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- SNP (12)
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- Spracherwerb (12)
- Toll-like-Rezeptoren (12)
- Ultrakurzer Lichtimpuls (12)
- Validierung (12)
- Zelladhäsion (12)
- adolescents (12)
- animal model (12)
- biofabrication (12)
- blood–brain barrier (12)
- carbenes (12)
- case report (12)
- cell cycle (12)
- chemistry (12)
- colorectal carcinoma (12)
- complications (12)
- database (12)
- dementia (12)
- drug delivery (12)
- dynamics (12)
- endothelium (12)
- enzyme replacement therapy (12)
- fear conditioning (12)
- genome (12)
- interaction (12)
- lymphocytes (12)
- malignant hyperthermia (12)
- measles (12)
- metaanalysis (12)
- microarray (12)
- molecular beam epitaxy (12)
- monoclonal antibodies (12)
- neuropathy (12)
- optimization (12)
- osteoarthritis (12)
- pollen (12)
- polymers (12)
- rats (12)
- recombination (12)
- reconstruction (12)
- reliability (12)
- screening (12)
- super-resolution microscopy (12)
- systematic review (12)
- therapeutic drug monitoring (12)
- tinnitus (12)
- total knee arthroplasty (12)
- trabeculectomy (12)
- translation (12)
- ubiquitin (12)
- ultrasound (12)
- vitamin D (12)
- vorsprachliche Entwicklung (12)
- zebrafish (12)
- Überleben (12)
- ++ (11)
- 3D (11)
- ARDS (11)
- Anorexia nervosa (11)
- Antigen CD8 (11)
- Arabidopsis (11)
- B-Zelle (11)
- Bioisosterie (11)
- Biosynthese (11)
- Bioverfügbarkeit (11)
- Bruchpilot (11)
- Candida (11)
- Chromatin (11)
- Click-Chemie (11)
- Diboren (11)
- Dynamik (11)
- EGFR (11)
- Elektronentransfer (11)
- Enzym (11)
- Epidermaler Wachstumsfaktor-Rezeptor (11)
- Flavonoide (11)
- Fließverhalten (11)
- Fluorescence (11)
- Fotovoltaik (11)
- Genom (11)
- Hirntumor (11)
- Hypoxie (11)
- Immuncytochemie (11)
- Immunotherapy (11)
- Japankärpfling (11)
- Knochen (11)
- Knochenersatz (11)
- Kolorektales Karzinom (11)
- Laser (11)
- Längsschnittuntersuchung (11)
- MS (11)
- Mais (11)
- Mathematik (11)
- Medienkompetenz (11)
- Megakaryozyt (11)
- Mensch-Maschine-Kommunikation (11)
- Mesenchymale Stammzellen (11)
- Mesenchymzelle (11)
- Model (11)
- NIRS (11)
- Nanodiamant (11)
- Neuropathie (11)
- Operation (11)
- Osteoinduktion (11)
- PCR (11)
- Parathormon (11)
- Perylenbisimid (11)
- Phylogenie (11)
- Proteaseinhibitor (11)
- Proteasen (11)
- Psychiatrie (11)
- Pulmonale Hypertonie (11)
- Quality of life (11)
- Quanten-Hall-Effekt (11)
- Reperfusion (11)
- Risikofaktoren (11)
- Rotatorenmanschette (11)
- Salmonella (11)
- Schizophrenia (11)
- Schlafapnoe (11)
- Schließzelle (11)
- Schule (11)
- Schädel-Hirn-Trauma (11)
- Silicate (11)
- Skala (11)
- Small RNA (11)
- Sprache (11)
- Squark (11)
- Stammzellen (11)
- Sterblichkeit (11)
- Supraleitung (11)
- Symbiose (11)
- T cell (11)
- Topologie (11)
- Training (11)
- Tuberkelbakterium (11)
- Tumor-Nekrose-Faktor <alpha> (11)
- USA (11)
- Ubiquitin (11)
- Vasodilatator-stimuliertes Phosphoprotein (11)
- Wahrnehmung (11)
- Westafrika (11)
- Zelltod (11)
- adhesion (11)
- age (11)
- allergy (11)
- amygdala (11)
- antibody (11)
- autoantibodies (11)
- biocompatibility (11)
- biofilm (11)
- cancer treatment (11)
- catalysis (11)
- cell adhesion (11)
- cochlear implant (11)
- communication (11)
- coping (11)
- dosimetry (11)
- emotions (11)
- fluorescence microscopy (11)
- glioblastoma multiforme (11)
- hypoxia (11)
- kinetics (11)
- lung (11)
- meiosis (11)
- membrane proteins (11)
- molecular dynamics (11)
- nervous system (11)
- neural networks (11)
- neuroendocrine tumor (11)
- next generation sequencing (11)
- nuclear envelope (11)
- periodontitis (11)
- plasticity (11)
- pollination (11)
- randomized controlled trial (11)
- reactive oxygen species (11)
- relapse (11)
- review (11)
- safety (11)
- synaptic plasticity (11)
- topological insulator (11)
- transport (11)
- university (11)
- Alkohol (10)
- Alzheimer's disease (10)
- Alzheimer’s disease (10)
- Antigen CD28 (10)
- Arzneimittelüberwachung (10)
- Atherosclerosis (10)
- BERA (10)
- Bacteria (10)
- Beschichtung (10)
- Bildverarbeitung (10)
- Bioinformatics (10)
- Biokompatibilität (10)
- Blazar (10)
- Borole (10)
- CRISPR/Cas-Methode (10)
- Cadherine (10)
- Calciumphosphate (10)
- Children (10)
- Chronische Niereninsuffizienz (10)
- Churritisch (10)
- Cochlear-Implantat (10)
- Computertomografie (10)
- Coronaviren (10)
- Cyclo-GMP (10)
- Depressivität (10)
- Diamant (10)
- Dimerisierung (10)
- Dotierung (10)
- Durchflusscytometrie (10)
- Echokardiographie (10)
- Eierstockkrebs (10)
- Elektrochemie (10)
- Elektronenkorrelation (10)
- Englisch (10)
- Enzyminhibitor (10)
- Epidemiologie (10)
- Erbkrankheit (10)
- Ereigniskorreliertes Potenzial (10)
- Erwachsener (10)
- Franken (10)
- Frau (10)
- Funktionalisierung <Chemie> (10)
- Förderung (10)
- Geldpolitik (10)
- Geschlecht (10)
- Glatter Krallenfrosch (10)
- HSM-Satztest (10)
- Herzmuskelzelle (10)
- Honigbiene (10)
- Hypophosphatasie (10)
- Immunology (10)
- Impfstoff (10)
- Induzierte pluripotente Stammzelle (10)
- Interleukin 4 (10)
- JNK (10)
- Klassifikation (10)
- Kniegelenk (10)
- Kohlenstoff (10)
- Komplikation (10)
- Kooperation (10)
- Kultur (10)
- LASP1 (10)
- LC-MS (10)
- LPS (10)
- Ladungstransfer (10)
- Ligand (10)
- Lokalisation (10)
- Mathematikunterricht (10)
- Mathematisches Modell (10)
- Medulloblastom (10)
- Metallocene (10)
- Methylphenidat (10)
- Mikrokerne (10)
- Multiple Myeloma (10)
- Musik (10)
- Mutagenität (10)
- Nahrungserwerb (10)
- Nebennierenrindenkarzinom (10)
- Neolithikum (10)
- Neuropathischer Schmerz (10)
- Niereninsuffizienz (10)
- Niger (10)
- Osteosynthese (10)
- Pain (10)
- Panikstörung (10)
- Parasit (10)
- Parodontitis (10)
- Pathogenität (10)
- Plattenepithelkarzinom (10)
- Prevalence (10)
- Prostaglandine (10)
- Präfrontaler Cortex (10)
- Pädagogik (10)
- Qualitätskontrolle (10)
- RNA interference (10)
- RNA-seq (10)
- RNS-Spleißen (10)
- Remote Sensing (10)
- Rhodium (10)
- Rituximab (10)
- SAR (10)
- Schilddrüse (10)
- Schultergelenk (10)
- Silaanaloga (10)
- Silber (10)
- Silicon (10)
- South Africa (10)
- Sphingolipide (10)
- Sprachverstehen (10)
- Starke Kopplung (10)
- Stickstoffmonoxid-Synthase (10)
- Stroke (10)
- Struktur (10)
- T-Lymphozyten (10)
- T-Lymphozyten-Rezeptor (10)
- Tagesrhythmus (10)
- Totalsynthese (10)
- Toxizität (10)
- Treg (10)
- Trypanosomen (10)
- Verwaltungsrecht (10)
- Vitamin D (10)
- Vor- und Frühgeschichte (10)
- Vorschulkind (10)
- Wachstum (10)
- Zebrabärbling (10)
- amino acids (10)
- antimicrobial resistance (10)
- bariatric surgery (10)
- biosynthesis (10)
- boranes (10)
- cartilage (10)
- chemokines (10)
- circadian rhythms (10)
- clinical trial (10)
- comparison (10)
- complex (10)
- coronary artery disease (10)
- decision-making (10)
- density functional calculations (10)
- eNOS (10)
- education (10)
- emotion regulation (10)
- fear (10)
- genome-wide association (10)
- head and neck cancer (10)
- heart rate (10)
- hydrogels (10)
- immunomodulation (10)
- injury (10)
- insect (10)
- knockout (10)
- leaf-cutting ants (10)
- leukemia (10)
- lymph nodes (10)
- mechanism (10)
- membrane potential (10)
- microbiome (10)
- microglia (10)
- molecular imaging (10)
- motivation (10)
- oncolytic virotherapy (10)
- oncolytic virus (10)
- oxidativer Stress (10)
- phenotype (10)
- proteomics (10)
- regulatorische T-Zellen (10)
- remodeling (10)
- senescence (10)
- silicon (10)
- social interaction (10)
- stem cell transplantation (10)
- tDCS (10)
- thrombosis (10)
- tight junctions (10)
- tumor microenvironment (10)
- tumors (10)
- vaccination (10)
- vertigo (10)
- water oxidation (10)
- Östrogene (10)
- 3 (9)
- Adenosin (9)
- Adenosine receptors (9)
- Affekt (9)
- Afrika (9)
- Alps (9)
- Analyse (9)
- Angeregter Zustand (9)
- Anxiety (9)
- Aorta (9)
- BMP-2 (9)
- Bakterielle Infektion (9)
- Bauchspeicheldrüsenkrebs (9)
- Beyond Standard Model (9)
- Bordetella pertussis (9)
- Borylierung (9)
- Boğazkale (9)
- Butyrat (9)
- CRISPR/Cas9 (9)
- Carbene (9)
- Carcinogenese (9)
- Catalysis (9)
- Chiralität <Chemie> (9)
- Cloud Computing (9)
- Computational chemistry (9)
- Covid-19 (9)
- Dendritic cells (9)
- Diborane (9)
- Digital Humanities (9)
- Diskursanalyse (9)
- Dünndarm (9)
- Einzelphotonenemission (9)
- Elektroencephalographie (9)
- Elektronenmikroskopie (9)
- Elektronenstruktur (9)
- Elementarteilchenphysik (9)
- Epithel (9)
- Ernährung (9)
- Experimentelle Psychologie (9)
- Extremwertstatistik (9)
- Familie (9)
- Fanconi Anämie (9)
- Fettgewebe (9)
- Fibroblastenwachstumsfaktor (9)
- Fibromyalgie (9)
- Frühgeborene (9)
- Funktionelle Kernspintomografie (9)
- GIS (9)
- Geistigbehindertenpädagogik (9)
- Gentherapie (9)
- Geoinformationssystem (9)
- Geruchswahrnehmung (9)
- Glioblastoma (9)
- Google Earth Engine (9)
- Grammatik (9)
- Grenzfläche (9)
- Handlungsorientierung (9)
- Hethiter (9)
- Hyaluronsäure (9)
- IL-4 (9)
- Immunfluoreszenz (9)
- Immunisierung (9)
- Innovation (9)
- Instrumentelle Analytik (9)
- Integrine (9)
- Interview (9)
- Iran (9)
- Isolierung <Chemie> (9)
- Jugendliche (9)
- Kapillarelektrophorese (9)
- Knorpel (9)
- Kommunikation (9)
- Koordinationslehre (9)
- Korpus <Linguistik> (9)
- Landsat (9)
- Leber (9)
- Linguistik (9)
- Löslichkeit (9)
- MAPK (9)
- Macrophage (9)
- Magnesiumphosphate (9)
- Magnetische Resonanz (9)
- Magnetismus (9)
- Mehrfachbindung (9)
- Mehrsprachigkeit (9)
- Messenger-RNS (9)
- Metakognition (9)
- Mice (9)
- Molekulare Erkennung (9)
- Monitoring (9)
- Morphologie (9)
- Mukoviszidose (9)
- Myokardprotektion (9)
- NAFLD (9)
- NO (9)
- Nebennierenrindenkrebs (9)
- Neuroinflammation (9)
- Nierentransplantation (9)
- Oberflächenphysik (9)
- Optoelektronik (9)
- PD-1 (9)
- Pathogenese (9)
- Pharmakotherapie (9)
- Photolumineszenzspektroskopie (9)
- Physiologie (9)
- Plasmamembran (9)
- Platelets (9)
- Protein (9)
- Pseudomonas syringae (9)
- Psychoonkologie (9)
- Psychotherapie (9)
- Quantenmechanik (9)
- Radiotherapy (9)
- Rechenzentrum (9)
- Rechtsvergleich (9)
- Regeneration (9)
- Regionalentwicklung (9)
- Revision (9)
- Sarkoidose (9)
- Satellit (9)
- Schmalwand <Arabidopsis> (9)
- Schwindel (9)
- Schüttgut (9)
- Sentinel-1 (9)
- Squaraine (9)
- Staphylococcus (9)
- Stathmin (9)
- Stereoselektive Synthese (9)
- Stressreaktion (9)
- Supply Chain Management (9)
- Syntax (9)
- Systembiologie (9)
- Südafrika (9)
- TWEAK (9)
- Textverstehen (9)
- Theologie (9)
- Tourismus (9)
- Trabekulektomie (9)
- Transplantat (9)
- Transplantat-Wirt-Reaktion (9)
- Transport (9)
- Trypanosoma (9)
- Tumorantigen (9)
- Vakuole (9)
- Vergleich (9)
- Visuelle Aufmerksamkeit (9)
- Wurzel (9)
- X-ray crystallography (9)
- Zellkern (9)
- Zinkselenid (9)
- aggregation (9)
- agriculture (9)
- aldosterone (9)
- antennal lobe (9)
- anxiety disorders (9)
- aromaticity (9)
- atrial fibrillation (9)
- biomechanics (9)
- blood brain barrier (9)
- body size (9)
- bone cement (9)
- cancer therapy (9)
- cell culture (9)
- cell wall (9)
- central nervous system (9)
- chronic heart failure (9)
- collagen (9)
- coronary heart disease (9)
- cystic fibrosis (9)
- decision making (9)
- dendritische Zellen (9)
- dialysis (9)
- dispersal (9)
- earth observation (9)
- electron microscopy (9)
- electrophysiology (9)
- energy (9)
- experimental autoimmune encephalomyelitis (9)
- family (9)
- fatigue (9)
- forest (9)
- gene therapy (9)
- genomics (9)
- glioma (9)
- global change (9)
- glucose (9)
- high energy physics (9)
- hip (9)
- hyaluronic acid (9)
- hydrogel (9)
- impact (9)
- incidence (9)
- inhibitor (9)
- interferon (9)
- mapping (9)
- mechanotransduction (9)
- mesenchymale Stammzellen (9)
- metapopulation (9)
- methylation (9)
- mitosis (9)
- monitoring (9)
- monoklonale Antikörper (9)
- myocardium (9)
- near-infrared spectroscopy (9)
- neurology (9)
- organic chemistry (9)
- organic semiconductors (9)
- pathway (9)
- permeability (9)
- platelet activation (9)
- platelet aggregation (9)
- prognostic factors (9)
- quality assurance (9)
- quantification (9)
- rectal cancer (9)
- reveals (9)
- spinal muscular atrophy (9)
- synapse (9)
- systematic uncertainty (9)
- temperature (9)
- tolerance (9)
- transcription factor (9)
- transient absorption (9)
- transmission (9)
- type 2 diabetes (9)
- vaccine (9)
- walking (9)
- water (9)
- wound healing (9)
- Übersetzung (9)
- ATLAS (8)
- Adhärenz (8)
- Aggregat <Chemie> (8)
- Akt (8)
- Aktiver galaktischer Kern (8)
- Alltagskultur (8)
- Ancistrocladaceae (8)
- Anthocyane (8)
- Antigen (8)
- Antigen CD40 (8)
- Aortenklappenersatz (8)
- Aortenstenose (8)
- Arthroskopie (8)
- Arzneimittelforschung (8)
- Asymmetrie (8)
- Asymmetrische Synthese (8)
- Auge (8)
- Autoaggressionskrankheit (8)
- Autonomer Roboter (8)
- Autophagie (8)
- Bauchspeicheldrüse (8)
- Biotransformation (8)
- Biradikal (8)
- Blimp-1 (8)
- Blutdruck (8)
- Blutstammzelle (8)
- Botanik (8)
- Brain (8)
- Burkina Faso (8)
- CD28 (8)
- CD40 (8)
- CD95 (8)
- COMT (8)
- CT (8)
- Caenorhabditis elegans (8)
- Camponotus floridanus (8)
- Chlamydia (8)
- Compressed Sensing (8)
- Cross-Section (8)
- Cysteinproteasen (8)
- Cytomegalie-Virus (8)
- DLBCL (8)
- Data Mining (8)
- Datenbank (8)
- Deep learning (8)
- Demenz (8)
- Deutschunterricht (8)
- Diagnose (8)
- Diborene (8)
- ERK (8)
- Elektronenspin (8)
- Elektronenspinresonanz (8)
- Emotionsregulation (8)
- Endothelzellen (8)
- Engagement (8)
- Erbrechen (8)
- Europa (8)
- Europe (8)
- Fachdidaktik (8)
- Femtosekundenbereich (8)
- Fibroblasten (8)
- Finite-Elemente-Methode (8)
- Fitness (8)
- Fluoreszenzspektroskopie (8)
- Forschung (8)
- Fußball (8)
- GABA (8)
- Gammastrahlung (8)
- Gedächtnisleistung (8)
- Geschlechtsunterschied (8)
- Gewebe (8)
- Gliom (8)
- HPLC-MS (8)
- Habichtskraut (8)
- Harnwegsinfektion (8)
- Haut (8)
- Hernie (8)
- Herzmuskelkrankheit (8)
- Hochbegabung (8)
- Hubbard-Modell (8)
- Humangenetik (8)
- Hymenoptera (8)
- Hypertrophie (8)
- Hüftgelenk (8)
- IL-10 (8)
- Immunantwort (8)
- Impulsivität (8)
- In vivo (8)
- Indien (8)
- Inklusion (8)
- Juvenile chronische Arthritis (8)
- Keilschrifttext (8)
- Kephalometrie (8)
- Kieferorthopädie (8)
- Kinetik (8)
- Kleinsatellit (8)
- Knockout (8)
- Komposit <Zahnmedizin> (8)
- Kondo-Effekt (8)
- Korrelation (8)
- Kreuzband (8)
- Kristallstruktur (8)
- Landwirtschaft (8)
- Langerhans-Inseln (8)
- Lanthanoide (8)
- Lehre (8)
- Lernautonomie (8)
- Lower Franconia (8)
- Lungenfibrose (8)
- Machine Learning (8)
- Magenbypass (8)
- Makuladegeneration (8)
- Mass (8)
- Meeresschwämme (8)
- Meiosis (8)
- Meningitis (8)
- Meningokokken (8)
- Methode (8)
- Mikroglia (8)
- Mikrokerntest (8)
- Mikrostruktur (8)
- Mitochondrien (8)
- Mobiler Roboter (8)
- Monozyt (8)
- Monozyten (8)
- Multiple myeloma (8)
- N-heterocyclic carbenes (8)
- NSCLC (8)
- Nachsorge (8)
- Naturstoff (8)
- Neugeborenes (8)
- Neutrino (8)
- Oberfläche (8)
- Obesity (8)
- Onkolyse (8)
- Optogenetik (8)
- Organisches Molekül (8)
- Oxylipine (8)
- PD-L1 (8)
- PONV (8)
- Pankreaskarzinom (8)
- Parton distributions (8)
- Pemphigus (8)
- Peptide (8)
- Periphere arterielle Verschlusskrankheit (8)
- Permeabilität (8)
- Persönlichkeit (8)
- Pharmakodynamik (8)
- Photodissoziation (8)
- Photovoltaik (8)
- Platin (8)
- Pollen (8)
- Polycyclische Aromaten (8)
- Protein p53 (8)
- Proteinbindung (8)
- Protonen-NMR-Spektroskopie (8)
- Präkonditionierung (8)
- Psychische Störung (8)
- Pump-Probe-Technik (8)
- Quantendynamik (8)
- Quelle (8)
- Quran (8)
- Radikal <Chemie> (8)
- Raf <Biochemie> (8)
- Raf-Kinasen (8)
- Raman spectroscopy (8)
- Rastertunnelmikroskop (8)
- Rechenzentrum Universität Würzburg (8)
- Regenerative Medizin (8)
- Rekombination (8)
- Retroviren (8)
- Ringöffnungspolymerisation (8)
- Roman (8)
- Röntgen-Photoelektronenspektroskopie (8)
- Salmonella typhimurium (8)
- Schmerzforschung (8)
- Schwämme (8)
- Semimagnetischer Halbleiter (8)
- Siliciumcarbid (8)
- Sozialpsychologie (8)
- Sprachaudiometrie (8)
- Statistik (8)
- Stent (8)
- Stofftransport <Biologie> (8)
- Synthesis (8)
- T cell activation (8)
- T lymphocytes (8)
- T-Zelle (8)
- TDM (8)
- Tabak (8)
- Tagung (8)
- Text Mining (8)
- Textanalyse (8)
- Therapy (8)
- Thrombosis (8)
- Thrombozyten (8)
- Thymus (8)
- Tight junction (8)
- Titan (8)
- Transkriptomanalyse (8)
- Transthorakale Echokardiographie (8)
- Trypanosomiase (8)
- Tumorimmunologie (8)
- UAV (8)
- Ultraschalldiagnostik (8)
- Virusinfektion (8)
- Visualisierung (8)
- Vulnerabilität (8)
- Wirkstofffreisetzung (8)
- Zahnmedizin (8)
- Zeitreihenanalyse (8)
- Zentralnervensystem (8)
- actin cytoskeleton (8)
- adherence (8)
- amyotrophic lateral sclerosis (8)
- analysis of variance (8)
- animal models (8)
- antigen (8)
- astrocytes (8)
- bioinformatics (8)
- body mass index (8)
- borylene (8)
- calcium phosphate (8)
- cardiac surgery (8)
- cardiovascular disease (8)
- cell migration (8)
- central complex (8)
- ceramide (8)
- cerebrospinal fluid (8)
- charge transfer (8)
- chromatin (8)
- chronic pain (8)
- cleft lip and palate (8)
- coagulation (8)
- cognitive impairment (8)
- coherence (8)
- computed tomography (8)
- copper (8)
- cortisol (8)
- cuticular hydrocarbons (8)
- decay (8)
- division of labor (8)
- domain (8)
- dystonia (8)
- electroencephalography (8)
- electronic properties and materials (8)
- electronic structure (8)
- embodiment (8)
- endocytosis (8)
- extinction (8)
- flavonoids (8)
- foamy virus (8)
- forest management (8)
- gephyrin (8)
- hearing (8)
- histology (8)
- immune evasion (8)
- immunology (8)
- implant (8)
- in vivo imaging (8)
- induced pluripotent stem cells (8)
- integrins (8)
- iron (8)
- jet energy scale (8)
- juvenile idiopathic arthritis (8)
- kinematic alignment (8)
- latency (8)
- mHealth (8)
- macrophage (8)
- major depression (8)
- meta-analysis (8)
- methylphenidate (8)
- microenvironment (8)
- microstructure (8)
- monocyte (8)
- mutualism (8)
- neurogenesis (8)
- oncology (8)
- optimal control (8)
- organic solar cells (8)
- pediatrics (8)
- perfusion (8)
- peripheral nervous system (8)
- personality (8)
- pharmacology (8)
- photocatalysis (8)
- phylogeny (8)
- polycyclic aromatic hydrocarbons (8)
- preconditioning (8)
- presence (8)
- protease (8)
- pulmonary hypertension (8)
- questionnaire (8)
- radiation (8)
- radicals (8)
- receptors (8)
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- secretion (8)
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- semiconductor (8)
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- signaling (8)
- sleep (8)
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- sodium (8)
- species richness (8)
- spintronics (8)
- staphylococcus aureus (8)
- structure (8)
- subthalamic nucleus (8)
- susceptibility (8)
- targeted therapy (8)
- thymus (8)
- tool (8)
- 53BP1 (7)
- Adsorption (7)
- Adulte Stammzelle (7)
- Africa (7)
- Aktin (7)
- Aktivierung (7)
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- Akute myeloische Leukämie (7)
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- Blut (7)
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- Bordetella (7)
- Borylenkomplexe (7)
- CMV (7)
- CNS (7)
- Calciumkanal (7)
- Catecholmethyltransferase <Catechol-0-Methyltransferase> (7)
- Charakterisierung (7)
- Charcot-Marie-Tooth (7)
- Chronobiologie (7)
- Chrysomelidae (7)
- Cisplatin (7)
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- Cytoskeleton (7)
- DHEA (7)
- DNS-Doppelstrangbruch (7)
- Darm (7)
- Degradation (7)
- Deutsch als Fremdsprache (7)
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- Dopamine (7)
- Durchblutung (7)
- Durchflusszytometrie (7)
- Dysgnathie (7)
- E-Learning (7)
- ELISA (7)
- ELISPOT (7)
- EMG (7)
- ERK1/2 (7)
- ERN (7)
- Einwandige Kohlenstoff-Nanoröhre (7)
- Eisen (7)
- Elektrokardiogramm (7)
- Embryo (7)
- Endoprothetik (7)
- Ethik (7)
- Exziton-Polariton (7)
- FISH (7)
- Fahrsimulator (7)
- Festkörperoberfläche (7)
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- LEED (7)
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- REMPI (7)
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- SMA (7)
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- Wolfram (7)
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- absorption (7)
- acute ischemic stroke (7)
- acute kidney injury (7)
- acute myeloid leukemia (7)
- adaptation (7)
- adipose tissue (7)
- adolescence (7)
- adolescent (7)
- adult neurogenesis (7)
- adults (7)
- aggression (7)
- algorithm (7)
- allogeneic stem cell transplantation (7)
- anemia (7)
- animal behavior (7)
- antibacterial activity (7)
- antibiotic resistance (7)
- antidepressant (7)
- arabidopsis thaliana (7)
- behaviour (7)
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- butyrate (7)
- caffeine (7)
- capillary electrophoresis (7)
- carbon dioxide (7)
- carcinoma (7)
- cell membranes (7)
- change detection (7)
- chemokine receptor (7)
- classical conditioning (7)
- click chemistry (7)
- cognition (7)
- cognitive control (7)
- cognitive decline (7)
- comparative genomics (7)
- complexes (7)
- crystallization (7)
- cytokinesis (7)
- cytotoxic T cells (7)
- degeneration (7)
- degradation (7)
- diborynes (7)
- diffusion (7)
- distribution (7)
- drought (7)
- drug (7)
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- efficacy (7)
- exciton (7)
- extracellular vesicles (7)
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- genes (7)
- genomic damage (7)
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- health-related quality of life (7)
- heterocycles (7)
- honey bee (7)
- hymenoptera (7)
- hypophosphatasia (7)
- immersion (7)
- immunofluorescence (7)
- immunoprecipitation (7)
- inflammatory bowel disease (7)
- kinase (7)
- knee (7)
- knockout mice (7)
- kolorektales Karzinom (7)
- learning and memory (7)
- lithium (7)
- localization (7)
- locomotion (7)
- luciferase (7)
- melt electrospinning writing (7)
- membrane (7)
- meningitis (7)
- minimally invasive (7)
- modeling (7)
- molecular biology (7)
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- morphology (7)
- motility (7)
- motoneuron (7)
- mri (7)
- multicenter (7)
- myelin (7)
- nanodiamond (7)
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- oxidation (7)
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- pancreas (7)
- pathogens (7)
- pemphigus (7)
- permafrost (7)
- photoinduced electron transfer (7)
- plasmodium falciparum (7)
- population (7)
- potassium (7)
- pre-speech development (7)
- precision medicine (7)
- primary care (7)
- progression (7)
- prospective (7)
- psoriasis (7)
- pulse shaping (7)
- quantum dots (7)
- quantum dynamics (7)
- radioiodine therapy (7)
- radioligand therapy (7)
- random forest (7)
- recovery (7)
- recruitment (7)
- reperfusion (7)
- resilience (7)
- responses (7)
- retina (7)
- risk factor (7)
- rotator cuff (7)
- sRNA (7)
- salt stress (7)
- secondary prevention (7)
- segmentation (7)
- semiconductors (7)
- serotonin transporter (7)
- sex chromosomes (7)
- shear stress (7)
- signaltransduction (7)
- smoking (7)
- social anxiety (7)
- social cognition (7)
- speech audiometry (7)
- superconductivity (7)
- target (7)
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- technology (7)
- telomeres (7)
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- total hip arthroplasty (7)
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- trial (7)
- variability (7)
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- wearable (7)
- Übergewicht (7)
- - (6)
- 18F-FDG (6)
- 2 (6)
- 3D tissue model (6)
- ABA (6)
- ACC (6)
- AMPK (6)
- ANP (6)
- ATLAS <Teilchendetektor> (6)
- Abwehrreaktion (6)
- AdS-CFT-Korrespondenz (6)
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- Frankreich (6)
- Französisch (6)
- Funktion (6)
- Funktionelle NMR-Tomographie (6)
- GC-MS (6)
- GaAs (6)
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- Karriere (6)
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- Keratinozyt (6)
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- Komplexität (6)
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- acid sphingomyelinase (6)
- actinomycetes (6)
- adenosine (6)
- adsorption (6)
- ageing (6)
- alignment (6)
- alkaloids (6)
- alternative splicing (6)
- altitudinal gradient (6)
- anorexia nervosa (6)
- antidepressants (6)
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- hyperekplexia (5)
- hypertrophy (5)
- immunization (5)
- implementation (5)
- in situ hybridization (5)
- in vitro model (5)
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- inhibitors (5)
- innovation (5)
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- integration (5)
- integrin (5)
- intestine (5)
- ion channel (5)
- iron oxide nanoparticles (5)
- irradiation (5)
- jasmonates (5)
- keratinocytes (5)
- kinematics (5)
- knee arthroplasty (5)
- lactate (5)
- land cover (5)
- language acquisition (5)
- larvae (5)
- late enhancement (5)
- lipid rafts (5)
- long-term outcome (5)
- longitudinal study (5)
- loss of heterozygosity (5)
- loudness (5)
- magnetism (5)
- masked priming (5)
- mechanical thrombectomy (5)
- medical education (5)
- medical rehabilitation (5)
- megakaryocyte (5)
- mental disorders (5)
- mesenchymal stem cell (5)
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- microbiology (5)
- microglomeruli (5)
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- modelling (5)
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- neurotrophic factor (5)
- newborn hearing screening (5)
- nickel (5)
- nitric oxide synthase (5)
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- nucleolus (5)
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- patch-clamp (5)
- pathogenicity (5)
- peptide (5)
- persistence (5)
- pharmacokinetic (5)
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- phylogenetic analysis (5)
- plants (5)
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- porin (5)
- power (5)
- predictors (5)
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- protein binding (5)
- protein expression (5)
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- psychological distress (5)
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- quality (5)
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- specificity (5)
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- spin (5)
- spinal cord (5)
- splicing (5)
- stability (5)
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- subtypes (5)
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- xx (5)
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- γ-H2AX (5)
- --- (4)
- 3D Printing (4)
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- 3D reconstruction (4)
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- ACL (4)
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- Johns Hopkins School of Medicine (18)
- Fraunhofer-Institut für Silicatforschung ISC (8)
- IZKF Nachwuchsgruppe Geweberegeneration für muskuloskelettale Erkrankungen (7)
- Akademie der Wissenschaften und der Literatur, Mainz (6)
- DFG Forschungsgruppe 2757 / Lokale Selbstregelungen im Kontext schwacher Staatlichkeit in Antike und Moderne (LoSAM) (6)
- Clinical Trial Center (CTC) / Zentrale für Klinische Studien Würzburg (ZKSW) (5)
- Helmholtz Institute for RNA-based Infection Research (HIRI) (5)
- Johns Hopkins University School of Medicine (5)
- Universität Leipzig (5)
ResearcherID
- B-1911-2015 (1)
- B-4606-2017 (1)
- C-2593-2016 (1)
- D-1221-2009 (1)
- D-1250-2010 (1)
- D-3057-2014 (1)
- I-5818-2014 (1)
- J-8841-2015 (1)
- M-1240-2017 (1)
- N-2030-2015 (1)
Die Dissertation befasst sich mit der Reaktivität von 1,2-Bis(dichlorboryl)benzol. Im ersten Kapitel wird auf die Problematik bei dessen Synthese eingegangen. Der zweite Teil der Arbeit befasst sich mit der Bildung von entsprechenden Boran-Addukten mit verschiedenen Lewis-Basen. Das dritte Kapitel beschreibt die Synthese eines neuartigen, vollständig ungesättigten 1,2-Diboretdiradikals, welches durch die schrittweise Reduktion des 1,2-[(CAAC)BCl2]2-Benzols erhalten wurde. Darüber hinaus konnte bei dieser schrittweisen Reduktion ebenfalls das einfache Borylradikal, das nicht-cyclische Diradikal und das dianionische gespannte C2B2-Ringsystem erhalten werden. Anfängliche Reaktivitätsstudien zum 1,2-Diboretdiradikal zeigen zudem, dass die B-B-Bindung durch Umsetzung mit Kohlenstoffmonoxid gespalten und so ein Bisborylen dargestellt werden kann. Im vierten Kapitel konnte das 1,2-Bis(dichlorboryl)benzol durch Transmetallierungsreaktionen zu verschiedenen, sich in ihren Eigenschaften stark unterscheidenden, Verbindungen umgesetzt werden. So konnte das fluoreszierende ortho-phenylenverbrückte Bis-9-Borafluoren erhalten werden, aus welchem durch Wärmezufuhr das ebenfalls fluoreszierendes diboraanthracenartige Umlagerungsprodukt gewonnen werden konnte. Beide Verbindungen wurden auf ihre photophysikalischen und elektrochemischen Eigenschaften untersucht. Weiterhin konnten polycyclische Boracyclen mit C10B2-Gerüst erhalten werden, bei welchen instantan die selektive Bildung von zwei chiralen Zentren über eine Vielzahl an B-C-Bindungsbrüchen und -knüpfungen beobachtet wurde. Zuletzt konnte ein thermisch empfindliches, potentiell explosives Azid-verbrücktes Azidoboran dargestellt werden, bei welchem eine Staudinger-artige Reaktivität beobachtet werden konnte.
Die idiopathische Lungenfibrose (IPF) stellt eine chronische Krankheit mit einer schlechten Prognose dar. Die Erkrankung zeichnet sich durch ein dysfunktionales Alveolarepithel, die Formation von α-smooth muscle actin (α-SMA)-positiven Myofibroblasten, eine starke Kollagendeposition sowie eine fehlgeleitete Inflammation aus. In der Vermittlung dieser pro-fibrotischen Effekte spielt das Zytokin transforming growth factor β (TGF-β) eine Schlüsselrolle. Aufgrund des tödlichen Verlaufs der IPF und der limitierten Therapieoptionen ist die Entdeckung neuer Behandlungsansätze erforderlich.
Der NO/cGMP-Signalweg ist in der Modulation grundlegender physiologischer Vorgänge wie der Blutdruckregulation und der Peristaltik involviert. Hierbei spielt die NO-sensitive Guanylyl-Cyclase (NO-GC) als NO-Rezeptor eine fundamentale Rolle. In der Lunge wird die NO-GC in glatten Muskelzellen und Perizyten exprimiert. Während das Enzym in glatten Muskelzellen die Relaxation der glatten Muskulatur vermittelt, reguliert die NO-GC in Perizyten die Angiogenese, die Kapillardurchlässigkeit und den Blutfluss. Neben den physiologischen Aufgaben wurden anti-fibrotische sowie anti-inflammatorische Effekte der NO-GC in Herz, Leber, Niere und Haut beschrieben.
Daher wurde im Rahmen dieser Arbeit die NO-GC auf eine anti-fibrotische und anti-inflammatorische Bedeutung in der Lungenfibrose der Maus überprüft. Hierzu wurden Wildtyp- (WT) und globale NO-GC-Knockout-Mäuse (GCKO) untersucht. Die Fibrose wurde durch einmalige, orotracheale Bleomycin-Gabe induziert und zu unterschiedlichen Zeitpunkten (Tag 7 und 21) untersucht. Unbehandelte (Tag 0) Tiere dienten als Kontrolle. Im ersten Teil dieser Arbeit wurde die NO-GC auf eine anti-fibrotische Wirkung untersucht. Mittels Immunfluoreszenz wurde das Verhalten der α-SMA-positiven Myofibroblasten in den platelet-derived growth factor receptor β (PDGFRβ)-positiven fibrotischen Regionen untersucht. Der Kollagengehalt wurde mithilfe eines Hydroxyprolin-Kollagenassays ermittelt. Die untersuchten Fibrose-Kriterien waren in beiden Genotypen an Tag 21 stärker ausgeprägt als an Tag 7. An Tag 21 konnten im GCKO mehr α-SMA-positive Myofibroblasten, ausgeprägtere PDGFRβ-positive fibrotische Areale und ein höherer Kollagengehalt als im WT festgestellt werden. Zudem zeigten die GCKO-Tiere ein schlechteres Überleben als WT-Mäuse. Diese Ergebnisse wiesen auf eine überschießende fibrotische Antwort im GCKO und somit auf eine anti-fibrotische Wirkung der NO-GC in der Bleomycin-induzierten Lungenfibrose hin. Dass an Tag 21 die Fibrose im GCKO stärker ausfiel als im WT, konnte mit dem signifikant höheren TGF-β-Gehalt in der bronchoalveolären Lavageflüssigkeit (BALF) im GCKO erklärt werden. Das Fehlen der NO-GC im GCKO könnte zu einem Wegfall der Inhibierung der TGF-β-vermittelten, pro-fibrotischen Effekte durch die NO-GC führen. Weitere Studien sind erforderlich, um die Hypothese zu belegen und zugrundeliegende Mechanismen aufzuklären.
Die de novo Entstehung von Myofibroblasten, die maßgeblich an der Kollagensynthese beteiligt sind, stellt ein entscheidendes Fibrose-Merkmal dar. Umso bedeutender ist die Identifikation zweier Myofibroblasten-Subtypen, die sich in Lokalisation, NO-GC-Expression und Herkunft unterscheiden: (1) interstitielle, NO-GC-positive Myofibroblasten, die von Perizyten abstammen und Kollagen Typ I produzieren, und (2) intra-alveoläre, NO-GC-negative Myofibroblasten, deren Ursprung noch nicht abschließend geklärt ist. Die Anwesenheit beider Myofibroblasten-Typen konnte zu beiden untersuchten Zeitpunkten nach Bleomycin-Gabe bestätigt werden. Die NO-GC-Expression der Alveolarwand-ständigen Myofibroblasten, deren Abstammung von NO-GC-positiven Perizyten sowie deren dauerhafte Präsenz sprechen für eine relevante Rolle der NO-GC in der murinen Lungenfibrose. In weiteren Untersuchungen müssen die exakten Funktionen und spezifische Marker der Myofibroblasten-Subtypen identifiziert werden.
Im zweiten Teil dieser Arbeit wurde die NO-GC auf anti-inflammatorische Effekte in der Bleomycin-induzierten Lungenfibrose untersucht. Mittels HE-Färbung und Immunfluoreszenz wurden lymphozytäre Infiltrate an Tag 21 im GCKO festgestellt, was auf einen modulatorischen Einfluss der NO-GC auf das Immunsystem hindeutete. An Tag 21 wurden in der BALF von GCKO-Tieren signifikant mehr Gesamtimmunzellen, Lymphozyten und neutrophile Granulozyten als im WT gezählt, was auf eine starke Einwanderung von Immunzellen und somit auf eine ausgeprägte Entzündung in GCKO-Lungen hinwies. Folglich könnte die NO-GC eine anti-inflammatorische Rolle über die Regulation der Immigration von Immunzellen in der Bleomycin-induzierten Lungenfibrose spielen. In der Literatur werden pro- und anti-fibrotische Effekte der Immunzellen in der murinen Lungenfibrose diskutiert. Durch Korrelationsanalysen wurde ein positiver Zusammenhang zwischen der Gesamtimmunzellzahl und der TGF-β-Konzentration an Tag 21 festgestellt. In verschiedenen Studien wurde ein pro-fibrotischer Einfluss der Immunzellen über die Aktivierung/Sekretion von TGF-β beschrieben. Die Abwesenheit der NO-GC im GCKO könnte also über die verstärkte Immigration von Immunzellen in einem erhöhten TGF-β-Gehalt resultieren und so zu einer überschießenden fibrotischen Reaktion an Tag 21 führen. Auf welche Weise die NO-GC die Einwanderung der Immunzellen in der Bleomycin-induzierten Lungenfibrose beeinflusst, muss in weiteren Studien untersucht werden. Zusammenfassend deuten die Daten dieser Arbeit auf eine anti-inflammatorische und anti-fibrotische Rolle der NO-GC in der Lungenfibrose der Maus hin.
Ischemia-reperfusion injury (I/R injury) is a common complication in ischemic stroke (IS) treatment, which is characterized by a paradoxical perpetuation of tissue damage despite the successful re-establishment of vascular perfusion. This phenomenon is known to be facilitated by the detrimental interplay of platelets and inflammatory cells at the vascular interface. However, the spatio-temporal and molecular mechanisms underlying these cellular interactions and their contribution to infarct progression are still incompletely understood. Therefore, this study intended to clarify the temporal mechanisms of infarct growth after cerebral vessel recanalization. The data presented here could show that infarct progression is driven by early blood-brain-barrier perturbation and is independent of secondary thrombus formation. Since previous studies unravelled the secretion of platelet granules as a molecular mechanism of how platelets contribute to I/R injury, special emphasis was placed on the role of platelet granule secretion in the process of barrier dysfunction. By combining an in vitro approach with a murine IS model, it could be shown that platelet α-granules exerted endothelial-damaging properties, whereas their absence (NBEAL2-deficiency) translated into improved microvascular integrity. Hence, targeting platelet α-granules might serve as a novel treatment option to reduce vascular integrity loss and diminish infarct growth despite recanalization.
Recent evidence revealed that pathomechanisms underlying I/R injury are already instrumental during large vessel occlusion. This indicates that penumbral tissue loss under occlusion and I/R injury during reperfusion share an intertwined relationship. In accordance with this notion, human observational data disclosed the presence of a neutrophil dominated immune response and local platelet activation and secretion, by the detection of the main components of platelet α-granules, within the secluded vasculature of IS patients. These initial observations of immune cells and platelets could be further expanded within this thesis by flow cytometric analysis of local ischemic blood samples. Phenotyping of immune cells disclosed a yet unknown shift in the lymphocyte population towards CD4+ T cells and additionally corroborated the concept of an immediate intravascular immune response that is dominated by granulocytes. Furthermore, this thesis provides first-time evidence for the increased appearance of platelet-leukocyte-aggregates within the secluded human vasculature. Thus, interfering with immune cells and/or platelets already under occlusion might serve as a potential strategy to diminish infarct expansion and ameliorate clinical outcome after IS.
Virtual humans (VHs) hold immense potential for collaboration in social virtual reality (VR). As VR technology advances, it's vital to assess the psychological effects on VH trust and user privacy to build meaningful social interactions in VR. In social VR, users must be able to trust the VHs they interact with as they navigate through socio-cultural activities. The evaluation of trustworthiness in VHs profoundly impacts interaction quality and user willingness to engage. Conversely, untrustworthy VHs can harm user experiences, privacy, and VR engagement. To address this, we conducted immersive VR studies, exploring how psychological factors influence user's VH trust evaluation under various psychological conditions. This research is pivotal for developing strategies to enhance user privacy, establish secure VR environments, and create a foundation of trust that supports immersive socio-cultural experiences in VR.
To date, there are no established interpersonal trust measurement tools specifically for VHs in VR. In study 1 (the familiarity study) of the current thesis the VR-adjusted version of the social conditioned place preference paradigm (SCPP) by Kiser et al., (2022) was identified as a potential trust measurement tool. We tested whether the familiarity of a VH influenced trust as measured with the SCPP paradigm and other self-defined outcome measures, in a Computer Augmented Virtual Environment (CAVE). The CAVE is a VR system that combines immersive VR with real-world elements. It consists of a room-sized space where the walls are used as projection screens to display virtual scenes and objects. In this within - subject design (n = 20), half of the participants were familiarized with one VH and tasked to explore and interact in a realistic looking virtual art museum environment. The participant’s evaluation of the VH’s trustworthiness was measured as well as their subsequent trust behaviours. Results revealed no significant differences in the evaluation of the VH’s trustworthiness nor any behavioural differences between conditions. The findings of the impact of a VH’s familiarity on trust is inconclusive due to the major limitations of the paradigm. We concluded that the SCPP paradigm needs further validation and the proposed proxies of trust need to be re-evaluated. The findings were considered in the following study.
The virtual maze paradigm design of Hale, (2018) was identified as a potential trust measurement tool, however several limitations are associated with its use to measure trust in VR. In study 2 (a validation study), improvements were made to the virtual maze paradigm of Hale, (2018) and a variant of this paradigm was implemented. We conducted a validation study with 70 participants in a between-subject design with VH trustworthiness as the between-subject factor. Participants wore a head-mounted display (HMD), to deliver an immersive VR experience. In our version of the virtual maze, it was the task of the users (the trustors) to navigate through a maze in VR, where they could interact with a VH (the trustee). They could choose to ask for advice and follow the advice from the VH if they wanted to. The number of times participants asked and followed advice and the time it took to respond to the given advice served as behavioural proxies/measures of trust. The two conditions (trustworthy vs. untrustworthy) did not differ in the content of the advice but in the appearance, tone of voice and engagement of the trustees (allegedly an avatar controlled by other participants). Results indicated that the experimental manipulation was successful, as participants rated the VH as more trustworthy in the trustworthy condition compared with the VH in the untrustworthy condition. Importantly, this manipulation affected the trust behaviour of participants, who, in the trustworthy condition, asked for advice and followed advice more often, indicating that the paradigm is sensitive to differences in VH’s trustworthiness. Thus, our paradigm can be used to measure differences in interpersonal trust towards VHs and may serve as a valuable research tool for researchers who study trust in VR. Therefore, study 2 fills the gap in the literature, for an interpersonal trust measurement tool specifically for VHs in VR.
Two experimental studies, with a sample size of 50 participants each, utilized the virtual maze paradigm where participants entered 12 rooms under different conditions. We examined the influence of cognitive load (CL) on trust towards VH in VR in study 3 (Cognitive load study), and the influence of emotional affect (Emotional affect study) on trust towards VH in VR in study 4 (EA study). In both studies, we assessed participant’s evaluation of a VH’s trustworthiness, along with three behavioural indicators of trust in the maze task: 1) frequency of advice asked, 2) frequency of advice followed, and 3) the time taken by participants to execute the received advice. In study 3, the CL was manipulated with the auditory 1-back task in the high cognitive load condition (HCL). In study 4, the Autobiographical Emotional Memory Task (AEMT) was used to manipulate the EA of participants in the negative emotional affect (NEA) condition. As an additional manipulation, while participants were immersed in VR, they were exposed to 12 negative pictures and sounds that was presented simultaneously to strengthen the initial manipulation. The manipulation of the within-subject factors (CL and EA) was successful in both studies, as significant differences between conditions were observed in both studies (higher CL in the HCL condition and a more negative EA in the NEA condition). However, only CL influenced participant’s evaluation of the VH’s trustworthiness. The VH were evaluated as significantly more trustworthy after the HCL condition. Despite the difference in trust evaluation, there was no difference in advice asking or following. Participants in study 4 asked and followed advice due to their trust in the VH and asked and followed advice equally often in both conditions. Importantly, significant differences were observed in the participants response times in both studies. In study 3 during the HCL condition participants followed advice quicker. The order in which the conditions were presented influenced the experience of CL. Participants experienced higher levels of CL and responded to advice significantly faster when low cognitive load (LCL) was presented as the first condition compared with LCL as the second condition. In study 4 participants in the NEA condition followed advice slower similar to the findings of study 3. The order in which the conditions were presented had a significant effect on the EA. Participants asked and followed advice less when the NEA condition was presented first compared with when it is presented second. Possible explanations for the findings are discussed in the thesis.
Overall, this thesis offers a novel tool for trust measurement (the virtual maze paradigm) and contributes to understanding the role of psychological factors in trust towards virtual humans in virtual reality.
Wie diese und auch weitere Studien gezeigt haben, ist die Prävalenz der PatientInnen mit einer LVEF zwischen 36-49% und einem begleitenden LSB nicht zu unterschätzen. Ziel der vorliegenden Arbeit war es zum einen, zu untersuchen, ob ein LSB einen signifikanten Einfluss auf die Mortalität und kardiovaskuläre Sterblichkeit bei sowohl HFmrEF- als auch HFrEF-PatientInnen hat und zum anderen, ob es einen Zusammenhang zwischen einem LSB und der Nierenfunktion gibt.
Methoden: Unsere retrospektive Studie untersuchte 2152 PatientInnen mit echokardiographisch bestätigter HI, die sich zwischen 2009 und 2017 in der Universitätsklinik Würzburg vorstellten. Das mittleres Alter betrug 69 Jahre (±13 Jahre) und 72,5% der HFmrEF-Gruppe und 75,7% der HFrEF-Gruppe waren männlich. Jeder Patient erhielt ein durchschnittliches Follow-Up-von 25 Monaten (13-39 Monate). Zunächst wurden beide Gruppen direkt bezüglich des Vorhandenseins eines LSB miteinander verglichen. Die mit in die Studie aufgenommenen PatientInnen wurden anschließend in zwei größere Gruppen eingeteilt. Dabei konnten 1011 PatientInnen der HFmrEF-Gruppe zugeteilt werden, 125 PatientInnen mit und 886 ohne LSB. In der HFrEF-Gruppe befanden sich 1141 PatientInnen, 281 mit und 860 ohne LSB. Die HFrEF-Gruppe wurde zudem erneut hinsichtlich der Nierenfunktion aufgeteilt. Von den 1141 HFrEF-PatientInnen wurden 648 in die Gruppe mit erhaltener Nierenfunktion aufgeteilt und 493 HFrEF-PatientInnen in die Gruppe mit eingeschränkter Nierenfunktion.
Ergebnisse: In der HFmrEF-Subgruppe zeigten sich keine relevanten Auswirkungen durch das Vorhandensein oder Fehlen eines LSB auf die Gesamtmortalität und die kardiovaskuläre Mortalität. Auch in der HFrEF-Gruppe hatte das Vorhandensein eines LSB keine signifikante Relevanz für die Gesamtmortalität (34,5% vs. 31,6%, p=0,165). Das Risiko an einem kardiovaskulären Ereignis zu versterben war allerdings für HFrEF-PatientInnen mit LSB deutlich höher als für PatientInnen ohne LSB (86,3% vs. 82,2%, p=0,041). Nach Adjustierung von Alter, Geschlecht, BMI, KHK sowie Schlaganfall war der Einfluss eines LSB nicht mehr signifikant. Es zeigte sich jedoch, dass HFrEF-PatientInnen mit LSB und normaler Nierenfunktion eine mehr als zweifach erhöhte kardiovaskuläre Sterblichkeit haben (8,2% vs. 16,2%, p=0,002). Nach dieser Feststellung wurde gesondert auf weitere Komorbiditäten als mögliche Einflussfaktoren eingegangen. Unabhängig von dem Vorhandensein eines LSB hatten PatientInnen mit eingeschränkter Nierenfunktion eine deutlich erhöhte Mortalität verglichen mit PatientInnen ohne Nierendysfunktion. Hingegen beeinflusste ein LSB bei HFrEF-PatientInnen mit erhaltener Nierenfunktion das Überleben deutlich. LSB-PatientInnen mit erhaltener Nierenfunktion verstarben häufiger an einem kardiovaskulären Ereignis als HFrEF-PatientInnen mit normaler Nierenfunktion ohne LSB (86,3% vs. 82,2%, p=0,041). Um diese Untersuchung weiter zu vertiefen, wurde die HFrEF-Gruppe anhand der EF erneut in drei Subgruppen eingeteilt. Hierbei konnte eindeutig festgestellt werden, dass PatientInnen mit LSB, erhaltener Nierenfunktion und einer BLEF ≤ 30% vor Adjustierung von Alter, Geschlecht, BMI, Schlaganfall und KHK signifikant häufiger kardiovaskulär verstarben als PatientInnen ohne LSB. Des Weiteren fiel besonders die Subgruppe mit einer BLEF zwischen 36 und 39% auf. Denn vor Adjustierung der kardiovaskulären Mortalität zeigte sich ein signifikant erhöhte Mortalitätsrate für PatientInnen mit LSB. Nach Adjustierung der Einflussfaktoren war der prozentuale Anteil immer noch erhöht, lediglich nicht mehr signifikant. Somit gibt diese Studie den Anreiz, weitere prospektive Studien mit einem größeren Stichprobenumfang durchzuführen, um diese Annahme zu bestätigen. Zudem sollte in weiteren Studien untersucht werden, ob speziell für HFrEF-PatientInnen mit LSB und einer EF zwischen 36 und 39% eine CRT einen positiven therapeutischen Effekt bringen könnte.
Die Aufmerksamkeitsdefizit-/Hyperaktivitätsstörung (ADHS) gehört weltweit zu den bedeutendsten psychiatrischen Erkrankungen des Kinder- und Jugendalters. Die Pathomechanismen sind aktuell noch nicht vollständig geklärt, wobei es deutliche Hinweise auf hirnorganische Veränderungen gibt. Die transkranielle Sonographie stellt eine nicht-invasive Methode dar, strukturelle Unterschiede tiefer Hirnstrukturen zu untersuchen. Bereits in vorangegangenen Studien konnte mit der Methode eine Veränderung der Echogenität der Substantia nigra (SN) bei Kindern mit ADHS im Vergleich zu gesunden Kontrollprobanden nachgewiesen werden. In dieser Studie sollen nun die möglichen physiologischen Hintergründe der erhöhten Echogenität der Substantia Nigra in Zusammenschau mit bildgebenden Verfahren betrachtet werden. Hierzu wurde in der vorliegenden multimodalen Studie bei 20 männlichen Kindern mit ADHS im Alter zwischen 8 und 12 Jahren eine transkranielle Ultraschalluntersuchung (TCS) zur Bestimmung der echogenen Fläche der Substantia Nigra sowie ein neuromelaninsensitives cMRT zur Bestimmung des neuromelaninassoziierten Volumens der SN, sowie des neuromelaninassoziierten Kontrastes SN/Cb durchgeführt. Als Kennwerte des peripheren Eisenhaushalts wurden die Konzentrationen von Eisen, Ferritin und Transferrin im Blut bestimmt. In die Auswertung gingen außerdem die Stärke der ADHS-Symptomatik (Strength and Difficulties Questionaire, SDQ; Fremdbeurteilungsbogen bei ADHS, FBB-ADHS), die kognitive Begabung (über CFT-20-R) und das Alter der Probanden ein. Psychiatrische Komorbidität wurde mit Hilfe der Child Behaviour Checklist (CBCL) erhoben.
Plasmonic nanostructures are considered promising candidates for essential components of integrated quantum technologies because of their ability to efficiently localize broad-band electromagnetic fields on the nanoscale. The resulting local near field can be understood as a spatial superposition of spectrally different plasmon-polariton modes due to the spectrally broad optical excitation, and thus can be described as a classical wave packet. Since plasmon polaritons, in turn, can transmit and receive non-classical light states, the exciting question arises to what extent they have to be described as quantum mechanical wave packets, i.e. as a superposition of different quantum states.
But how to probe, characterize and eventually manipulate the quantum state of such plasmon polaritons? Up to now, probing at room temperatures relied completely on analyzing quantum optical properties of the corresponding in-going and out-going far-field photon modes. However, these methods so far only allow a rather indirect investigation of the plasmon-polariton quantum state by means of transfer into photons. Moreover, these indirect methods lack spatial resolution and therefore do not provide on-site access to the plasmon-polariton quantum state. However, since the spectroscopic method of coherent two-dimensional (2D) nanoscopy offers the capability to follow the plasmon-
polariton quantum state both in Hilbert space and in space and time domain a complete characterization of the plasmon polariton is possible.
In this thesis a versatile coherent 2D nanoscopy setup is presented combining spectral tunability and femtosecond time resolution with spatial resolution on the nanometer scale due to the detection of optically excited nonlinear emitted electrons via photoemission electron microscopy (PEEM). Optical excitation by amplitude- and phase-shaped, systematically-modified and interferometric-stable multipulse sequences is realized, and characterized via Fourier-transform spectral interferometry (FTSI). This linear technique enables efficient data acquisition in parallel to a simultaneously performed experiment. The full electric-field reconstruction of every generated multipulse sequence is used to analyze the effect of non-ideal pulse sequences on the two-dimensional spectral data of population-based multidimensional spectroscopy methods like, e.g., the coherent 2D nanoscopy applied in this thesis. Investigation of the spatially-resolved nonlinear electron emission yield from plasmonic gold nanoresonators by coherent 2D nanoscopy requires a quasi-particle treatment of the addressed plasmon-polariton mode and development of a quantum model to adequately describe the plasmon-assisted multi-quantum electron emission from nanostructures. Good agreement between simulated and experimental data enables to connect certain spectral features to superpositions of non-adjacent plasmon-polariton quantum states, i.e, non-adjacent occupation-number states of the underlying quantized, harmonic oscillator, thus direct probing of the plasmon-polariton quantum wave packet at the location of the nanostructure.
This is a necessary step to locally control and manipulate the plasmon-polariton quantum state and thus of general interest for the realization of nanoscale quantum optical devices.
Das Leitmotiv „Nachhaltigkeit“ durchdringt mit ungebrochener Dynamik das Recht in seiner nationalen, supranationalen und internationalen Ausgestaltung und erweist sich als bestimmendes Momentum der Rechtsetzung. So auch im Rahmen der europäischen Regulierung zu Sustainable Finance, welche die klimaneutrale Transformation der Realwirtschaft über das Vehikel nachhaltiger Finanzprodukte zum Ziel hat. Dieser Aufsatz untersucht nach einem kurzen Abriss zur Zielsetzung und Ausgangslage des Rechtsrahmens dessen einzelne Maßnahmen, namentlich die Offenlegungs-Verordnung (VO), Taxonomie-VO, Benchmark-VO und Green-Bond-VO, unter Berücksichtigung der regulatorischen Leitprinzipien und der rechtlichen Ausgestaltung des Nachhaltigkeitsbegriffs im Verhältnis zu ESG und Sustainable Finance. Dabei wird sich zeigen, dass zwar die Summe der Rechtsakte ein substanzielles Umdenken auf dem Kapitalmarkt zu etablieren vermag, die zugrunde liegende rechtliche Ausgestaltung von „Nachhaltigkeit“ jedoch weder trennscharf noch kongruent gelingt. Alternativ hierzu wird ein kontextabhängiger Definitionsansatz präsentiert, um der überbordenden Regulierung vermöge eines genuin europäischen Nachhaltigkeitskontext entgegenzuwirken und den mit nachhaltigen Finanzprodukten verbundenen Erwartungslagen besser Rechnung zu tragen.
Band 71 der Keilschrifttexte aus Boghazköi setzt die Publikation der keilschriftlichen Funde aus der Hethiterhauptstadt Boğazköy-Ḫattuša fort. Lieferungen 1–6 enthalten die Textfunde der Grabungskampagnen 2017 (Nr. 26–36), 2018 (Nr. 39–82), 2019 (Nr. 86–95), 2020 (Nr. 96–101), 2021 (Nr. 102–10), 2022 (Nr. 125–41), 2023 (Nr. 142–72) sowie Nachträge zu früheren Heften (Nr. 1–25, 37–38, 83–85, 111–24, 173–74).
The RNAs of many viruses contain a frameshift stimulatory element (FSE) that grants access to an alternate reading frame via −1 programmed ribosomal frameshifting (PRF). This −1PRF is essential for effective viral replication. The −1PRF efficiency relies on the presence of conserved RNA elements within the FSE, such as a slippery sequence, spacer, and a downstream secondary structure – often a hairpin or a pseudoknot. The PRF efficiency is also affected by trans-acting factors such as proteins, miRNAs and metabolites. The interactions of these factors with the RNA and the translation machinery have not yet been completely understood. Traditional ensemble methods used previously to study these events focus on the whole population of molecular species. This results in innate averaging of the molecular behavior and a loss of heterogeneity information.
Here, we first established the experimental workflow to study the RNA structures and the effect of potential trans-acting factors using single-molecule force spectroscopy technique, optical tweezers. Additionally, to streamline the data analysis, we developed an algorithm for automatized data processing.
Next, we harnessed this knowledge to study viral RNA elements responsible for stimulation of PRF and how the presence of trans-acting factors affects the RNA behavior. We further complemented these single-molecule structural data with ensemble functional assays to gain a complex view on the dynamics behind the programmed ribosomal frameshifting.
Specifically, two different viral RNA elements have been studied in the presented work. First, the dynamics of SARS-CoV-2 FSE and the role of extended sequences have been explored. Then, the mode of action of the host-encoded trans-acting factor ZAP-S inhibition of SARS-CoV-2 PRF has been examined. Finally, the mechanism of the trans-acting viral factor induced PRF in Encephalomyocarditis virus (EMCV) has been uncovered.
Biological systems are in dynamic interaction. Many responses reside in the core concepts of biological systems interplay (competition and cooperation). In infection situation, the competition between a bacterial system and a host is shaped by many stressors at spatial and temporal determinants. Reactive chemical species are universal stressors against all biological systems since they potentially damage the basic requirements of these systems (nucleic acids, proteins, carbohydrates, and lipids). Either produced endogenously or exogenously, reactive chemical species affect the survival of pathogens including the gram-positive
Staphylococcus aureus (S. aureus). Therefore, bacteria developed strategies to overcome the toxicity of reactive species.
S. aureus is a widely found opportunistic pathogen. In its niche, S. aureus is in permanent contact with surrounding microbes and host factors. Deciphering the deterministic factors
in these interactions could facilitate pinpointing novel bacterial targets. Identifying
the aforementioned targets is crucial to develop new strategies not only to kill the pathogenic organisms but also to enhance the normal flora to minimize the pathogenicity and virulence of potential pathogens. Moreover, targeting S. aureus stress response can be used
to overcome bacterial resistance against host-derived factors. In this study, I identify a novel
S. aureus stress response factor against reactive electrophilic, oxygen, and hypochlorite species to better understand its resilience as a pathogen.
Although bacterial stress response is an active research field, gene function is a current bottleneck in characterizing the understudied bacterial strategies to mediate stress conditions. I aimed at understanding the function of a novel protein family integrated
in many defense systems of several biological systems.
In bacteria, fungi, and plants, old yellow enzymes (OYEs) are widely found. Since the first isolation of the yellow flavoprotein, OYEs are used as biocatalysts for decades to reduce activated C=C bonds in α,β-unsaturated carbonyl compounds. The promiscuity
of the enzymatic catalysis is advantageous for industrial applications.
However, the physiological function of OYEs, especially in bacteria, is still puzzling.
Moreover, the relevance of the OYEs in infection conditions remained enigmatic.
Here, I show that there are two groups of OYEs (OYE flavin oxidoreductase, OfrA and OfrB) that are encoded in staphylococci and some firmicutes. OfrA (SAUSA300_0859) is more conserved than OfrB (SAUSA300_0322) in staphylococci and is a part of the staphylococcal core genome.
A reporter system was established to report for ofrA in S. aureus background.
The results showed that ofrA is induced under electrophilic, oxidative, and hypochlorite stress. OfrA protects S. aureus against quinone, methylglyoxal, hydrogen peroxide,
and hypochlorite stress. Additionally, the results provide evidence that OfrA supports
thiol-dependent redox homeostasis. At the host-pathogen interface, OfrA promotes S. aureus fitness in murine macrophage cell line. In whole human blood, OfrA is involved in S. aureus survival indicating a potential clinical relevance to bacteraemia.
In addition, ofrA mutation affects the production of the virulence factor staphyloxanthin via the upper mevalonate pathway. In summary, decoding OfrA function and its proposed mechanism of action in S. aureus shed the light on a conserved stress response within multiple organisms.
Biofabrication technologies must address numerous parameters and conditions to reconstruct tissue complexity in vitro. A critical challenge is vascularization, especially for large constructs exceeding diffusion limits. This requires the creation of artificial vascular structures, a task demanding the convergence and integration of multiple engineering approaches. This doctoral dissertation aims to achieve two primary objectives: firstly, to implement and refine engineering methods for creating artificial microvascular structures using Melt Electrowriting (MEW)-assisted sacrificial templating, and secondly, to deepen the understanding of the critical factors influencing the printability of bioink formulations in 3D extrusion bioprinting.
In the first part of this dissertation, two innovative sacrificial templating techniques using MEW are explored. Utilizing a carbohydrate glass as a fugitive material, a pioneering advancement in the processing of sugars with MEW with a resolution under 100 microns was made. Furthermore, by introducing the “print-and-fuse” strategy as a groundbreaking method, biomimetic branching microchannels embedded in hydrogel matrices were fabricated, which can then be endothelialized to mirror in vivo vascular conditions.
The second part of the dissertation explores extrusion bioprinting. By introducing a simple binary bioink formulation, the correlation between physical properties and printability was showcased. In the next step, employing state-of-the-art machine-learning approaches revealed a deeper understanding of the correlations between bioink properties and printability in an extended library of hydrogel formulations.
This dissertation offers in-depth insights into two key biofabrication technologies. Future work could merge these into hybrid methods for the fabrication of vascularized constructs, combining MEW's precision with fine-tuned bioink properties in automated extrusion bioprinting.
The slowly activating vacuolar SV/TPC1 channel is ubiquitously expressed in plants and provides a large cation conductance in the vacuolar membrane. Thereby, monovalent (K+, Na+) and in principle also divalent cations, such as Ca2+, can pass through the channel. The SV/TPC1 channel is activated upon membrane depolarization and cytosolic Ca2+ but inhibited by luminal calcium. With respect to the latter, two luminal Ca2+ binding sites (site 1 Asp240/Asp454/Glu528, site 2 Glu239/Asp240/Glu457) were identified to coordinate luminal Ca2+. In this work, the characteristics of the SV/TPC1 channels in terms of regulation and function were further elucidated, focusing on the TPC1s of Arabidopsis thaliana and Vicia faba. For electrophysiological analysis of the role of distinct pore residues for channel gating and luminal Ca2+ sensing, TPC1 channel variants were generated by site-directed mutagenesis and transiently expressed as eGFP/eYFP-fusion constructs in Arabidopsis thaliana mesophyll protoplasts of the TPC1 loss-of-function mutant attpc1-2.
1. As visualized by confocal fluorescence laser-scanning microscopy, all AtTPC1 (WT, E605A/Q, D606N, D607N, E605A/D606N, E605Q/D606N/D607N, E457N/E605A/D606N) and VfTPC1 channel variants (WT, N458E/A607E/ N608D) were correctly targeted to the vacuole membrane.
2. Patch-clamp studies revealed that removal of one of the negative charges at position Glu605 or Asp606 was already sufficient to promote voltage-dependent channel activation with higher voltage sensitivity. The combined neutralization of these residues (E605A/D606N), however, was required to additionally reduce the luminal Ca2+ sensitivity of the AtTPC1 channel, leading to hyperactive AtTPC1 channels. Thus, the residues Glu605/Asp606 are functionally coupled with the voltage sensor of AtTPC1 channel, thereby modulating channel gating, and form a novel luminal Ca2+ sensing site 3 in AtTPC1 at the luminal entrance of the ion transport pathway.
3. Interestingly, this novel luminal Ca2+ sensing site 3 (Glu605/Asp606) and Glu457 from the luminal Ca2+ sensing site 2 of the luminal Ca2+-sensitive AtTPC1 channel were neutralized by either asparagine or alanine in the TPC1 channel from Vicia faba and many other Fabaceae. Moreover, the VfTPC1 was validated to be a hyperactive TPC1 channel with higher tolerance to luminal Ca2+ loads which was in contrast to the AtTPC1 channel features. As a result, VfTPC1 but not AtTPC1 conferred the hyperexcitability of vacuoles. When AtTPC1 was mutated for the three VfTPC1-homologous polymorphic site residues, the AtTPC1 triple mutant (E457N/E605A/D606N) gained VfTPC1-like characteristics. However, when VfTPC1 was mutated for the three AtTPC1-homologous polymorphic site residues, the VfTPC1 triple mutant (N458E/A607E/N608D) still sustained VfTPC1-WT-like features. These findings indicate that the hyperactivity of VfTPC1 is achieved in part by the loss of negatively charged amino acids at positions that - as part of the luminal Ca2+ sensing sites 2 and 3 – are homologous to AtTPC1-Glu457/Glu605/Asp606 and are likely stabilized by other unknown residues or domains.
4.The luminal polymorphic pore residues (Glu605/Asp606 in AtTPC1) apparently do not contribute to the unitary conductance of TPC1. Under symmetrical K+ conditions, a single channel conductance of about 80 pS was determined for AtTPC1 wild type and the AtTPC1 double mutant E605A/D606A. This is in line with the three-fold higher unitary conductance of VfTPC1 (232 pS), which harbors neutral luminal pore residues at the homologous sites to AtTPC1.
In conclusion, by studying TPC1 channel from Arabidopsis thaliana and Vicia faba, the present thesis provides evidence that the natural TPC1 channel variants exhibit differences in voltage gating, luminal Ca2+ sensitivity and luminal Ca2+ binding sites.
Ziel dieser klinisch-experimentellen Studie war die Untersuchung
elektromyographischer Kaumuskelprofile von beschwerdefreien Probandinnen
unterschiedlichen Bruxismusgrades nach sensomotorischem Training. Die aufgestellte
Hypothese postulierte signifikante Unterschiede der EMG-Parameter nach
sensomotorischem Training. Nach einer Ruhephase ohne Intervention sollten die
Unterschiede in den Ausgangszustand zurückkehren. Hierzu wurden 40 Probandinnen
mit einem Durchschnittsalter von 24,58 ± 2,72 Jahren über einen Zeitraum von fünf
Wochen untersucht. Die Probandinnen wurden mittels zufälliger Verteilung und
altersentsprechend gematcht in zwei gleichgroße Gruppen eingeteilt. Sowohl die
Teilnehmerinnen der Kontrollgruppe, als auch die der Interventionsgruppe absolvierten
im Verlauf der Studie drei elektromyographische Messungen. Nach einer einwöchigen
Voruntersuchungsphase fand die erste Messung (T1) statt. Nach drei Wochen und nach
fünf Wochen erfolgten die zweite (T2) und die dritte Messung (T3). Während der
Messungen führten die Probandinnen kraftkontrollierte Übungen mit drei
submaximalen Kraftleveln und maximalen Kräften aus. Zusätzlich absolvierte die
Interventionsgruppe zwischen T1 und T2 ein sensomotorisches Training mit dem
RehaBite®-Gerät. Die bipolaren Oberflächen-EMG-Ableitungen erfolgten für beide Mm.
masseteres und Mm. temporales. Insgesamt wurden acht Muskelareale aufgezeichnet.
Sechs für die Mm. masseteres und zwei für die Mm. temporales. Die submaximalen
Kräfte wurden als RMS %MVC und die maximalen Kräfte als RMS MVC verglichen. Die
statistischen Vergleiche erfolgten anhand von T-Tests und Mixed ANOVAs. Nach
Beurteilung der Ergebnisse konnte kein signifikanter Effekt des sensomotorischen
Trainings identifiziert werden. Die aufgestellte Hypothese muss daher abgelehnt
werden. Für das erste der drei submaximalen Kraftlevel konnte für die Initialmessung
(T1) ein signifikanter Unterschied zwischen Probandinnen mit und ohne Schlafbruxismus
in zwei der acht Muskelareale festgestellt werden. Für zukünftige Folgeuntersuchungen
zur Wirksamkeit des sensomotorischen Trainings bei Bruxismus ist die Verlängerung des
Interventionsintervalls sowie eine Vergrößerung des Studienkollektivs samt Einschluss
männlicher Probanden empfehlenswert.
Zweck: Obwohl Bruxismus im Wesentlichen als Verhalten mit multifaktorieller Genese gilt, konnten bisher nicht eindeutig die damit assoziierten Komorbiditäten aufgeklärt werden. Die Zielsetzung war, anamnestische und psychosoziale Unterschiede zwischen Proband(inn)en mit und ohne möglichem bzw. definitivem Bruxismus zu ermitteln. Darüber hinaus sollte die Übereinstimmung verschiedener Instrumente zur Bruxismus-Diagnostik und der Effekt von zwei Interventionen (bedingte elektrische Stimulation (CES) und Kautraining) analysiert werden.
Methoden: In dieser klinischen, explorativen Studie wurden 76 Proband(inn)en untersucht. Die Proband(inn)en wurden in die drei Gruppen Kontrollgruppe, aktive Interventionsgruppe und Rehabite Interventionsgruppe eingeteilt. Die Kontrollgruppe trug ein portables EMG-Gerät (GrindCare) jede Nacht über einen Beobachtungszeitraum von 5 Wochen inaktiv. Die aktive Interventionsgruppe trug es die erste Woche inaktiv, dann 2 Wochen aktiv mit CES und anschließend erneut 2 Wochen inaktiv. Die RehaBite Interventionsgruppe verwendete das GrindCare eine Woche inaktiv, darauf folgte ein zweiwöchiges Kautraining mit einer Bissgabel namens RehaBite aber ohne EMG-Begleitung und die letzten zwei Wochen verliefen ohne Rehabite und GrindCare. Zu Beginn und am Ende des Beobachtungszeitraums füllten alle drei Gruppen die gleichen Fragebögen, u.a. die Oral Behavior Checklist (OBC) und verschiedene Fragebögen zu körperlichen und psychologischen Parametern, aus. Das GrindCare misst die Episoden und ermöglicht damit die Diagnose eines definitiven Schafbruxismus (SB).
Ergebnisse: Es existierten signifikante Unterschiede zwischen Proband(inn)en mit und ohne Bruxismus (möglicher und definitiver SB, möglicher Wachbruxismus (WB), möglicher kombinierter SB und WB) in diversen anamnestischen und psychosozialen Parametern. Außerdem bestand ein signifikanter Zusammenhang zwischen erhöhter Kieferaktivität (diagnostiziert mittels OBC) und SB- sowie WB-Selbstangabe sowie zwischen den Selbstangaben von SB und WB untereinander, nicht jedoch zwischen Fragebögen und apparativer Diagnostik. Die CES bewirkte keine Reduktion der Episoden, dafür verbesserten sich jedoch einzelne körperliche und psychosoziale Parameter in der aktiven bzw. in der Rehabite Gruppe im Laufe des Beobachtungszeitraums.
Fazit: Personen mit und ohne möglichem bzw. definitivem Bruxismus unterschieden sich in verschiedenen anamnestischen, körperlichen und psychosozialen Eigenschaften voneinander. Außerdem bestehen signifikante Korrelationen zwischen SB und WB laut Selbstangabe, nicht jedoch bezüglich der apparativen Bruxismus-Diagnostik mit dem GrindCare. Während die Episoden nicht durch die CES gesenkt wurden, verringerten sich -eventuell durch RehaBite bzw. CES bedingt- bestimmte Beschwerden. Weiterer Forschungsbedarf besteht, um auf der Basis größerer Stichproben die gefundenen Auffälligkeiten statistisch abzusichern.
Exploring and explaining diversity and patterns of stateness is crucial for understanding causes of efficiency, duration, or the collapse of a state. The new Stateness Index (StIx) contributes to the conceptual and analytical debate on stateness and state fragility. StIx is a tool for measuring stateness and state quality since 1950 that includes country-ranking through aggregated and disaggregated data to advance performance comparison and policy analysis. This article first sums up the main theoretical aspects, followed by descriptive results.
Spielfilme gelten im Sinne einer „Visual History“ als wertvolle medizinhistorische Quellen. Dass die Arztfilme der DDR-Zeit ebenfalls als solche zu betrachten sind, da sie realhistorische Parallelen aufweisen, soll dieses Projekt zeigen. Anhand dreier Spielfilme aus den verschiedenen Jahrzehnten, in denen die DDR Bestand hatte, werden für die damalige Zeit typische Konflikte und Themen des Arztseins in der DDR näher beleuchtet. Die drei Hauptfilme dieses Projekts – „Ärzte“ (1960), „Dr. med. Sommer II“ (1970) und „Ärztinnen“ (1983/84) – wurden hinsichtlich ihrer Hauptfiguren, Filmtechnik und -musik analysiert und mittels Filmkritiken, Werbematerial und Aufsätzen aus der damaligen Zeit in einen realhistorischen Kontext gesetzt. Außerdem wurden zur besseren filmgeschichtlichen Einordnung weitere Arztfilme aus der DDR in die Arbeit miteinbezogen. Das Medium Film spielte in Zeiten der DDR auch zur allgemeinen gesellschaftlichen Beeinflussung eine wichtige Rolle. Durch die Analyse der Filme unter Einbeziehung von historischen Zeitungsartikeln und Werbematerial wird das Bild eines sozialistischen Idealmenschen und -arztes, wie von der SED propagiert, dargestellt und untersucht.
Within this thesis, three main approaches for the assessment and investigation of altered hemodynamics like wall shear stress, oscillatory shear index and the arterial pulse wave velocity in atherosclerosis development and progression were conducted:
1. The establishment of a fast method for the simultaneous assessment of 3D WSS and PWV in the complete murine aortic arch via high-resolution 4D-flow MRI
2. The utilization of serial in vivo measurements in atherosclerotic mouse models using high-resolution 4D-flow MRI, which were divided into studies describing altered hemodynamics in late and early atherosclerosis
3. The development of tissue-engineered artery models for the controllable application and variation of hemodynamic and biologic parameters, divided in native artery models and biofabricated artery models, aiming for the investigation of the relationship between atherogenesis and hemodynamics
Chapter 2 describes the establishment of a method for the simultaneous measurement of 3D WSS and PWV in the murine aortic arch at, using ultra high-field MRI at 17.6T [16], based on the previously published method for fast, self-navigated wall shear stress measurements in the murine aortic arch using radial 4D-phase contrast MRI at 17.6 T [4]. This work is based on the collective work of Dr. Patrick Winter, who developed the method and the author of this thesis, Kristina Andelovic, who performed the experiments and statistical analyses. As the method described in this chapter is basis for the following in vivo studies and undividable into the sub-parts of the contributors without losing important information, this chapter was not split into the single parts to provide fundamental information about the measurement and analysis methods and therefore better understandability for the following studies. The main challenge in this chapter was to overcome the issue of the need for a high spatial resolution to determine the velocity gradients at the vascular wall for the WSS quantification and a high temporal resolution for the assessment of the PWV without prolonging the acquisition time due to the need for two separate measurements. Moreover, for a full coverage of the hemodynamics in the murine aortic arch, a 3D measurement is needed, which was achieved by utilization of retrospective navigation and radial trajectories, enabling a highly flexible reconstruction framework to either reconstruct images at lower spatial resolution and higher frame rates for the acquisition of the PWV or higher spatial resolution and lower frame rates for the acquisition of the 3D WSS in a reasonable measurement time of only 35 minutes. This enabled the in vivo assessment of all relevant hemodynamic parameters related to atherosclerosis development and progression in one experimental session. This method was validated in healthy wild type and atherosclerotic Apoe-/- mice, indicating no differences in robustness between pathological and healthy mice.
The heterogeneous distribution of plaque development and arterial stiffening in atherosclerosis [10, 12], however, points out the importance of local PWV measurements. Therefore, future studies should focus on the 3D acquisition of the local PWV in the murine aortic arch based on the presented method, in order to enable spatially resolved correlations of local arterial stiffness with other hemodynamic parameters and plaque composition.
In Chapter 3, the previously established methods were used for the investigation of changing aortic hemodynamics during ageing and atherosclerosis in healthy wild type and atherosclerotic Apoe-/- mice using the previously established methods [4, 16] based on high-resolution 4D-flow MRI. In this work, serial measurements of healthy and atherosclerotic mice were conducted to track all changes in hemodynamics in the complete aortic arch over time. Moreover, spatially resolved 2D projection maps of WSS and OSI of the complete aortic arch were generated. This important feature allowed for the pixel-wise statistical analysis of inter- and intragroup hemodynamic changes over time and most importantly – at a glance. The study revealed converse differences of local hemodynamic profiles in healthy WT and atherosclerotic Apoe−/− mice, with decreasing longWSS and increasing OSI, while showing constant PWV in healthy mice and increasing longWSS and decreasing OSI, while showing increased PWV in diseased mice. Moreover, spatially resolved correlations between WSS, PWV, plaque and vessel wall characteristics were enabled, giving detailed insights into coherences between hemodynamics and plaque composition. Here, the circWSS was identified as a potential marker of plaque size and composition in advanced atherosclerosis. Moreover, correlations with PWV values identified the maximum radStrain could serve as a potential marker for vascular elasticity. This study demonstrated the feasibility and utility of high-resolution 4D flow MRI to spatially resolve, visualize and analyze statistical differences in all relevant hemodynamic parameters over time and between healthy and diseased mice, which could significantly improve our understanding of plaque progression towards vulnerability. In future studies the relation of vascular elasticity and radial strain should be further investigated and validated with local PWV measurements and CFD.
Moreover, the 2D histological datasets were not reflecting the 3D properties and regional characteristics of the atherosclerotic plaques. Therefore, future studies will include 3D plaque volume and composition analysis like morphological measurements with MRI or light-sheet microscopy to further improve the analysis of the relationship between hemodynamics and atherosclerosis.
Chapter 4 aimed at the description and investigation of hemodynamics in early stages of atherosclerosis. Moreover, this study included measurements of hemodynamics at baseline levels in healthy WT and atherosclerotic mouse models. Due to the lack of hemodynamic-related studies in Ldlr-/- mice, which are the most used mouse models in atherosclerosis research together with the Apoe-/- mouse model, this model was included in this study to describe changing hemodynamics in the aortic arch at baseline levels and during early atherosclerosis development and progression for the first time. In this study, distinct differences in aortic geometries of these mouse models at baseline levels were described for the first time, which result in significantly different flow- and WSS profiles in the Ldlr-/- mouse model. Further basal characterization of different parameters revealed only characteristic differences in lipid profiles, proving that the geometry is highly influencing the local WSS in these models. Most interestingly, calculation of the atherogenic index of plasma revealed a significantly higher risk in Ldlr-/- mice with ongoing atherosclerosis development, but significantly greater plaque areas in the aortic arch of Apoe-/- mice. Due to the given basal WSS and OSI profile in these two mouse models – two parameters highly influencing plaque development and progression – there is evidence that the regional plaque development differs between these mouse models during very early atherogenesis.
Therefore, future studies should focus on the spatiotemporal evaluation of plaque development and composition in the three defined aortic regions using morphological measurements with MRI or 3D histological analyses like LSFM. Moreover, this study offers an excellent basis for future studies incorporating CFD simulations, analyzing the different measured parameter combinations (e.g., aortic geometry of the Ldlr-/- mouse with the lipid profile of the Apoe-/- mouse), simulating the resulting plaque development and composition. This could help to understand the complex interplay between altered hemodynamics, serum lipids and atherosclerosis and significantly improve our basic understanding of key factors initiating atherosclerosis development.
Chapter 5 describes the establishment of a tissue-engineered artery model, which is based on native, decellularized porcine carotid artery scaffolds, cultured in a MRI-suitable bioreactor-system [23] for the investigation of hemodynamic-related atherosclerosis development in a controllable manner, using the previously established methods for WSS and PWV assessment [4, 16]. This in vitro artery model aimed for the reduction of animal experiments, while simultaneously offering a simplified, but completely controllable physical and biological environment. For this, a very fast and gentle decellularization protocol was established in a first step, which resulted in porcine carotid artery scaffolds showing complete acellularity while maintaining the extracellular matrix composition, overall ultrastructure and mechanical strength of native arteries. Moreover, a good cellular adhesion and proliferation was achieved, which was evaluated with isolated human blood outgrowth endothelial cells. Most importantly, an MRI-suitable artery chamber was designed for the simultaneous cultivation and assessment of high-resolution 4D hemodynamics in the described artery models. Using high-resolution 4D-flow MRI, the bioreactor system was proven to be suitable to quantify the volume flow, the two components of the WSS and the radStrain as well as the PWV in artery models, with obtained values being comparable to values found in literature for in vivo measurements. Moreover, the identification of first atherosclerotic processes like intimal thickening is achievable by three-dimensional assessment of the vessel wall morphology in the in vitro models. However, one limitation is the lack of a medial smooth muscle cell layer due to the dense ECM. Here, the utilization of the laser-cutting technology for the generation of holes and / or pits on a microscale, eventually enabling seeding of the media with SMCs showed promising results in a first try and should be further investigated in future studies. Therefore, the proposed artery model possesses all relevant components for the extension to an atherosclerosis model which may pave the way towards a significant improvement of our understanding of the key mechanisms in atherogenesis.
Chapter 6 describes the development of an easy-to-prepare, low cost and fully customizable artery model based on biomaterials. Here, thermoresponsive sacrificial scaffolds, processed with the technique of MEW were used for the creation of variable, biomimetic shapes to mimic the geometric properties of the aortic arch, consisting of both, bifurcations and curvatures. After embedding the sacrificial scaffold into a gelatin-hydrogel containing SMCs, it was crosslinked with bacterial transglutaminase before dissolution and flushing of the sacrificial scaffold. The hereby generated channel was subsequently seeded with ECs, resulting in an easy-to-prepare, fast and low-cost artery model. In contrast to the native artery model, this model is therefore more variable in size and shape and offers the possibility to include smooth muscle cells from the beginning. Moreover, a custom-built and highly adaptable perfusion chamber was designed specifically for the scaffold structure, which enabled a one-step creation and simultaneously offering the possibility for dynamic cultivation of the artery models, making it an excellent basis for the development of in vitro disease test systems for e.g., flow-related atherosclerosis research. Due to time constraints, the extension to an atherosclerosis model could not be achieved within the scope of this thesis. Therefore, future studies will focus on the development and validation of an in vitro atherosclerosis model based on the proposed bi- and three-layered artery models.
In conclusion, this thesis paved the way for a fast acquisition and detailed analyses of changing hemodynamics during atherosclerosis development and progression, including spatially resolved analyses of all relevant hemodynamic parameters over time and in between different groups. Moreover, to reduce animal experiments, while gaining control over various parameters influencing atherosclerosis development, promising artery models were established, which have the potential to serve as a new platform for basic atherosclerosis research.
Drug Discovery based on Oxidative Stress and HDAC6 for Treatment of Neurodegenerative Diseases
(2024)
Most antioxidants reported so far only achieved limited success in AD clinical trials. Growing evidences suggest that merely targeting oxidative stress will not be sufficient to fight AD. While multi-target directed ligands could synergistically modulate different steps in the neurodegenerative process, offering a promising potential for treatment of this complex disease.
Fifteen target compounds have been designed by merging melatonin and ferulic acid into the cap group of a tertiary amide HDAC6 inhibitor. Compound 10b was screened as the best hybrid molecule exhibit potent HDAC6 inhibition and potent antioxidant capacity. Compound 10b also alleviated LPS-induced microglia inflammation and led to a switch from neurotoxic M1 to the neuroprotective M2 microglial phenotype. Moreover, compound 10b show pronounced attenuation of spatial working memory and long-term memory damage in an in vivo AD mouse model. Compound 10b can be a potentially effective drug candidate for treatment of AD and its druggability worth to be further studied.
We have designed ten novel neuroprotectants by hybridizing with several common antioxidants, including ferulic acid, melatonin, lipoic acid, and trolox. The trolox hybrid compound exhibited the most potent neuroprotective effects in multiple neuroprotection assays. Besides, we identified the synergistic effects between trolox and vitamin K derivative, and our trolox hybrid compound showed comparable neuroprotection with the mixture of trolox and vitamin K derivative.
We have designed and synthesized 24 quinone derivatives based on five kinds of different quinones including ubiquinone, 2,3,5-trimethyl-1,4-benzoquinone, memoquin, thymoquinone, and anthraquinone. Trimethylbenzoquinone and thymoquinone derivatives showed more potent neuroprotection than other quinones in oxytosis assay. Therefore, trimethylbenzoquinone and thymoquinone derivatives can be used as lead compounds for further mechanism study and drug discovery for treatment of neurodegenerative disease.
We designed a series of photoswitchable HDAC inhibitors, which could be effective molecular tools due to the high spatial and temporal resolution. In total 23 target compounds were synthesized and photophysicochemically characterized. Azoquinoline-based compounds possess more thermally stable cis-isomers in buffer solution, which were further tested in enzyme-based HDAC inhibition assay. However, none of those tested compounds show significant differences in activities between trans-isomers and corresponding cis-isomers.
In aqueous environment, hydrophobic interactions play an important role for DNA. The introduction of modifications based on hydrophobic aromatic moieties offers additional ways for controlling recognition and reactivity of functional groups in DNA. Modifications are introduced through an artificial backbone or in the form of an extension of the nucleobases, resulting in additional properties of the DNA.
This dissertation focuses on the use of hydrophobic units for the functionalization of DNA.
In the first part of the work, the tolane (i. e. diphenylacetylene) motif was used in combination with the acyclic backbone of GNA and BuNA to generate recognition units in the DNA context. Fluorination of the aromatic rings in the tolane moiety provided the basis for a supramolecular language based on arene-fluoroarene interactions. The specific recognition was investigated by thermodynamic, kinetic and NMR spectroscopic methods.
In the second part of the work, deoxyuridine derivatives with a hydrophobic aromatic modification were prepared and incorporated into DNA duplexes. The irradiation with UV light led to a [2+2] cycloaddition reaction between two modified nucleosides in the DNA. This reaction product was structurally characterized and the reaction was used in various biochemical and nanotechnological DNA applications.