammoniakkonzentration erfolgten laborchemische Bestimmungen der Ammoniakkonzentration im EDTA-Blut ebenfalls vor und nach der Dialyse. Auch weitere Laborparameter, wie Aspartataminotransferase, Alaninaminotransferase, Gamma-Glutamyl-Transferase, Harnstoff, Kreatinin sowie Hämoglobin HbA1c wurden mitbestimmt. Die Analyse der endexspiratorischen Ammoniakkonzentration erfolgte mittels des durchstimmbaren Infrarotdiodenlasers unter der Anwendung der Absorptionsspektroskopie als eine hoch sensitive und selektive Methode zur Bestimmung der organischen Atembestandteile.
Die Ergebnisse dieser Studie zeigen einen signifikanten Abfall der endexspiratorischen Ammoniakkonzentrationen im Verlauf der Dialyse (mediane Werte: von 236,3 ppb
auf 120,6 ppb (p < 0,001)). Beim genaueren Betrachten des individuellen Verlaufs von Dialysepatienten fällt auf, dass 18 Patienten mit einer hohen endexspiratorischen Ammoniakkonzentration vor der Dialyse (über 300 ppb) einen deutlichen Abfall (> 100 ppb) im Verlauf der Behandlung aufweisen. Von den Patienten, bei denen vor der Dialyse ein niedriger Atemammoniakspiegel (< 300 ppb) erfasst wurde, zeigten sich bei fünf Probanden ein deutlichen Abfall, bei elf Probanden ein geringerer Abfall (< 100 ppb), bei vier Probanden keine signifikante Veränderung (±10 ppb) und bei sieben Teilnehmern eine Erhöhung der endexspiratorischen Ammoniakkonzentration während der Dialyse.
Die statistische Analyse ergab weiterhin eine deutlich positive Korrelation zwischen den Ammoniakkonzentrationen im Blut vor der Dialyse mit den Blutammoniakwerten nach der Dialyse und eine mäßig positive Korrelation zwischen den endexspiratorischen Ammoniakkonzentrationen vor der Dialyse mit den Ammoniakspiegel im Atem nach der Dialyse. Eine schwach positive Korrelation wurde zwischen den endexspiratorischen Ammoniakwerten nach der Dialyse mit den Blutammoniakwerten nach der Dialyse gefunden. Die lineare Regressionsanalyse ergab eine signifikante Assoziation von Nephrektomie und Restdiurese mit den endexspiratorischen Ammoniakwerten, welche vor der Dialyse gemessen wurden. Damit wird verdeutlich, das nephrektomierte Patienten und Patienten mit einer höheren Restdiurese einen deutlichen Abfall der endexspiratorischen Ammoniakkonzentrationen während der Dialyse aufzeigten und somit vermehrt von der Dialyse als Behandlung profitieren.
In Anlehnung an die Ergebnisse dieser Studie, dass im Verlauf der Dialyse ein signifikanter Abfall der endexspiratorischen Ammoniakkonzentration vorliegt, wird eine klinische Etablierung der nicht-invasiven Ammoniakkonzentrationsmessung vor und nach der Dialyse als eine gute Möglichkeit der Überwachung einer Dialysesitzung empfohlen. Aus unserer Sicht sollte am besten die Messung nicht offline mittels Sammelns der Atemproben im Tedlar-Beutel, sondern durch direktes Ausatmen in das Messsystem erfolgen, um den Verlust von an der Oberfläche des Beutels haftenden Ammoniaks zu verhindern. Falls jedoch die offline Methode bevorzugt werden sollte, müsste gewährleistet werden, dass die Atemgasproben so schnell wie möglich analysiert werden, um die Messgenauigkeit zu stärken.
Human T-cell lymphotropic virus type 1 (HTLV-1) infection affects millions of individuals worldwide and can lead to severe leukemia, myelopathy/tropical spastic paraparesis, and numerous other disorders. Pursuing a safe and effective immunotherapeutic approach, we compared the viral polyprotein and the human proteome with a sliding window approach in order to identify oligopeptide sequences unique to the virus. The immunological relevance of the viral unique oligopeptides was assessed by searching them in the immune epitope database (IEDB). We found that HTLV-1 has 15 peptide stretches each consisting of uniquely viral non-human pentapeptides which are ideal candidate for a safe and effective anti-HTLV-1 vaccine. Indeed, experimentally validated HTLV-1 epitopes, as retrieved from the IEDB, contain peptide sequences also present in a vast number of human proteins, thus potentially instituting the basis for cross-reactions. We found a potential for cross-reactivity between the virus and the human proteome and described an epitope platform to be used in order to avoid it, thus obtaining effective, specific, and safe immunization. Potential advantages for mRNA and peptide-based vaccine formulations are discussed.
An Innovative Protocol for Metaproteomic Analyses of Microbial Pathogens in Cystic Fibrosis Sputum
(2021)
Hallmarks of cystic fibrosis (CF) are increased viscosity of mucus and impaired mucociliary clearance within the airways due to mutations of the cystic fibrosis conductance regulator gene. This facilitates the colonization of the lung by microbial pathogens and the concomitant establishment of chronic infections leading to tissue damage, reduced lung function, and decreased life expectancy. Although the interplay between key CF pathogens plays a major role during disease progression, the pathophysiology of the microbial community in CF lungs remains poorly understood. Particular challenges in the analysis of the microbial population present in CF sputum is (I) the inhomogeneous, viscous, and slimy consistence of CF sputum, and (II) the high number of human proteins masking comparably low abundant microbial proteins. To address these challenges, we used 21 CF sputum samples to develop a reliable, reproducible and widely applicable protocol for sputum processing, microbial enrichment, cell disruption, protein extraction and subsequent metaproteomic analyses. As a proof of concept, we selected three sputum samples for detailed metaproteome analyses and complemented and validated metaproteome data by 16S sequencing, metabolomic as well as microscopic analyses. Applying our protocol, the number of bacterial proteins/protein groups increased from 199-425 to 392-868 in enriched samples compared to nonenriched controls. These early microbial metaproteome data suggest that the arginine deiminase pathway and multiple proteases and peptidases identified from various bacterial genera could so far be underappreciated in their contribution to the CF pathophysiology. By providing a standardized and effective protocol for sputum processing and microbial enrichment, our study represents an important basis for future studies investigating the physiology of microbial pathogens in CF in vivo – an important prerequisite for the development of novel antimicrobial therapies to combat chronic recurrent airway infection in CF.
Zusammenfassung
Kaltes atmosphärisches Plasma (CAP) ist eine mögliche neue Therapieoption für das hochaggressive Glioblastoma multiforme. Bisher konnte die Wirksamkeit der Behandlung von Glioblastomzellen mit CAP sowohl in vitro, als auch in vivo bestätigt und reaktive Sauerstoffspezies (ROS) als ein wichtiger Mediator der CAP-Wirkung identifiziert werden. Sowohl die zytotoxische Wirkung von CAP auf Glioblastomzellen, als auch eine positive Korrelation der Behandlungsdauer mit der Stärke der CAP-Wirkung konnten wir bestätigen. Mit dem Ziel einer molekularen Charakterisierung der zugrundeliegenden Vorgänge innerhalb der Zellen untersuchten wir die Veränderung des Expressions- und Aktivierungsmusters relevanter Proteine zentraler Wachstums- und Apoptosewege, sowie der microRNA-1 in den humanen Glioblastomzelllinien U87-MG und LN-18 unter Behandlung mit CAP.
Die Kinase ERK1/2, der Zellzyklusregulator p21 und das Hitzeschockprotein Hsp90 sind zentrale Effektoren der Tumorprogression. Obgleich die CAP-Behandlung leichte Änderungen der Expressionsraten dieser Proteine zeigte, kann ohne weitere Untersuchungen nicht von der Beteiligung dieser Faktoren ausgegangen werden. Ein Einfluss auf die Zellproliferation ist jedoch denkbar.
Im Falle der proliferativen Kinase AKT1 konnte eine Induktion in beiden untersuchten Glioblastomzellinien nachgewiesen werden. Diese könnte möglicherweise eine zytoprotektive Antwort auf den CAP-vermittelten Redox-Stress darstellen und wäre demnach als eine Resistenz gegenüber der CAP-Behandlung anzusehen. Im Gegensatz dazu stellt die Induktion der tumorsuppressiven MikroRNA miR-1, im Einklang mit in der Literatur beschriebener Inhibition des Zellwachstums bei Induktion, einen Wirkmechanismus des CAP dar.
Insgesamt kommt es in den Glioblastomzellen nach der Behandlung mit CAP zu einer Veränderung verschiedener Signalkaskaden. Insbesondere die vermutlich protektive Wirkung der Kinase AKT1, sowie die wirkungs-verstärkenden Effekte von miR-1 könnten eine entscheidende Rolle bei der Wirkung von CAP auf Glioblastomzellen darstellen. Weiterführende Untersuchungen insbesondere dieser Mediatoren und deren Interaktionen könnten zu einem tieferen Verständnis der Wirkungsweise von CAP auf die Zelle beitragen und die Entwicklung dieser neuen und innovativen Behandlungsmethode vorantreiben.
In der vorliegenden Studie wurden 121 Frauen mit Zustand nach einer Operation eines Mammakarzinoms und anschließender Brustrekonstruktion mittels des BreastQ – Fragebogens zu ihrer subjektiven Zufriedenheit und Lebensqualität nach der Operation befragt. Anhand der Ergebnisse wurde untersucht ob sich bei den Patientinnen, abhängig von dem zur Rekonstruktion verwendeten Interponats, Unterschiede bezüglich der oben genannten Kriterien zeigen. Die in dieser Studie befragten Patientinnen wurden alle im Zeitraum von 2010 – 2018 im Universitätklinikum Greifswald behandelt. Nach SSM/NSM erfolgte bei jeder Patientin eine Interponat gestützte heterologe Brustrekonstruktion mittels Silikonimplantat. Die in dieser Studie untersuchen Interponate waren das titanisierten Polypropylennetz (TiLOOP®Bra), das teilresorbierbare Bikomponentennetz (SERAGYN®BR) und die azellulärer Dermis (StratticeTM). Die Erhebung der Daten erfolgte mittels des standardisierten Fragebogens BreastQ reconstruction Modul, welche die subjektive Zufriedenheit und Lebensqualität nach der Operation eruierte. Hierfür wurde den Patientinnen der Fragebogen sowie ein frankierter Rücksendeumschlag der Post zugesandt. Die Patientinnen wurden gebeten, den Fragebogen retrospektiv zu beantworten und ihn danach an die Universitätsklinik Greifswald zurück zu senden. Die Auswertung der Fragebögen erfolgte mittels der extra hierfür entworfenen QScore Scoring Software. Diese Software generiert für die einzelnen Abschnitte des Fragebogens aus den erhobenen Daten die Summendaten. Die Summendaten werden in eine Skala von 0 bis 100 konvertiert. Null steht in diesem Fall für sehr unzufrieden und 100 für sehr zufrieden. In Bezug auf die damit erhobene subjektive Zufriedenheit und Lebensqualität ergaben sich in Abhängigkeit von dem verwendeten Interponat keine signifikanten Unterschiede.
Gemäß Patienten - Reported Outcome (BreastQ – Fragebogen) beeinflusst das verwendete Material die Lebensqualität und Zufriedenheit der Patientinnen nicht. Aus diesen Daten kann gefolgert werden, dass alle drei Interponate zur Unterstützung einer heterologen Brustrekonstruktion geeignet sind und zu einem, für die Patientinnen zufriedenstellendem Ergebnis führen. Es besteht kein Vorteil eines Interponats gegenüber den anderen. Alle Patientinnen fühlten sich über die Behandlung gut informiert und aufgeklärt. Während ihrer Behandlung fühlten sie sich zudem gut und professionell betreut. Die Auswahl des zu verwendenden Interponats muss individuell nach den Wünschen der Patientin, der Expertise des behandelnden Chirurgen und nach den anatomischen Gegebenheiten bzw. der Größe des Implantats getroffen werden.
Zusätzlich wurde in dieser Studie der Einfluss von zusätzlichen Parametern (Alter, Gewicht, OP – Technik, OP – Zeitraum, RTX und prophylaktisch oder therapeutisch) auf die postoperative Lebensqualität und Zufriedenheit untersucht. Bei Patientinnen nach prophylaktischer Mastektomie zeigte sich materialunabhängig eine signifikante Verbesserung des physischen Wohlbefindens (Brust) (p = .04). Eine postoperative Radiotherapie (RTX) führte zu einer signifikanten Verschlechterung der Zufriedenheit mit dem Ergebnis (p = .005). Außerdem gaben jüngere Patientinnen (<50 J.) postoperativ ein signifikant höheres sexuelles Wohlbefinden (p = .03) an. Die restlichen Berechnungen wurden mit einem p > 0,05 als nicht signifikant bewertet. Hervorzuheben ist jedoch, dass jüngere (< 50 Jahre) und normalgewichtige (BMI 24 kg/m2) Patientinnen, sowie Patientinnen, welche eine prophylaktische Mastektomie, NSM, eine primäre Brustrekonstruktion oder keine RTX im Mittel höhere postoperative Zufriedenheiten erzielten.
Um die Ergebnisse dieser Arbeit zu prüfen, sollten zukünftig prospektive, randomisiert und multizentrische Studien angefertigt werden.
Zusammenfassung
Zielsetzung: Eine Analyse des Hygienestatus im Rettungsdienst in Deutschland ergab eine Reihe von Defiziten (Groß 2010). Die sich daraus ergebenden Schlussfolgerungen wurden zunächst publiziert (Groß et al. 2010, Kramer et al. 2013), fanden 2014 Eingang in die Leitlinie der AWMF zu „Hygienemaßnahmen beim Patiententransport“ und wurden 2019 bei der Aktualisierung der Leitlinie berücksichtigt, wobei die ursprünglichen Schlussfolgerungen der o.g. Arbeit nicht an Gültigkeit eingebüßt haben. Um die Situation in einem ganzen Land zu analysieren, wurde Island als kleines Land ausgewählt.
Methode: Im Juli 2011 wurde eine Islandweite flächendeckende Umfrage in Form eines Fragebogens durchgeführt und an alle Rettungswachen verteilt, die am Krankentransport und Rettungsdienst beteiligt sind und 24-Stunden Bereitschaftsdienst haben. Ein Fragebogen mit 43 Fragen richtete sich an die Wachleiter*innen, ein separater Fragebogen mit 35 Fragen an das Personal.
Ergebnisse: 33 Fragebögen der Wachleiter*innen und 94 Fragebögen des Personals wurden vollständig beantwortet und ausgewertet.
Es kann auf beinahe allen befragten Themengebieten ein Defizit in der Gesetzeslage bzw. in Bezug auf Vorschriften und Leitlinien festgestellt werden. Das hat einen mangelhaften Wissensstand des Personals des Rettungsdiensts und Krankentransports zur Folge. Die Personalhygiene (Hände, Kleidung, Impfungen), der Fahrzeuge, Schutzmaßnahmen gegen multiresistente Erreger, die Qualitätssicherung und die Schulung bedürfen einer durchgreifenden Verbesserung. Gerade wenn vor allem in ländlichen Regionen Islands nur wenige Krankentransporte durchgeführt werden, entbindet das nicht von der Einhaltung der Basishygiene.
Schlussfolgerung: In der rasch globalisiert wachsenden Welt muss eine einheitliche landesübergreifende Regelung hygienischer Verfahrensweisen zum Schutz des Personals und der Patienten*innen im Rettungsdienst und Krankentransport in Island ausgearbeitet und unterrichtet werden.
Da es nur wenig offizielle und v.a. länderübergreifende Empfehlungen bzw. Verfahrensanweisungen gibt, wird zur Verbesserung ein Maßnahmenkatalog vorgeschlagen, der der Nationalen Gesundheitsbehörde übergeben wurde.
Analysis and Reduction of Cellular Heterogeneity in Strain Optimization of Bacillus licheniformis
(2021)
Bacillus species invest substantial resources in inherent cellular processes for pre-adaptation to environmental changes, many of which are dispensable in the controlled environment of industrial bioprocesses. The underlying physiological mechanisms are well characterized in B. subtilis, but only little is known about these processes in the closely related B. licheniformis. Moreover, experimental conditions in previous studies differ from industrial settings in most parameters, foremost in batch cultures or plate-based analysis over fed-batch processes. In this thesis, cellular heterogeneity was analyzed in B. licheniformis in optimized, nutrient-rich media in batch and fed-batch cultivations. Systematic inactivation of genes involved in biofilm formation and synthesis of the flagellar apparatus or global regulators thereof resulted in higher protein production and provided new insights into biofilm formation and cellular heterogeneity in this strain.
Analysis of bioactive lipids from different infection models during bacterial and viral infections
(2021)
Bioactive lipids or lipid mediators influence numerous processes like the reproduction, the bone turnover, the pain perception, the cardiovascular function and the immune system. Eicosanoids and oxylipins are parts of the immunomodulatory lipid mediators, which can be synthesized from polyunsaturated fatty acids (PUFAs) by enzymatic and non-enzymatic reactions. Typical members of eicosanoids are prostaglandins and leukotrienes. The properties of bioactive lipids include the activation of inflammatory reactions as well as the support of resolution. Like hormones, they act locally restricted and in low concentrations. Further bioactive lipids exist i.e. intermediates of the sphingolipid class. The biosynthesis of some of these compounds like the prostaglandins can be influenced by different drugs whereas for other groups of lipid selective inhibitors are still missing. Their impact on inflammatory processes and against chronic diseases has already been analyzed, while studies in context with infection are largely limited. Infection of the upper respiratory tract caused by viral and bacterial pathogens constitute a huge burden for the human healthcare. The main pathogens are the Influenza A virus (IAV), Staphylococcus aureus (S. aureus), Streptococcus pneumoniae (S. pneumoniae) and Streptococcus pyogenes (S. pyogenes). Besides mono-infection with one of these pathogens, frequently occurring bacto-viral co-infections exist, which negatively influence the etiopathology. The main task of the immune system is the detection and the elimination of pathogens, which can essentially be affected by lipid mediators. Their instability due to oxidizability, the existence of regioisomers and the low abundance of eicosanoids and other oxylipins are the main problems for their analytical measurement.
The mayor objective of this dissertation was the establishment of a suitable analytical method for selected lipid mediators and the detection of infection-related changes. The separation and detection was performed by using high-performance liquid chromatography (HPLC) coupled with triple quad mass spectrometry. This combination is called tandem mass spectrometry (MS/MS). The MS parameters were optimized for approximately 30 lipid mediators by use of chemical standards and the detection was achieved by dynamic multiple reaction monitoring (MRM). Furthermore, the spatial resolution of selected sphingolipids was analyzed in tissue samples using matrix-assisted laser desorption ionization mass spectrometry imaging (MALDI-MS-Imaging). Concerning the HPLC-MS/MS detection, an MS method was established and optimized with standard compounds. Another crucial part of the establishment was the extraction of bioactive lipids from the different sampling materials. Whereas well tested protocols exist for the extraction and detection of lipid mediators, such protocols for MALDI-MS-Imaging are still limited due to the novelty of this measurement. Ultimately, robust and reproducible protocols for both techniques that were used for the analysis of a broad array of samples from infection experiments were established for both techniques. The analyses of infected cell culture, mice and pigs revealed infection-related perturbations of host lipid mediator levels. Depending on the scientific issue, the sample types cell pellets, lungs, spleens, livers, blood plasmas, pawns including bones or bronchoalveolar lavages were analyzed. For MALDI-MS-Imaging, the spatial distribution of sphingolipids in lung and spleen was detected.
The present dissertation includes four coherent research scopes, in which the pathogen impact on host-derived lipid mediators was detected with the above mentioned analytical methods. The infection models epithelial cells (article II), mouse (article III and IV) and pig (article I) – the latter as the most human like model - showed different aspects of the host-pathogen interaction. The analysis of samples from IAV infection for all three hosts revealed a couple of similarities for some oxylipins that were also described in human infections. Additionally, cell culture and mouse samples from mono-infections as well as co-infections with the pathogens S. aureus and S. pneumoniae were measured. In particular for the bacterial mono- and co-infections, these are the first published results with aspects of infection related changes of lipid mediators. The additional spatial resolution of the sphingolipid intermediates sphingosine 1-phosphate and ceramide 1-phosphate revealed important new insights into their tissue distribution and changes during co-infection.
Article I describes the IAV-specific oxylipin changes in the pig (german landrace) as infection model. Therefore, the sample types lung, spleen, blood plasma, and bronchoalveolar lavage from infected animals at different time points after infection were analyzed and compared with samples from uninfected pigs. Mainly in the lung and the spleen, increased amounts of certain lipid mediators were observed. These changes coincide well with already described alterations in humans and mice. Furthermore, the analysis of different sample material provided an overview about appropriate sample types. Surprisingly, many perturbations were detected in the spleen, which itself was uninfected. Based on the local reaction of lipid mediators, most studies concentrate on sample material with close contact to side of infection. Therefore, this dissertation reveals new insights into a form of systemic immune response. Besides the use of animals with a complex immune system for infection experiments, human bronchial epithelial cells (16HBE) were mono- and co-infected with the pathogens S. aureus, S. pneumoniae and IAV as described in article II. Such cells are the initial barrier for and first contact site with pathogens and thus the comprehension of this host-pathogen interaction is of essential importance. Most changes were detected during pneumococcal infection. Furthermore, the analyzed infections with bacterial pathogens differed from IAV infection by an increased synthesis of 5-hydroxyeicosatetraenoic acid (HETE). For further infections with the above mentioned pathogens, the mouse was used as an infection model. Besides infections affecting the respiratory tract, also the impact of an S. pyogenes infection in different mice strains was analyzed and described in article III. Infection-related changes in prostaglandins, which are involved in bone turnover in swollen pawns as well as enhanced amounts of sepsis- and arthritis-associated lipid mediators were detected, in case arthritis had been induced prior to infection. Furthermore, increased amounts of 20-HETE could be observed for such severe infections. An enhanced biosynthesis of 20-HETE was further confirmed in a high-pathogenic S. aureus LUG2012 infection in article IV for all examined sample types. In this last article of this dissertation, bacterial and viral infections in mice were analyzed similar to those described in article II. Mainly IAV-specific lipid mediator alterations were detected, which are in accordance with the findings of the infected pigs. The additional MALDI-MS-Imaging measurements revealed so far unknown accumulation of ceramide 1-phosphate in lung and spleen as well as enrichment in the red pulp of the spleen.
In summary, this dissertation provides substantial lipid mediator profiles for infections in three different model systems with selected bacterial and viral pathogens. The obtained data constitute a suitable basis for continuative research projects, in which the influence of single bioactive lipids on the course of infection could be examined in more detail.
This work presents the first experimental investigation of the gas balance on the optimized modular stellarator Wendelstein 7-X (W7-X). A balance of all injected and removed particles and a measurement of internal particle reservoirs allows inference of the bound particle reservoir in the wall, which is of interest due to its effects on plasma density control and fuel retention. Different scenarios of the gas balance are presented with data from the operation campaign 1.2 with an inertially cooled graphite divertor. Both net outgassing and net retention scenarios are presented and W7-X is found to operate stable in a wide range of scenarios with varying wall conditions.
Since fusion experiments are conducted in ultra-high vacuum, suitable gauges are required for total and partial pressure measurement. The challenges and opportunities of the operation of pressure gauges in the steady magnetic field extending beyond plasma pulses are discussed. The performance of newly improved neutral pressure gauges, based on crystal cathode emitters is quantified. These provide improved operational robustness since they can be operated for long periods of time in strong magnetic fields. A crystal cathode setup and and its operation performance is presented along with a fast calibration scheme.
Partial pressure measurements provide additional important information complementing the total neutral pressure measurements, and allowing additional physics insights. As part of this thesis work, a new diagnostic of this kind was implemented on W7-X, the so-called diagnostic residual gas analyzer (DRGA). It provides a wealth of information on various neutral gas species, with a relatively high time resolution - of order a few seconds. The diagnostic setup and its first results are presented in this thesis.
Anaplasma phagocytophilum and Anaplasma ovis–Emerging Pathogens in the German Sheep Population
(2021)
Knowledge on the occurrence of pathogenic tick-borne bacteria Anaplasma phagocytophilum and Anaplasma ovis is scarce in sheep from Germany. In 2020, owners from five flocks reported ill thrift lambs and ewes with tick infestation. Out of 67 affected sheep, 55 animals were clinically examined and hematological values, blood chemistry and fecal examinations were performed to investigate the underlying disease causes. Serological tests (cELISA, IFAT) and qPCR were applied to all affected sheep to rule out A. phagocytophilum and A. ovis as a differential diagnosis. Ticks were collected from selected pastures and tested by qPCR. Most animals (n = 43) suffered from selenium deficiency and endoparasites were detected in each flock. Anaplasma spp. antibodies were determined in 59% of examined sheep. Seventeen animals tested positive for A. phagocytophilum by qPCR from all flocks and A. phagocytophilum was also detected in eight pools of Ixodes ricinus. Anaplasma phagocytophilum isolates from sheep and ticks were genotyped using three genes (16S rRNA, msp4 and groEL). Anaplasma ovis DNA was identified in six animals from one flock. Clinical, hematological and biochemical changes were not significantly associated with Anaplasma spp. infection. The 16S rRNA analysis revealed known variants of A. phagocytophilum, whereas the msp4 and groEL showed new genotypes. Further investigations are necessary to evaluate the dissemination and health impact of both pathogens in the German sheep population particularly in case of comorbidities.