Institutes
Refine
Year of publication
Document Type
- Article (320)
- Doctoral Thesis (179)
- Preprint (41)
Language
- English (540) (remove)
Has Fulltext
- yes (540)
Is part of the Bibliography
- no (540)
Keywords
- Podospora anserina (8)
- aging (8)
- SARS-CoV-2 (7)
- Cyanobacteria (5)
- Ecology (5)
- Membrane Proteins (5)
- Phylogeny (5)
- mitochondria (5)
- Acetogenesis (4)
- Biodiversity (4)
- Haloferax volcanii (4)
- Saccharomyces cerevisiae (4)
- Synechococcus (4)
- alternative splicing (4)
- bats (4)
- fungi (4)
- Acetogen (3)
- Bioenergetics (3)
- Biogeography (3)
- Biomarker (3)
- COVID19-NMR (3)
- Carotenoids (3)
- Evolution (3)
- Lipid and Fatty Acid Composition (3)
- Marine Diatoms (3)
- Membrane Transport (3)
- Microbiology (3)
- Oxidoreductases (3)
- Photooxidation (3)
- Pigmentation (3)
- Protein Structure (3)
- RNA (3)
- Solution NMR spectroscopy (3)
- Taxonomy (3)
- Thermophile (3)
- Transcriptomics (3)
- biodiversity (3)
- climate change (3)
- sleep (3)
- structural biology (3)
- zebrafish (3)
- 14CO2 Fixation (2)
- 5′-UTR (2)
- Acetogenic bacteria (2)
- Acinetobacter (2)
- Adhesion (2)
- Aloe (2)
- Amino Acid Pools (2)
- Archaea (2)
- Asphodelaceae (2)
- Bioaccumulation (2)
- Biomarkers (2)
- Biosynthesis (2)
- Bleaching Herbicides (2)
- Climate change (2)
- Community ecology (2)
- Conservation biology (2)
- Covid19-NMR (2)
- Crustacea (2)
- DNA Transformation (2)
- DNA uptake (2)
- Desiccation resistance (2)
- Dicarboxylic acids (2)
- Downy mildew (2)
- Ecological modelling (2)
- Ecotoxicogenomics (2)
- Electron Bifurcation (2)
- Electron Transfer (2)
- Electron Transport (2)
- Energy Conservation (2)
- Energy Metabolism (2)
- Energy conservation (2)
- Entomology (2)
- Enzyme Mechanisms (2)
- European beech (2)
- Host-parasite interaction (2)
- Iron-Sulfur Protein (2)
- Land cover (2)
- Light-sheet microscopy (2)
- MICOS (2)
- Magnetic compass (2)
- Maxent (2)
- Membrane Biogenesis (2)
- Metabolic Engineering (2)
- Metabolic engineering (2)
- Metabolism (2)
- Metalloenzymes (2)
- Methylorubrum extorquens (2)
- Methylorubrum extorquens AM1 (2)
- Microplastic (2)
- Mitochondria (2)
- Modification (2)
- Morphogenesis (2)
- Morphology (2)
- NMR (2)
- NMR spectroscopy (2)
- Non-invasive sampling (2)
- Oaks (2)
- Oomycetes (2)
- Oxidative stress (2)
- Peronosporaceae (2)
- Photosynthesis (2)
- Phycocyanin-Free Lamellae (2)
- Protein Translocation (2)
- Psychology (2)
- Risk assessment (2)
- Solution NMR-spectroscopy (2)
- Species distribution modelling (2)
- Synaptic transmission (2)
- Synchron Cultures (2)
- Thermus (2)
- Trypanosoma cruzi (2)
- UV-B Stress (2)
- Wood-Ljungdahl pathway (2)
- Wood–Ljungdahl pathway (2)
- Xenorhabdus (2)
- Zebrafish (2)
- angiogenesis (2)
- aroma (2)
- autophagy (2)
- bacteria (2)
- biodiversity protection (2)
- biosynthesis (2)
- carotenoid biosynthesis (2)
- climate (2)
- color (2)
- community composition (2)
- conservation (2)
- conservation funding (2)
- conservation genetics (2)
- conservation planning (2)
- cox2 (2)
- cristae (2)
- cryptochrome (2)
- decision making (2)
- development (2)
- environmental attitudes (2)
- environmental education (2)
- extremophile (2)
- gene expression (2)
- genomics (2)
- global change (2)
- heat stress (2)
- inclination compass (2)
- integrins (2)
- long non-coding RNA (2)
- metabarcoding (2)
- microglia (2)
- migration (2)
- morphology (2)
- nuclear magnetic resonance (NMR) (2)
- one new species (2)
- oomycetes (2)
- peroxisomes (2)
- phylogeny (2)
- population genetics (2)
- population genomics (2)
- post-2020 biodiversity targets (2)
- pre-mRNA (2)
- predation (2)
- prefrontal cortex (2)
- prostate carcinoma cells (2)
- strategic site selection (2)
- structure–activity relationships (2)
- tumor microenvironment (2)
- 14C- and 15N-Assimilation (1)
- 15N-Labelled Amino Acids (1)
- 16S rRNA gene (1)
- 18S rRNA gene (1)
- 2030 Agenda (1)
- 3-Hydroxybutyric acid (1)
- 5'-UTR (1)
- 5-Hydroxyaloin A (1)
- 5_SL4 (1)
- ABR (1)
- AChE (1)
- ADAM15 (1)
- ADCD (1)
- ALE (1)
- AMPK (1)
- ATG24 (1)
- ATP (1)
- Absorption Spectra (1)
- Acetobacterium (1)
- Acetogenic metabolism (1)
- Acid transporters (1)
- Active Particles (1)
- Adenosine (1)
- Aedes (1)
- Agent-based modeling (1)
- Aging (1)
- Aging Phenomenon (1)
- Aichi targets (1)
- Air Pollutants (1)
- Alien species (1)
- Allohormone pheromones (1)
- Alphaproteobacteria (1)
- Amino Acids (1)
- Amphibia (1)
- Amplexus (1)
- Anabaena flos-aquae (1)
- Anacystis (1)
- Anaerobes (1)
- Anaerobic bacteria (1)
- Androst-4-en-3,17-dione (1)
- Anion Transport System (1)
- Anthraquinones (1)
- Anthropocene (1)
- Antibiotic Resistance (1)
- Antibiotics and Metabolite Export (1)
- Antioxidants (1)
- Aphanomyces astaci (1)
- Apoptosis (1)
- Aposematism (1)
- Aquilegia (1)
- Arabidopsis thaliana (1)
- Arctic Ocean (1)
- Ascomycota (1)
- Assignment (1)
- Assimilation of 15N-Nitrate (1)
- Asymmetrie Reconstitution (1)
- Auditory midbrain (1)
- Autism Spectrum Disorder (1)
- Autism Spectrum disorder (1)
- Automobile Exhaust (1)
- B chromosome (1)
- Bacillariaphyceae (1)
- Bacillus (1)
- Background expression (1)
- Bacteria (1)
- Bacterial Metabolism (1)
- Bacterial genes (1)
- Bacterial physiology (1)
- Bacterial structural biology (1)
- Bacteriology (1)
- Baleen whales (1)
- Band 3 Protein (1)
- Bartonella henselae (1)
- Basidiomycota (1)
- Behaviour (1)
- Benin (1)
- Benthic environment (1)
- Benthos (1)
- Biochemistry (1)
- Biodiversity tools and pipelines (1)
- Bioenergetics/Electron Transfer Complex (1)
- Bioengineering (1)
- Biofuels (1)
- Biohydrogen (1)
- Biological anthropology (1)
- Bioreactor (1)
- Biosecurity (1)
- Biotechnology (1)
- Biotic interactions (1)
- Biotransformation (1)
- Body burden (1)
- Bogert’s rule (1)
- Bolivia (1)
- Bovidae (1)
- Brain-stimulus synchrony (1)
- Breeding glands (1)
- Brudenell River (1)
- Bungarus (1)
- Bungarus niger (1)
- Bungarus walli (1)
- Business strategy in drug development (1)
- Butyrate (1)
- CAZy (1)
- CLIP (1)
- CLP protease (1)
- CNV 16p11.2 (1)
- COVID-19 (1)
- CRISPR-Cas9 (1)
- CRISPR-Cas9 gene conversion (1)
- CXCL12 (1)
- CXCR4 (1)
- CaMPARI (1)
- Caffeate Respiration (1)
- Calathea (1)
- Calmodulin (1)
- Canada (1)
- Canis lupus (1)
- Canis lupus familiaris (1)
- Carbohydrates (1)
- Carbon capture (1)
- Carbon cycling (1)
- Cardiac regeneration (1)
- Cardiac remodeling (1)
- Carnivora (1)
- Carnivores (1)
- Carotene Isomerase (1)
- Carotenoid Desaturation (1)
- Castor bean tick (1)
- Catalase (1)
- Cation Proton Antiporter (1)
- Cell Wall (1)
- Cellular microbiology (1)
- Cellulase gene expression (1)
- Cercospora (1)
- Chagas disease (1)
- Chaperone Chaperonin (1)
- Chaperones (1)
- Chemical communication (1)
- Chemical dispersant (1)
- Chemical dispersants (1)
- Chemistry (1)
- Chemotaxonomy (1)
- Chironomus riparius (1)
- Chlorophyll (1)
- Chlorophyll Fluorescence (1)
- Chlorophyll Formation (1)
- Chlorophyll fluorescence (1)
- Chloroplast (1)
- Chlorosis (1)
- Chromatin (1)
- Chromones (1)
- Chrysops (1)
- Climate (1)
- Climate Change (1)
- Climate-change ecology (1)
- Climatic conditions (1)
- Closely related fungal species (1)
- ClpB (1)
- Coevolution (1)
- Colorectal Cancer (1)
- Community barcoding (1)
- Computational model (1)
- Conservation (1)
- Coronaries (1)
- Cortex (1)
- Cortical column (1)
- Costs (1)
- Crude oil (1)
- Crystal Structure (1)
- Cucumis sativus (Cucumber) (1)
- Cumate (1)
- D. magna (1)
- DCMU-Type Inhibitors (1)
- DCMU-Type Inhibitors Shade Adaptation (1)
- DEPDC5 (1)
- DIRAS2 (1)
- DNA Amplification Fingerprinting (1)
- DNA metabarcoding (1)
- DNA-Specific Labelling (1)
- Daboia russelii (1)
- Dark fermentation (1)
- Data standard (1)
- Data standards (1)
- Deep sea (1)
- Dehydration (medicine) (1)
- Dental Tissues (1)
- Depth (1)
- Development (1)
- Diatomophthora (1)
- Dicellomyces (1)
- Dimer Yield Ratio (1)
- Dimerization domain (1)
- Dioscorea (1)
- Diosgenin Production (1)
- Direct seeding (1)
- Discovery (1)
- Diseases (1)
- Dispersal capacity (1)
- Dissemination (1)
- Diversity (1)
- Drought (1)
- Drought reaction (1)
- Drug discovery (1)
- Drug therapy (1)
- Dynamics (1)
- E-NTPDase (1)
- ER (1)
- ERAL1 (1)
- EROD (1)
- Earth sciences (1)
- Earthworms (1)
- EcNhaA (1)
- Ech (1)
- Ecological niche modelling (1)
- Ecological requirements (1)
- Ecosystem Services (1)
- Ecotoxicology (1)
- Ecto-5'-nucleotidase (1)
- Ectrogella (1)
- Electron Microscopy (1)
- Electron transport chain (1)
- Electron-bifurcating hydrogenase (1)
- Electrophysiology (1)
- Elimination of Rho Factor (1)
- Embryo toxicity (1)
- Embryogenesis (1)
- Emerging insect model organisms (1)
- Endocrine disruptors (1)
- Endocrine-disrupting compounds (1)
- Endothelial (1)
- Endothelial-to-mesenchymal transition (1)
- Engineering (1)
- Entolomataceae (1)
- Entorrhizales (1)
- Envelope (1)
- Environmental factors (1)
- Environmental fate (1)
- Environmental partitioning (1)
- Environmental sciences (1)
- Environmental studies (1)
- Enzyme Induction (1)
- Enzyme Kinetics (1)
- Enzyme engineering (1)
- EphrinB2 (1)
- Equilibrium partitioning theory (1)
- Erythrocyte Membrane (1)
- Ethiopia (1)
- Ethylmalonyl-CoA (1)
- Eubacterium (1)
- Europe (1)
- European Beech (1)
- European Union (1)
- Evolutionary biology (1)
- Evolutionary developmental biology (1)
- Evolutionary genetics (1)
- Excretion (1)
- Extinction (1)
- Extracellular matrix (1)
- Extremophile (1)
- Extremophiles (1)
- F1Fo-ATP-synthase (1)
- FAD (1)
- FAD synthase (1)
- FAD1 (1)
- Fabaceae (1)
- Fabclavine (1)
- Fagaceae (1)
- Far UV (1)
- Felidae (1)
- Filamentous fungi (1)
- Flavoproteins (1)
- Fluorescence imaging (1)
- Folic Acid Antagonists (1)
- Foraminiferal (1)
- Freshwater (1)
- Freshwater Ecosystems (1)
- Freshwater invertebrate (1)
- Functional Ecology (1)
- Functional genomics (1)
- Functional traits (1)
- Fungal pan-genomes (1)
- G protein-coupled receptor (GPCR) (1)
- G3BP1 (1)
- GRAND-SLAM (1)
- Gal2 (1)
- Galakturonsäure (1)
- Gas Vacuoles (1)
- Gene sll0033 (1)
- Genetic variation (1)
- Genetic vectors (1)
- Genetics (1)
- Genome (1)
- Genome sequence (1)
- Genotoxicity (1)
- Genotyping and haplotyping (1)
- Geoffrey Burnstock (1)
- Geomagnetic field (1)
- Global warming (1)
- Glucose-6-phosphate- and 6-phosphogluconate dehydrogenase (1)
- Glycolate Oxidase (1)
- Glycophorin A dimerization (1)
- Graminicolous downy mildews (1)
- H+ transport (1)
- HARS2 (1)
- HCMV (1)
- HER (1)
- HWC database (1)
- Habitat transfer (1)
- Haematopota (1)
- Hazard assessment (1)
- Health care (1)
- Heart (1)
- Heat-Bleaching (of Plastids) (1)
- Hematophagous arthropods (1)
- Herbicide Resistance (1)
- Herbicide Resistant Mutants (1)
- Herbicide-Tolerant Mutants (1)
- Herbivores (1)
- Hi-C (1)
- High Performance Liquid (1)
- Hippocampal development (1)
- Hippocampus (1)
- History (1)
- Hominins (1)
- Host jump (1)
- Human impact (1)
- Hybridization (1)
- Hydrogen storage (1)
- Hydrogen-dependent CO2 reductase (1)
- Hydrogen-dependent CO2 reductase (HDCR) (1)
- Hydrogenase (1)
- Hypercolumn (1)
- Hypothermia (1)
- I50 Value (1)
- IDP (1)
- ITS (1)
- IUCN protection categories (1)
- In situ burning (1)
- In vivo electrophysiology (1)
- Inducible Promoter (1)
- Infectious diseases (1)
- Inferior colliculus (1)
- Influenza (1)
- Insularity (1)
- International survey (1)
- Intestinal bacterial community (1)
- Inthraszentin (1)
- InvaCost (1)
- Invasive species (1)
- Isoprenoids (1)
- Isozyme Pattern (1)
- Ixodes ricinus (1)
- Kinetics of Dimer Formation (1)
- Klebsiella (1)
- Kordyana (1)
- LARS2 (1)
- LASSO algorithm (1)
- LanI Protein (1)
- Lantibiotic (1)
- Lantibiotic Immunity (1)
- Larmor frequency (1)
- Larva (1)
- Latent Injury (1)
- Laurasiatheria (1)
- Leaf Peroxisomes (1)
- Leguminosae (1)
- Life-Satisfaction (1)
- Life-history (1)
- Lifespan (1)
- Light dark transition test (1)
- Light sheet-based fluorescence microscopy (1)
- Limnology (1)
- Limonene-3-hydroxylase (1)
- Lineage Through Time (1)
- Lipoprotein (1)
- Long-term potentiation (1)
- MARTINI force field (1)
- MEK inhibition (1)
- MMN (1)
- Macrobenthosda (1)
- Macroevolution (1)
- Macrotermes (1)
- Macrozoobenthos (1)
- Magnetic conditioning (1)
- Magnetic map (1)
- Marantaceae (1)
- Marine biodiversity (1)
- Marine ecosystem (1)
- Marine invertebrates (1)
- Mass spectrometry (1)
- Maternal Immune Activation (1)
- Mawson Bank (1)
- Mechanisms of disease (1)
- Mediterranean plants (1)
- Meliolales (1)
- Membrane Energetics (1)
- Membrane Enzymes (1)
- Membrane Protein Complex (1)
- MetVF (1)
- Metabolomics (1)
- Metagenomic shotgun sequencing (1)
- Metamorphosis (1)
- Methylene-THF reductase (1)
- Methylene-tetrahydrofolate reductase (1)
- Methylotroph (1)
- Methyltransferase (1)
- Mevalonic Acid (1)
- Microbiota (1)
- Microbotryales (1)
- Microenvironment (1)
- Microplastics (1)
- Microscopy (1)
- Mikroplastik (1)
- Mineralization (1)
- Mitochondrial Transport (1)
- Mitochondrial proteases (1)
- MjNhaP1 (1)
- Model (1)
- Molecular biology (1)
- Monoterpenoid (1)
- Monoterpenoid tolerance (1)
- Montane forest (1)
- Mount Kilimanjaro (1)
- Museum samples (1)
- Mutual information (1)
- Myocardial infarction (1)
- Myotis bechsteinii (1)
- NMR solution structure (1)
- NW Pacific (1)
- Na Gradient (1)
- Na+ transport (1)
- Naja (1)
- Nanoplastic (1)
- Natural Products (1)
- Natural products (1)
- Natural sounds (1)
- Nature Contributions to People (1)
- Nature Interest Scale (NIS) (1)
- Nature Valuation (1)
- Nature conservation (1)
- Nature's Contributions to People (1)
- Naturstoffe (1)
- Neocaridina palmata (1)
- Neotropic (1)
- Neural circuits (1)
- Neural map (1)
- Neurodevelopmental Psychiatric Disorders (1)
- Neuroligins (1)
- Neuronal Differentiation (1)
- Neurotoxicity (1)
- New host (1)
- New species (1)
- Niche (1)
- Nitrogen Metabolism (1)
- Noctuidae (1)
- Non-canonical terpenes (1)
- Non-ribosomal peptide synthetases (1)
- Non-structural protein (1)
- Norflurazon (1)
- Normative dimension (1)
- Nothopassalora (1)
- Nuclear Magnetic Resonance (1)
- Nucleic acid-binding domain (1)
- Nucleocapsid (1)
- Nucleus reuniens (1)
- Nyctalus leisleri (1)
- O-CAS assay (1)
- OXPHOS (1)
- Obituary (1)
- Oil spills (1)
- Olfactory Receptors (1)
- Olpidiopsis (1)
- Omp85-independent OMP Insertion (1)
- Optimal wiring (1)
- Optimization (1)
- Organic micropollutants (1)
- Organoids (1)
- Organophosphates (1)
- Orientation preference (1)
- Oxidation-Reduction (1)
- Oxidative Stress (1)
- Oxygen (1)
- Oxygen Evolution (1)
- Ozone (1)
- P 700 (1)
- P. anserina (1)
- P. maximowiczii Henry x P. nigra L. cv. Rochester (1)
- POTRA Domains (1)
- PURA (1)
- PaCRD1 (1)
- PaIAP (1)
- Panama (1)
- Panolis flammea (1)
- Parkinson (1)
- Parkinson’s disease (1)
- Particle toxicity (1)
- Passalora (1)
- Pathogenesis (1)
- Pathways (1)
- Pelagic (1)
- Peptide natural products (1)
- Pesticides (1)
- Pheromone Inhibitor (1)
- Pheromones (1)
- Phosphohydrolases (1)
- Photoinactivation (1)
- Photorhabdus (1)
- Photosynthetic CO2 Fixation (1)
- Photosynthetic Reaction Center (1)
- Photosystem II (1)
- Phvtoene Desaturase (1)
- Phvtofluene (1)
- Phylogenetics (1)
- Physical chemistry (1)
- Physiology (1)
- Phytoene (1)
- Pigment Composition (1)
- Pigment and Protein Content (1)
- Pink1 (1)
- Pinnotheres (1)
- Pinwheel (1)
- Planetary boundaries (1)
- Plant regeneration (1)
- Plant regeneration; community assembly; diversity (1)
- Plant sciences (1)
- Plant stress (1)
- Plastic pollution (1)
- Plastic response (1)
- Plasticity (1)
- Plastics (1)
- Plastid rRNA (1)
- Podocarpus National Park (1)
- Polyhedral Bodies (1)
- Polyketides (1)
- Polymer (1)
- Polypeptides (1)
- Population density (1)
- Population dynamics (1)
- Populus nigra L. cv. Loenen (1)
- Porin (1)
- Potato Tuber Slices (1)
- Potato Tuber Tissue (1)
- Prediction (1)
- Premature Leaf Drop (1)
- Prenyl pyrophosphates (1)
- Product reuptake (1)
- Protein Assembly (1)
- Protein Complexes (1)
- Protein DNA-Interaction (1)
- Protein Purification (1)
- Protein Shape (1)
- Protein Sorting (1)
- Protein drugability (1)
- Protein druggability (1)
- Proteomics (1)
- Pseudocercospora (1)
- Pseudomonas (1)
- Pseudomonas putida (1)
- Pure Cultures of Marine Diatoms (1)
- Purkinje cell (1)
- Pyrophosphatase (1)
- QuEChERS (1)
- Quality of life (1)
- Quantum Requirement (1)
- Quarantine (1)
- Quercus (1)
- Quercus frainetto (1)
- Quercus frainetto Ten. (Ungarische Eiche) (1)
- Quercus ilex L. (Steineiche) (1)
- Quercus pubescens (1)
- Quercus pubescens Willd. (Flaumeiche) (1)
- Quercus robur L. (Stieleiche) (1)
- Quercus rubra L. (Roteiche) (1)
- Quinolinate Phosphoribosyltransferase (1)
- Quinones (1)
- Qв Binding Protein (1)
- R-INLA (1)
- RBFOX1 (1)
- REM sleep (1)
- RMP1 (1)
- RNA Polymerase (1)
- RNA genome (1)
- RNA polymerase (1)
- RNA sequencing (1)
- RNA stability (1)
- RNA turnover (1)
- RNA-binding proteins (1)
- Radical Pair model (1)
- Radiotherapy (1)
- Range expansion (1)
- Recolonization (1)
- Regeneration (1)
- Regulation of D1 Protein (1)
- Reintroduction (1)
- Rep gene (1)
- Reproduction (1)
- Resilience (1)
- Respiration (1)
- Respiratory chain (1)
- Rheumatoid Arthritis (1)
- Rhodnius prolixus (1)
- Ribosomally synthesized and post-translationally modified peptides (1)
- Ribosomen, rRNA Prozessierung, snoRNA, Ribosomenbiogenesefaktoren (1)
- Rnf (1)
- Robert Koch Institute (1)
- Ross Sea (1)
- Russell´s Viper (1)
- S-azidoacyl-N-acetylcysteamine (1)
- S9 (1)
- SL1 (1)
- SL5b (1)
- SL5b + c (1)
- SL5c (1)
- SLAM-seq (1)
- SNF1 (1)
- SNP (1)
- SNP genotyping (1)
- SNPs (1)
- SPAD (1)
- SR proteins (1)
- SSA (1)
- Salinity (1)
- Scale-up (1)
- Schistosomiaisis (1)
- Schizokinen (1)
- Science–society interactions (1)
- Scrotifera (1)
- Sea water (1)
- Secondary metabolites (1)
- Secretin (1)
- Secretins (1)
- Secretion (1)
- Seed sowing experiment (1)
- Seedling establishment (1)
- Sensorimotor processing (1)
- Sensory processing (1)
- Sex Attractants (1)
- Shade Adaptation (1)
- Shallow water (1)
- Shores (1)
- Sign posts (1)
- Simuliidae (1)
- Smut fungi (1)
- Social sciences (1)
- Sodefrin precursor-like factor (1)
- Sodium Proton Exchange (1)
- Sodium Transport (1)
- Sodium transport (1)
- Solanum lycopersicum (1)
- Solid Supported Membrane (1)
- SpaI (1)
- Spatial navigation (1)
- Species richness (1)
- Spectral clustering algorithm (1)
- Sporisorium reilianum (1)
- Ste2p (1)
- Stewardship (1)
- Stewardship and dissemination (1)
- Streams (1)
- Streptomyces hydrogenans (1)
- Structural protein (1)
- Structured Illumination Microscopy (1)
- Subjective Well-Being (1)
- Subtilin (1)
- Summer drought (1)
- Super resolution (1)
- Super resolution fluorescence microscopy (1)
- Supervised machine learning (1)
- Surface range (1)
- Sustainability research (1)
- Sustainable chemistry (1)
- Svetamycin (1)
- Swimming (1)
- Swimming behavior (1)
- Symbiont evolution (1)
- Symbiosis (1)
- Synaptosomal preparation (1)
- Synovial Fibroblast (1)
- Synthesis gas (1)
- Systematics (1)
- TWNK (1)
- Tabanidae (1)
- Tabanus (1)
- Temperature preference (1)
- Terbutryn (1)
- Terpenes (1)
- Terpenoid (1)
- Testosterone (1)
- Tetrad Analysis (1)
- Thalassiosira (1)
- Thermoanaerobacter kivui (1)
- Thermoascus aurantiacus (1)
- Thermophiles (1)
- Thermophilic acetogenic bacteria (1)
- Thermus thermophilus (1)
- Thin Layer Chromatography (1)
- Thioesterase (1)
- Threatened species (1)
- Three-Dimensional Structure (1)
- Thylakoid Membrane (1)
- Thymidylate Low Requirement (1)
- Thymidylate Sensitivity (1)
- Thymidylate Synthetase (1)
- Thymidylate Uptake (1)
- Thymine Dimers (1)
- Tick-borne diseases (1)
- Tie2 (1)
- Tigray (1)
- Tocochromanol (1)
- TolC (1)
- Tools and pipelines (1)
- Tooth Development (1)
- Topology (1)
- Toxicity (1)
- Tragelaphus oryx (1)
- Transgenic organisms (1)
- Translational Psychiatry (1)
- Transport (1)
- Traumatic mating (1)
- Tree rings (1)
- Triatominae (1)
- Trichoptera (1)
- Trimethylamine biosynthesis (1)
- Tropical forest restoration (1)
- Tropical montane forest (1)
- Truffle (1)
- Trypanosoma rangeli (1)
- Tuber magnatum (1)
- Tylosis (1)
- Type IV Pili (1)
- UV-B Effects (1)
- UV/V cones (1)
- Ultrastructure (1)
- University students (1)
- Uptake (1)
- Urgent actions (1)
- Ustilaginales (1)
- Ustilaginomycotina (1)
- Ustilago maydis (1)
- Ustilagomaydis (1)
- V1 (1)
- VEGF (1)
- Variability (1)
- Vector-host-interaction (1)
- Viral infection (1)
- Visual cortex (1)
- Vitality monitoring (1)
- WL110547 (1)
- Water accommodated fractions (1)
- Weather conditions (1)
- West Africa (1)
- Western Kenya (1)
- Wood properties (1)
- X-ray crystallography (1)
- Xylem (1)
- Zea mays (1)
- Zebrafish eleutheroembryo (1)
- aIF (1)
- abiotic factors (1)
- abundance (1)
- acetogen (1)
- acetogenic metabolism (1)
- acetyl-CoA (1)
- acoustic features (1)
- acoustic stream (1)
- acquisition strategy (1)
- active sensing (1)
- activity budgetx (1)
- adaptive transgenerational plasticity (1)
- additive manufacturing (1)
- additives (1)
- adhesin (1)
- adipogenesis (1)
- alarm calls (1)
- algae (1)
- all-E Lycopene (1)
- alzheimer’s disease (1)
- amplicon sequencing (1)
- angipoietin (1)
- animal behaviour (1)
- animal movement (1)
- animal welfare (1)
- annual plants (1)
- anomaly zone (1)
- antibiotic resistance (1)
- antibiotics (1)
- antimicrobial resistance (1)
- antipredator (1)
- apex bird species (1)
- aptamers (1)
- arabinose (1)
- archaea (1)
- arid climate (1)
- articular chondrocytes (1)
- artificial docking domains (1)
- asgard group (1)
- assembly gaps (1)
- assisted migration (1)
- ataxia (1)
- attitudes towards species conservation (1)
- auditory cortex (1)
- automated radiotelemetry system (1)
- azido-fatty acids (1)
- bacillary angiomatosis (1)
- bacteria-host interaction (1)
- bacterial community (1)
- bacterial infection (1)
- barrier (1)
- behaviour (1)
- benchmarking (1)
- benthic fauna (1)
- bioacoustics (1)
- bioactivity testing (1)
- bioassays (1)
- biodiversity conservation (1)
- biodiversity in literature (1)
- bioenergetics (1)
- biofilm (1)
- bioinformatics (1)
- biological variables (1)
- biomarkers (1)
- biosonar (1)
- biotic factors (1)
- biotrophic parasites (1)
- birds (1)
- bitopic transmembrane α-helix (1)
- blood vessels (1)
- boundary patrolling (1)
- brain cancer (1)
- brain rhythms (1)
- brain waves (1)
- branching (1)
- breeding sites (1)
- cardiolipin (1)
- cardiovascular disease (1)
- carnivora (1)
- carnivores (1)
- carotenogenic pathways (1)
- carotenoid distribution (1)
- carotenoid pathway engineering (1)
- carotenoid structures (1)
- caudate (1)
- central place foraging (1)
- cerebellum (1)
- checklist (1)
- checkpoint inhibitors (1)
- chlorophyll fluorescence (1)
- chromosomes (1)
- click-chemistry (1)
- climatic variables (1)
- co-transcriptional regulation (1)
- coalescence (1)
- cobra (1)
- coevolution (1)
- communication (1)
- communication-mediating domains (1)
- community ecology (1)
- community mean (1)
- compass orientation (1)
- complete chloroplast genome (1)
- complexome profiling (1)
- computational literary studies (1)
- connection to nature (1)
- consortia (1)
- control theory (1)
- cooperation (1)
- cophylogeny (1)
- cospeciation (1)
- cotransformation (1)
- coupling (1)
- cpDNA (1)
- cross-species RNA-sequencing (1)
- crosslinking-mass spectrometry (1)
- crustacea (1)
- cryo-EM (1)
- cultural ecosystem services (1)
- custom (1)
- cyclooctyne (1)
- cytosolic free calcium (1)
- de novo Synthesis (1)
- de novo transcription (1)
- decomposition (1)
- deep learning (1)
- deep sea (1)
- deep-sea sediment (1)
- deletion mutant (1)
- demography (1)
- dendrite (1)
- dendritic branching (1)
- dendritic morphology (1)
- depth (1)
- dermosphere (1)
- diagnostics (1)
- diatoms (1)
- differentially regulated orthologs (1)
- differentiation diversity (1)
- digital student lab (1)
- dimer interface formation (1)
- discrete choice modeling (1)
- distribution (1)
- diurnal variation (1)
- docking domains (1)
- domain architecture evolution (1)
- downy mildew (1)
- drug design (1)
- easyPACId (1)
- ecological risk assessment (1)
- ecology and biodiversity (1)
- ecospat (1)
- ecosystem management (1)
- ecosystem services (1)
- ectomycorrhizal (1)
- ectrogella (1)
- effect monitoring (1)
- effectors (1)
- elapid snake (1)
- elephant (1)
- elevational gradient (1)
- endocrine disruption (1)
- endocrine-disrupting chemicals (1)
- endophytes (1)
- endothelium (1)
- energy (1)
- energy-converting hydrogenase (Ech) (1)
- engineering (1)
- envenoming (1)
- environmental DNA (1)
- environmental behavior (1)
- environmental factors (1)
- environmental gradients (1)
- environmental humanities (1)
- environmental knowledge (1)
- environmental pollution (1)
- eukaryotic biodiversity (1)
- evolution (1)
- evolutionary traceability (1)
- exon coalescence (1)
- exon concatenation (1)
- experiment (1)
- exposome (1)
- exposure (1)
- expression system (1)
- extracellular matrix (1)
- extreme frost (1)
- failure to diverge (1)
- fatty acid dependency (1)
- fatty acid desaturation (1)
- fatty acid metabolism (1)
- fence (1)
- fitness (1)
- flowering (1)
- foliar pathogens (1)
- food contact materials (1)
- foraging (1)
- foraging site fidelity (1)
- foraging site switching (1)
- forest management (1)
- freshwater crayfish (1)
- functional group (1)
- functional traits (1)
- fungal effectors (1)
- fungal pathogens (1)
- fungal phylogeny (1)
- fungal traits (1)
- fuzzy clustering (1)
- gamma oscillations (1)
- gas exchange (1)
- gene conversion (1)
- gene families (1)
- gene models (1)
- generalised additive models (1)
- genetic engineering (1)
- genome architecture (1)
- genome assembly (1)
- genome assembly and annotation (1)
- genomic diversity (1)
- genotype (1)
- genotyping (1)
- geoecology (1)
- geographical origin (1)
- giraffe behavior (1)
- glidobactins (1)
- global biomes (1)
- glucocorticoid receptor (1)
- glucocorticoid response (1)
- graded structure (1)
- grasslands (1)
- gravity (1)
- growth promotion (1)
- guanidine riboswitch (1)
- guided zoo tours (1)
- habitat heterogeneity (1)
- hands-on elements (1)
- heat (1)
- heat and drought (1)
- heat-shock protein (1)
- heathlands (1)
- hematopoietic stem cell (1)
- herbaria (1)
- herbivores (1)
- heteroplasmy (1)
- heterozygous cells (1)
- high temperature (1)
- high throughput screening (1)
- hippo (1)
- historical biodiversity (1)
- homeostasis (1)
- homologous gene expression (1)
- honey bee classification (1)
- honey bees (1)
- horizontal gene transfer (1)
- host specificity (1)
- host-switch (1)
- housing conditions (1)
- human footprint (1)
- human-wildlife conflict (1)
- hydroxamate (1)
- hyperparasitic fungi (1)
- hyperparasitism (1)
- hypoxia (1)
- in-vitro Assay (1)
- inbreeding (1)
- indel (1)
- individual interest (1)
- individuality (1)
- infectious diseases (1)
- infra-slow oscillation (1)
- integrate-and-fire (1)
- inter- seasonal predictability (1)
- interaction networks (1)
- interest in nature (1)
- intersexuality (1)
- invasive mammals (1)
- iron starvation (1)
- krait (1)
- lab motivation scale (LMS) (1)
- land use (1)
- landscape fragmentation (1)
- lantibiotic (1)
- large subunit maturation (1)
- lateral line (1)
- latitudinal gradient (1)
- learning technology (1)
- left ventricular hypertrophy (1)
- leukodystrophy (1)
- light (1)
- light-harvesting (1)
- lipid metabolism (1)
- lipoprotein (1)
- livelihood (1)
- liver cancer (1)
- local field potentials (1)
- long noncoding RNA (1)
- long sequencing reads (1)
- long-term protection (1)
- long36 term protection (1)
- mPFC (1)
- mPTP (1)
- mRNA (1)
- mTOR (1)
- machine learning (1)
- macroevolution (1)
- macrohabitat (1)
- magnetoreception (1)
- maladaptation (1)
- mathematical modeling (1)
- maturity (1)
- maximum likelihood (1)
- mean fruit body size (1)
- mechanics (1)
- medically relevant (1)
- meerkats (1)
- membrane protein (1)
- membrane trafficking (1)
- memory (1)
- metabolic disruptors (1)
- metabolomics (1)
- metazoans (1)
- microRNA (1)
- microbiome (1)
- microplastics (1)
- microsatellite (1)
- miracula (1)
- missing data (1)
- mitochondria localization (1)
- mitochondrial dysfunction (1)
- mitochondrial localization motif (1)
- mitohormesis (1)
- mitophagy (1)
- molecular phylogenetic analysis (1)
- monetary impacts (1)
- monocytes (1)
- morphology evaluation (1)
- moth indicator groups (1)
- mounting (1)
- movement (1)
- mt DNA (1)
- mtDNA haplotypes (1)
- multi-generation experiment (1)
- mushroom (1)
- mycorrhiza (1)
- myeloid angiogenic cells (1)
- natural behavior (1)
- natural products (1)
- naturalistic stimuli (1)
- nature connectedness (1)
- navigation (1)
- nematode diversity (1)
- network analysis (1)
- neural coding (1)
- neuro-vascular (1)
- neurobiology (1)
- neurodegeneration (1)
- neurodevelopment (1)
- neuroethology (1)
- neuromodulation (1)
- neuronal coherence (1)
- neurosimulation (1)
- nightly behavior (1)
- nisin binding (1)
- nocturnal activity (1)
- nomadism (1)
- non-destructive sampling (1)
- non-material contribution (1)
- non-ribosomal peptide syntheses (1)
- non-ribosomal peptide synthetase (1)
- non-target chemical analysis (1)
- non-timber forest products (NTFPs) (1)
- nonsense-mediated mRNA decay (1)
- nontarget (1)
- northern giraffe (1)
- novel natural products (1)
- obesogens (1)
- obligate pathogens (1)
- octanoic acid (1)
- oncomodulation (1)
- oomycete (1)
- open-source 3D bioprinting (1)
- organoids (1)
- orientation behavior (1)
- orthogroup (1)
- orthology (1)
- orthology assignment (1)
- outdoor education (1)
- oxygenic photosynthesis (1)
- pH Regulation (1)
- paleobiology (1)
- parabolic flight (1)
- paralogy (1)
- parasitism (1)
- parasitoid (1)
- parathyroid hormone 2 (1)
- pathogenicity (1)
- pathway (1)
- pathway complexity (1)
- pathway evolution (1)
- peptide-antimicrobial-Xenorhabdus peptide (1)
- phenology (1)
- phosphoketolase (1)
- phosphotransacetylase (1)
- photocycle (1)
- phylogenetic informativeness (1)
- phylogenetic profiles (1)
- phylogenetic profiling (1)
- physiological stress (1)
- planning and design (1)
- plant regeneration (1)
- plasma (1)
- plasmid (1)
- plasmid copy number (1)
- playback experiment (1)
- policies (1)
- politics and governance (1)
- pollinator crisis (1)
- polymers (1)
- polyploidy (1)
- population structure (1)
- postglacial colonisation (1)
- posture estimation (1)
- power law (1)
- precipitation (1)
- prediction error (1)
- priority natural areas (1)
- probe kit (1)
- propagating waves (1)
- proteasome inhibitors (1)
- protein folding (1)
- protein production (1)
- protein structure (1)
- proteobacteria (1)
- proteoliposomes, (1)
- proteomics (1)
- proton translocation (1)
- protoplast fusion (1)
- qH2 (1)
- quality control (1)
- quantitative disease resistance (1)
- quercus (1)
- raccoon dog (Nyctereutes procyonoides) (1)
- radical pair model (1)
- random forest (1)
- range boundary (1)
- range expansion (1)
- reaction mechanisms (1)
- receptor (1)
- regulation (1)
- reliability (1)
- repeat elements (1)
- repetition suppression (1)
- reptiles (1)
- resource losses (1)
- retrophylogenomics (1)
- ribosome (1)
- ribosomes, Arabiodpsis thaliana, pre-rRNA processing, snoRNA, (1)
- rock-climbing impact (1)
- root allocation strategy (1)
- root functional traits (1)
- roots (1)
- runs of homozygosity (1)
- sage downy mildew (1)
- saprobic and ectomycorrhizal basidiomycetes (1)
- saprotrophic (1)
- scale development (1)
- scale invariance (1)
- seafloor bathymetry (1)
- search (1)
- sediment (1)
- selection gradients (1)
- senescence (1)
- sensory (1)
- sensory acquisition (1)
- serine/arginine-rich proteins (1)
- shallow water (1)
- shroom (1)
- siderophore (1)
- siderophore-dependent iron uptake (1)
- signaling (1)
- silicate (1)
- simplified production (1)
- small angle x-ray scattering (1)
- small animals (1)
- small protein (1)
- small proteins (1)
- smut fungi (1)
- snake bite (1)
- social information (1)
- social isolation (1)
- socio-economic sectors (1)
- socio-economics (1)
- soil degradation (1)
- soil fungal communities (1)
- sound coding (1)
- spatial analysis (1)
- spatial modelling (1)
- special needs students (1)
- speciation (1)
- species delimitation (1)
- species distribution model (1)
- species richness (1)
- splicing (1)
- splicing regulation (1)
- stairway plot (1)
- stereolithography (1)
- stimulus repetition (1)
- stingless bee (1)
- stochastic factors (1)
- strained promoted cycloadditon (1)
- sub-Saharan Africa (1)
- sugar uptake (1)
- sun exposure (1)
- suricates (1)
- surround suppression (1)
- survival rate (1)
- sustainability (1)
- symbiont association patterns (1)
- systems knowledge (1)
- tRNA (1)
- tRackIT (1)
- tafazzin (1)
- target knowledge (1)
- taxonomy (1)
- teaching tool (1)
- technology acceptance model (TAM) (1)
- temperate forest (1)
- temperature (1)
- terrestrial mammal (1)
- text mining (1)
- thermal-melanism hypothesis (1)
- thiolation domain (1)
- threatened cliff plant species (1)
- tight junctions (1)
- topology (1)
- trait evolution (1)
- traits (1)
- transcription (1)
- transcriptome (1)
- transcriptome analysis (1)
- transdisciplinarity (1)
- transformation knowledge (1)
- transglutaminase 2 (1)
- translation initiation (1)
- transplant experiment (1)
- trimeric autotransporter adhesin (1)
- trisporic acids (1)
- tritrophic interaction (1)
- trophic interactions (1)
- tumor model (1)
- tumor-associated macrophages (1)
- ungulate (1)
- universal (1)
- university students (1)
- unselected segregation (1)
- validity (1)
- vascular integrity (1)
- vegetation (1)
- venomous snakes (1)
- video action classification (1)
- video observation (1)
- viruses (1)
- vocalization (1)
- vocalization production; (1)
- volatile (1)
- warming (1)
- water security (1)
- white truffle (1)
- wing geometric morphometrics (1)
- wolf (1)
- wwtr1 (1)
- xenology (1)
- xylose (1)
- yap1 (1)
- yeast (1)
- zinc finger (1)
- zoo (1)
- zoo biology (1)
- zoo education (1)
- zoo elephants (1)
- µ-protein (1)
- β-Barrel Proteins (1)
- β-oxidation (1)
- ζ-Carotene (1)
Institute
- Biowissenschaften (540)
- Senckenbergische Naturforschende Gesellschaft (33)
- Medizin (17)
- Biodiversität und Klima Forschungszentrum (BiK-F) (15)
- Biochemie, Chemie und Pharmazie (13)
- Buchmann Institut für Molekulare Lebenswissenschaften (BMLS) (13)
- Zentrum für Biomolekulare Magnetische Resonanz (BMRZ) (13)
- Institut für Ökologie, Evolution und Diversität (11)
- MPI für Biophysik (8)
- Biochemie und Chemie (7)
Smut fungi (Ustilaginomycotina) were previously defined as plant parasites that produced blackish or brownish masses of teliospores in or on various organs of plants. Each teliospore germinates to form a single basidium with usually four basidiospores that subsequently grow as a saprobic, yeast-like, haploid stage. The Ustilaginomycotina are a highly diverse group with about 1,700 species in 115 different genera. All of the species were united in a single order, the Ustilaginales, in late 19th century. These teliospore producing fungi are now considered the classic smut fungi. Towards the end of the 20th century, new ideas were brought into this classification system. Most notable was the comparative work regarding the ultrastructure of septal pores and the anatomy of the interaction zones between host and parasite. This work changed the whole concept of smut fungi and their evolutionary relationships. These results were subsequently supported by molecular phylogenetic studies. Both lines of investigation led to the classification of the smut fungi into four different classes, Ustilaginomycetes, Exobasidiomycetes, Malasseziomycetes and Moniliellomycetes (see chapter 1.3).
A reliable taxonomy that reflects phylogenies needed in order to estimate the diversity and the relationships between the diverse groups of smut fungi. In the last 20 years, molecular investigations based mostly on rDNA loci, e.g. ITS (internal transcribed spacer) or LSU (large subunit), have revealed the evolutionary relationships between many taxa of smut fungi. However, there are few phylogenetic studies available for smut fungi (see chapter 1.5.1), and much work is needed to develop backbone phylogenetic trees and to resolve species complexes of many smut fungi.
This thesis reports the results of six different studies that aimed to develop new and improved tools for the phylogenetic analyses of smut fungi, and then apply these methods to selected groups of smut fungi. The first study (Kruse et al. 2017a, Chapter 3) developed a method to improve the amplification of ITS sequences of some smut fungi. Due to its high discrimination value, the ITS gene region is widely used as a barcoding locus for species delimitation of fungi. For this purpose, the general ITS primers ITS1 and ITS4 or more specific modifications, e.g. ITS1F for Ascomycota, ITS4B for Basidiomycota or M-ITS1 for smut fungi, were used. As these primer combinations often yielded unsatisfactory results, due to coamplification of other (contaminant) fungi or the host plant DNA, improvement of the amplification of the ITS region was needed. In order to design new smut specific primers for the ITS region, a representative set of several sequences of the flanking regions of the ITS region (LSU and SSU) of smut fungi, plants and other fungi were downloaded from GenBank. A set of primers was designed on this dataset. These primers were tested on a representative set of about 70 different smut genera under different PCR conditions. Finally, three different primers, one forward primer, smITS-F, and two reverse primers, smITS-R1 and -R2, were selected as the best ones. The following tests with different combinations of these primers, and also under inclusion of the M-ITS1 primer, showed only slight differences in the number of different genera that successfully amplified. But there were some differences regarding the genera that amplified. A broader test on 205 samples in 39 genera showed that the PCR efficiency of the newly designed primers was much better than the primer set ITS4/M-ITS1. With the primers designed in this study almost no non-target ITS was amplified, giving new opportunities especially for amplifying ancient DNA or DNA from older herbarium samples. However, many species groups remain unresolved by only one gene region.
The second study (Kruse et al. 2017c, Chapter 4) found new loci and suitable primers that better resolved multi-locus trees. To date, the most frequently used loci for making multi-locus trees are SSU (small subunit), LSU (large subunit) and ITS (internal transcribed spacer). While the LSU is not always sufficient to distinguish between closely related species, it is highly discriminative above the species level. In an effort to increase the phylogenetic resolution of smut phylogenies, some protein-coding genes were used, including rpb1, rpb2, and atp6 with varying success (see Chapter 2.1.2). As most of these loci are seldom used or sometimes only work on pure cultures because of their low specifity, new protein-coding loci were identified that produced reliable phylogenetic trees. Based on five available genomes, potential gene loci were filtered for possible primers. Initially, 40 different primer combinations for 14 gene loci were tested on a set of twelve different genera of smut fungi. The best candidates were selected and optimized during further tests. Finally, 22 different forward primers and 17 different reverse primers for nine different gene regions were developed, with each differentiating at least one genus of smut fungi (preferably for Ustilaginomycetes). The different primers showed varying discriminative power for different smut genera. They worked best for the Ustilaginaceae, based on the primer designed from Ustilaginomycetes genomes. These new primer sets and loci have the potential to resolve different species groups within the smut fungi and furthermore to produce reliable phylogenetic trees with high resolution. To prove their applicability, three species complexes were investigated in-depth, two from the Ustilaginomycetes and one from the Exobasidiomycetes.
...
The objectives of this thesis were to understand how distinct classes of cell types interact to shape oscillatory activity in cortical circuits of the turtle. We chose the turtle cortex as a model system for cortical computations for two reasons. One is that the phylogenetic position of turtles makes their cortex functionally and anatomically particularly interesting. The second is that reptilian brains present several unique experimental advantages. Turtles have a three-layered cortex that forms the dorsalmost part of their pallium and receives direct input from visual thalamus. Thus turtle cortex, while sharing several features with mammalian cortices, constitutes a simpler system for studying cortical computations and dynamics. Freshwater turtles are semiaquatic species, that dive for hours and hibernate for months without breathing. Their brains are adapted to these behaviors so that they can operate under severe anoxia. This property allows for ex vivo wholebrain and whole-cortex (”cortical slab”) preparations in vitro, enabling the use of many sophisticated techniques for monitoring activity in parallel.
I thus set out to utilize the advantages of our model system, by using optogenetic methods to reliably evoke oscillations in an ex vivo whole-cortex preparation while observing activity in parallel with planar multi-electrode arrays (MEA), linear silicon depth-electrodes and patch-clamp recording techniques. This required several technical aspects to be solved. Prior work in turtle cortex (Prechtl, 1994; Prechtl et al., 1997; Senseman and Robbins, 2002) indicated that visual stimuli evoke complex activity patterns (e. g. wave patterns) in dorsal cortex. The goal was to examine these dynamics in detail and to provide mechanistic explanations for them whenever possible. The recent advent of optogenetics, the development of microelectrode arrays, and the possibility to combine these techniques with classical electrophysiological approaches on a resistant, accessible and stable preparation led me to explore a number of technical avenues.
First I had to establish gene delivery methods in reptiles. I settled on recombinant viruses, and show results from several serotypes of adeno-associated virus (AAV), i lentivirus and rabies virus. I report successful gene expression of genes of interest with several subtypes of AAV, including the commonly used AAV2/1 and AAV2/5 serotypes. Second I had to find promoters enabling global and cell-type specific gene expression in reptiles. Ubiquitous high-yield promoters such as CAG/CB7 or CMV drive high levels of expression in turtles; cell-type specific promoters such as hSyn (expression limited to neurons) and CaMKIIa (expression limited exclusively o mostly to excitatory neurons) appear similarly biased in turtles. Other cell-type specific promoters reported in the literature (fNPY, fPV, fSST) failed to express in turtles.
A second major aspect of my work focused on electrophysiological recordings using microelectrode arrays and the interpretation of extracellular signals recorded from cortex in ex vivo preparations. We observed that spike signals produced by pyramidal and inhibitory neurons were very often followed by a slower potential. We identified these slower potentials as reflections of synaptic currents, and thus of the axonal projections of the neurons, at least within the deep layers of cortex. This also resulted in a means to classify neurons as excitatory or inhibitory with much higher reliability than classical methods (e. g. spike width). The final aspect of my work concerns the use of optogenetics to dissect the mechanisms of cortical oscillations and wave propagation. I show that oscillations can be induced by light in turtle cortex after transfection with AAV2/1 carrying the gene for channelrhodopsin 2 (ChR2). By using the CaMKIIa promoter, ChR2 induced currents are limited to LII/III excitatory cells; we can therefore control excitatory drive to cortical networks. If this drive is strong enough, layer III inhibitory interneurons are recruited and fire in a concerted fashion, silencing the excitatory population. The visually evoked 20 Hz oscillations observed in chronically recorded animals (Schneider, 2015) or in anaesthetized animals (Fournier et al., in press) thus appear to result from a feedback loop between E and I cells within layers II & III. Details of these interactions are being investigated but - layer I interneurons, by contrast, do not seem to be involved. By pulsing light I could control the frequency of the oscillations within a range of several Hz around the natural oscillation frequency. Above this range, cortex could only follow the stimulus at a fraction (1/2, 1/3,...) of the light pulse frequency. Using a digital micromirror device, I limited activation of the cortical networks spatially, enabling the study of wave propagation in this system.
Reptilian cortex offers a relatively simple model system for a reductionist and comparative strategy on understanding cortical computations and dynamics. Turtle dorsal cortex could thus give fundamental insights to the primordial organization tional, computational and functional principles of cortical networks. These insights are relevant to our understanding of mammalian brains and may prove valuable to decipher fundamental questions of modern neuroscience.
To date, chemicals are used ubiquitous in everyday life and an increasing consumption of pharmaceuticals and personal care products and industrial chemicals results in an increased water pollution. Conventional wastewater treatment plants are not able to completely remove the variety of (polar) organic compounds from today’s wastewater and thus serve as constant key point sources for the unintentional release of (micro-)pollutants into the aquatic environment. Anthropogenic micropollutants are detectable in very low concentrations in almost every aquatic compartment and may cause adverse effects on aquatic organisms. Considering the current situation of water pollution and to enhance water quality with regard to environmental and human health, the implementation of advanced wastewater treatment technologies, such as ozonation and activated carbon filtration was extensively discussed and investigated in recent years. Yet, besides their advantages regarding the efficient removal of a variety of recalcitrant, organic compounds as well as pathogens from the wastewater, it is known that especially the treatment with ozone may lead to the formation of largely unknown ozonation by-products with often unknown toxicity and unknown threats to human and the environment. To address these topics the joint research project TransRisk aimed at the “characterization, communication and minimization of risks originating from emerging contaminants and pathogens in the water cycle”. Within this research project the present thesis focuses on the ecotoxicological investigation of emerging waterborne contaminants, including their potential transformation products (TPs). Additionally, focus was laid on the investigation of combined effects of anthropogenic contaminants and pathogens with effects especially on aquatic invertebrate organisms.
The potential ecotoxicological effects of the antiviral drug acyclovir and two of its structurally identified TPs, were investigated on three aquatic organisms (Raphidocelis subcapitata, Daphnia magna and embryos of Danio rerio). While the parent compound acyclovir caused no acute toxicity up to a tested concentration of 100 mg/l on any of the investigated organisms, both TPs were shown to exhibit an increased aquatic toxicity. Carboxy-acyclovir, the biodegradation product of acyclovir, significantly reduced reproduction of D. magna by 40% at 102 mg/l, and the ozonation product COFA significantly inhibited growth of green algae R. subcapitata (EC10 = 14.1 mg/l). In the present case, advanced wastewater treatment was shown to lead to the formation of TPs, that reveal a higher toxicity towards investigated organisms, than the parent compound. Results highlight the necessity of further research related to the topic of identification and characterization of TPs, formed during advanced wastewater treatment processes.
To investigate the potential reduction or enhancement of toxic effects of nine differently treated wastewater effluents, selected bioassays with Daphnia magna, Lumbriculus variegatus and Lemna minor were conducted in flow-through test systems on a pilot treatment plant. The different treatment processes included ozonation of conventional biological treatment, with subsequent filtration processes as well as membrane bioreactor treatment in combination with ozonation. While exposure to the conventionally treated wastewater did not result in significant impairing effects on D. magna and L. minor, a reduced abundance of L. variegatus (by up to 46%) was observed compared to the medium control. Subsequent ozonation and additional filtration of the wastewater enhanced water quality, visible in an improved performance of L. variegatus. In general, direct evidence for the formation of toxic TPs due to the advanced wastewater treatments was not found, at least not in concentrations high enough to cause measurable effects in the investigated test systems. Additionally, no evidence for immunotoxic effects of the investigated wastewater effluents were observed. Yet, study-site- and species-specific effects hindered the definite interpretation of results. That underline the importance of a suitable test battery consisting of representatives of different taxonomic groups and trophic levels, to ensure a comprehensive evaluation of the complex matrix of wastewater and to avoid false-negative or false-positive results.
With aim to improve knowledge regarding immunotoxicity in invertebrates, the potential immunotoxic effects of the immunosuppressive pharmaceutical cyclosporine A (CsA) were investigated by applying the host-parasite model system Daphnia magna – Pasteuria ramosa in an adapted host resistance assay. Co-exposure to CsA and Pasteuria synergistically affected long-term survival of D. magna. Additionally, the enhanced virulence of the pathogen upon chemical co-exposure was expressed in synergistically increased infection rates and an increased speed of Pasteuria-induced host sterilization. In conclusion, results provide evidence for a suppressed disease resistance in a chemically stressed invertebrate host, highlighting the importance of investigating the conjunction of environmental pollutants and pathogens in the environmental risk assessment of anthropogenic pollutants.
Die Analyse früher Entwicklungsstadien von Säugetierembryonen und daraus gewonnener Stammzelllinien kann entscheidende Erkenntnisse im Bereich der Reproduktionsbiologie und der regenerativen Medizin hervorbringen. Dabei spielt die Maus, als geeignetes Modellsystem für die Übertragbarkeit auf den Menschen eine wichtige Rolle, in erster Linie weil die Blastozysten der Maus verglichen mit menschliche Blastozysten eine morphologische Ähnlichkeit aufweisen. Humane embryonale Stammzelllinien haben großes Potential für die Anwendung in der regenerativen Medizin und vergleichend dazu wurde Gen-Targeting in embryonalen Stammzellen verwendet, um tausende neuer Mausstämme zu generieren. Die Gewinnung embryonaler Stammzellen erfolgt im Blastozystenstadium, diese können dann nach Injektion in eine andere Blastozyste zur Entwicklung aller Gewebearten, einschließlich der Keimbahngewebe, beitragen (Martin, 1981; Evans and Kaufman 1981).
Ursache einer Fehlgeburt können vor allem Defekte in der Entwicklung des Trophoblasten und des primitive Entoderms (PrE) sein, dabei sind ca. 5 % der Paare betroffen die versuchen ein Kind zu bekommen (Stephenson and Kutteh, 2007). Eine Untersuchung dieser Zelllinien im Mausmodell könnte weitere Erkenntnisse für die Gründe einer Fehlentwicklung liefern. Trophoblasten Stammzelllinien können aus den Blastozysten der Maus und dem extraembryonalen Ektoderm von bereits implantieren Embryonen gewonnen werden (Tanaka et al., 1998). Diese Zelllinien geben Aufschluss über die Entwicklung des Trophoblasten, fördern die Entwicklung der Plazenta und sind gleichzeitig ein gutes Modellsystem um die Implantation des Embryos im Uterus näher zu untersuchen. Zellen des primitive Entoderms (PrE) beeinflussen das im Dottersack vorhandene extraembryonale Entoderm, welches dort als “frühe Plazenta” fungiert und für die Versorgung des Embryos mit Nährstoffen zuständig ist (Cross et al., 1994). Des Weiteren besitzt das Entoderm einen induktiven Einfluss auf die Bildung von anterioren Strukturen und die Bildung von Endothelzellen sowie Blutinseln (Byrd et al., 2002).
Extraembryonale Endodermstammzellen (XEN Zellen) können aus Blastozysten gewonnen und in embryonale Stammzellen (ES-Zellen) umgewandelt werden (Fujikura et al., 2002; Kunath et al., 2005). Es war jedoch nicht bekannt, ob XEN-Zellen auch aus Postimplantations-Embryonen gewonnen werden können. XEN-Zellen tragen in vivo zur Entwicklung des Darmendoderms bei (Kwon et al., 2008; Viotti et al., 2014) und könnten als alternative, selbsterneuernde Quelle für extraembryonale Endoderm-abgeleitete Zellen dienen, die zur Herstellung von Geweben für die regenerative Medizin verwendet werden könnten (Niakan et al., 2013).
In der Embryogenese der Maus zeigt sich an Tag E3.0 eine kompakte Morula die sich allmählich in das Trophektoderm (TE) differenziert, welches wiederum den Embryonalknoten (“innere Zellmasse”) umschließt (Johnson and Ziomek, 1981). Ein wichtiger Schritt im Rahmen der Entwicklung findet an Tag E3.5 statt, in diesem Zeitraum gehen aus dem Embryonalknoten der pluripotente Epiblast und das primitive Entoderm hervor. Im späten Blastozystenstadium an Tag E4.5 liegt das PrE als Zellschicht entlang der Oberfläche der Blastocoel-Höhle. Aus dem Epiblast entwickeln sich im weiteren Verlauf der Embryo, das Amnion und das extraembryonale Mesoderm des Dottersacks. Die Zellen des Trophektoderm führen zur Entwicklung der Plazenta. Das PrE differenziert sich im Zuge der Weiterentwicklung in das viszerale Entoderm (VE) und das parietale Entoderm (PE) des Dottersacks (Chazaud et al., 2006; Gardner and Rossant, 1979; Plusa et al., 2008). VE umgibt den Epiblast und extraembryonisches Ektoderm (ExE). PE-Zellen wandern entlang der inneren Oberfläche von TE und sezernieren zusammen mit Trophoblasten-Riesenzellen Basalmembranproteine, um die Reichert-Membran zu bilden (Hogan et al., 1980). Die Reichert-Membran besteht aus Basalmembranproteinen, einschließlich Kollagenen und Lamininen, die zwischen den parietalen Endoderm- und Trophoblastzellen liegen. Diese Membran wirkt als ein Filter, der dem Embryo den Zugang zu Nährstoffen ermöglicht, während er eine Barriere zu den Zellen der Mutter bildet (Gardner, 1983).
...
Angesichts heutiger Umweltprobleme ist die Stärkung positiver Mensch-Natur-Beziehungen wichtiger denn je. Zeitgenössische Umweltbildung zielt darauf ab, Motivation und Einstellungen zu fördern sowie eine grundlegende Wissensbasis zu schaffen (IUCN, UNEP, & WWF, 1991; Potter, 2010), um einen selbstbestimmten, verantwortungsvollen Umgang mit der Natur zu ermöglichen. Positiver Naturbezug und Umwelteinstellungen gelten als Basis für aktiven Umweltschutz. Direkte Naturerfahrungen gelten dabei als didaktische Möglichkeit, die Motivation für Umweltschutz zu festigen (Kaiser, Roczen, & Bogner, 2008). Einstellungen verändern sich im Laufe des Lebens und so kann das Alter eine wichtige Rolle bezüglich der Effektivität von Umweltbildungsprogrammen spielen (Ernst & Theimer, 2011). Auch Umweltwissen gilt als Grundlage von Umwelthandeln. Denn sinnliche Erfahrungen allein führen nicht zum Verständnis ökologischer Zusammenhänge (Frick, Kaiser, & Wilson, 2004; Liefländer, Bogner, Kibbe, & Kaiser, 2015). Die biologiedidaktische Forschung sieht Fakten-, Handlungs- und Effektivitäts-wissen als zentral für die Genese von Umwelthandeln (Frick, Kaiser, & Wilson, 2004). Isoliertes Fachwissen wiederum führt nach aktueller Erkenntnis auch nicht zur Entwicklung von Haltungen und Wertvorstellungen, welche unser Handeln beeinflussen (Barr, 2003; Finger, 2010; Leiserowitz, Kates, & Parris, 2005).
Bis heute sind altersbasierte Unterschiede bei Schülerinnen und Schülern bezüglich ihrer Naturverbundenheit und Umwelteinstellungen nicht hinreichend untersucht. Auch ist die nötige Dauer der Naturerfahrungen noch nicht nachgewiesen. Es gibt bislang keine Studie, die Umwelteinstellungen, -wissen und –handeln von Kindern verschiedener Regionen der Erde untersucht und Daten auf internationaler Ebene erhoben und ausgewertet hat. Die gezielte Integration der drei Umweltwissensarten in ein solch globales Umweltbildungsprojekt stellt eine zusätzliche bislang nicht angegangene Aufgabe dar. Die vorliegende Arbeit schließt diese Forschungslücken, indem sie auf internationaler Ebene jene Variablen mit einbezieht, die einen nahezu vollständigen Eindruck der Effektivität von Umweltbildung in verschiedenen Regionen, Sozialisationen und Altersklassen zulässt. So wird der Einfluss eines umfassenden Umweltbildungsprogramms auf Naturverbundenheit, Umwelteinstellungen und -wissen der verschiedenen Typen untersucht und ein Bezug zur eventuellen Veränderung des Umwelthandelns hergestellt. Dabei stehen sowohl traditionelle als noch unerforschte mögliche Einflussfaktoren im Fokus. Die Studie umfasst insgesamt 1454 Schülerinnen und Schüler aus Bangladesch, Malaysia, Deutschland und Singapur, die alle an dem Umweltbildungsprojekt „Global denken, lokal handeln – wir schützen unsere Umwelt!“ bzw. “Think global, act local – we protect our environment!“ teilgenommen haben.
Zur Messung der Naturverbundenheit diente Schulz’ INS-Skala (Inclusion of Nature in Self) (2002). Umwelteinstellungen wurden mit dem 2-MEV-Modell (Two Major Environmental Values) gemessen (Johnson & Manoli, 2011). Eine Skala zur Erhebung von Umweltwissen wurde eigens erstellt und hinsichtlich der drei Wissenstypen nochmals modelliert. Eine Skala zur Ermittlung von Umwelthandeln wurde auf Grundlage von Bögeholz (1999) erstellt. Alle Skalen waren Teil eines Fragebogens, welcher in Form eines Pre-, Post- und Follow-up-Test eingesetzt wurde. Kinder aus Parallelklassen, die nicht am Projekt teilnahmen, aber Klassenunterricht zu den jeweiligen Themen erhielten, dienten als Kontrollgruppen.
Die Ergebnisse bestätigen einen positiven Effekt außerschulischer Umweltbildung bezüglich der Entwicklung der untersuchten Variablen. So wurde nach der Teilnahme am eintägigen und auch nach dem fünftägigen Umweltbildungsprogramm eine signifikante Verstärkung des Naturbezugs gemessen, wohingegen die Kontrollgruppen keine messbare Veränderung zeigten. Jedoch nur die fünftägige Intervention führte auch zu nachhaltigen Veränderungen. Hierbei am stärksten beeinflusst wurden Kinder zwischen sieben und neun Jahren.
Bei der Untersuchung demographischer Einflussfaktoren auf Umwelteinstellung, -wissen und –handeln stellten sich das Wohnsitzland sowie die städtische bzw. ländliche Prägung der Wohngegend als entscheidend heraus. So waren dies die einflussreichsten Determinanten zur Vorhersage des Grundvorhandenseins sowie Veränderungen der untersuchten Variablen in Folge der Bildungsmaßnahme. Einzig bei der Entwicklung des Umwelthandelns schien die direkte Naturerfahrung unwesentlich, zeigten die Kontrollgruppen ähnlichen Wandel in ihrem aktiven Einsatz für die Umwelt. Im internationalen Vergleich scheint die komplexe Verkettung diverser einflussnehmender Faktoren, wie der Wohlstand des jeweiligen Staates, das generelle politische System sowie spezifische bildungspolitische Begebenheiten, den Erfolg von Umweltbildungsprogrammen mit zu bestimmen.
Die Daten zeigen, dass Faktenwissen Grundlage für Handlungs- und Effektivitätswissen ist. Alle Dimensionen wurden durch die Intervention signifikant gesteigert. Effektivitätswissen wuchs am stärksten. Auch das Umweltverhalten wurde positiv verstärkt. Jedoch ließen sich nur schwache Korrelationen zwischen den einzelnen Wissenstypen und Handeln feststellen. Zusammenfassend war das durchgeführte Bildungsprojekt erfolgreich in der Förderung von Naturverbundenheit sowie Umwelteinstellungen, -wissen und- handeln. Die Ergebnisse werden im Rahmen dieser Arbeit im Hinblick auf ihre Bedeutung für die schulische Umweltbildung sowie die didaktische Forschung erörtert.
Colorectal cancer (CRC) has the third highest incidence and the fourth highest mortality rate worldwide and represents a substantial health care burden and affects the life of millions of people. CRC is a genetic disease caused by the stepwise accumulation of genetic alterations. The initiating event in colorectal carcinogenesis is the aberrant activation of the WNT pathway, but other pathways are also commonly deregulated, including the PI3K/AKT pathway. A number of previous studies using genetically engineered mouse models aimed at dissecting the exact role of PI3K/AKT pathway in CRC, but have yielded in rather conflicting results. Despite the inconsistent results, these studies already put forward the idea that PI3K/AKT signaling in combination with other genetic events might substantially contribute to tumor progression. Since the PI3K/AKT pathway is frequently activated in CRC, it represents an ideal candidate for therapeutic intervention. Although extensive efforts had led to the development of numerous inhibitors targeting the PI3K/AKT pathway, the diversity of genetic alterations can challenge the identification of the most effective therapeutic targets. Therefore, the discovery of shared tumor-promoting mechanisms downstream of these genetic alterations might unravel new biomarkers and druggable targets. The aim of this study was to elucidate the precise role of PI3K/AKT pathway during the course of colorectal carcinogenesis and to decipher novel protumorigenic molecular mechanisms downstream of PI3K/AKT activation that can be used for therapeutic intervention.
To obtain a better insight into the role of the PI3K/AKT pathway during colorectal carcinogenesis, mice expressing an oncogenic variant of AKT1 (AktE17K) specifically in the intestinal epithelial cells (IEC) were used. At the age of 6 months untreated AktE17K mice showed clearly perturbed intestinal homeostasis, but no tumor formation. To induce colonic tumorigenesis, AktE17K mice were subjected to treatment with the colonic carcinogen azoxymethane (AOM). In response to AOM, AktE17K mice developed invasive but non-metastatic tumors, which showed strong nuclear accumulation of TP53. To investigate the role of PI3K/AKT signaling specifically in CRC progression, AktE17K mice were crossed to TP53-deficient mice (Tp53ΔIEC). Unlike AktE17K mice, untreated Tp53ΔIEC; AktE17K, developed highly invasive small
intestinal tumors by the age of 6 months. To investigate the role of AKT hyperactivation in colonic tumor progression, Tp53ΔIEC; AktE17K mice were subjected to AOM treatment. AKT hyperactivation significantly enhanced tumor progression and induced metastatic dissemination.
To get a better insight how AKT signaling can promote tumor progression, whole tumor tissues from AOM-treated Tp53ΔIEC and Tp53ΔIEC; AktE17K mice were subjected to next generation mRNA sequencing and phospho-proteomic analysis by mass spectrometry. Both analyses indicated that AKT hyperactivation expands the inflammatory tumor microenvironment and upregulates pathways associated with invasion and metastasis. Importantly, Gene Set Enrichment Analysis revealed that AOM-induced colon tumors of Tp53ΔIEC; AktE17K animals, are highly similar in their gene expression profile to the CMS4 subtype of human CRC, which is associated with worse overall- and relapse-free survival. Gene expression analysis also suggested elevated NOTCH signaling in the Tp53ΔIEC; AktE17K tumors. Interestingly, while the expression of Notch3 mRNA was increased in the tumors of Tp53ΔIEC; AktE17K mice, the expression of the other NOTCH receptors was unaffected by AKT hyperactivation. In vitro experiments using TP53-deficient mouse tumor organoids with hyperactive AKT signaling confirmed the direct, tumor cell-intrinsic link between AKT activation and increased Notch3 expression. Moreover, inhibition of EZH2 mimicked the effect of AKT hyperactivation on Notch3 expression, suggesting that AKT regulates Notch3 via an epigenetic mechanism.
Knock-down of Notch3 in TP53-deficient mouse tumor organoids with hyperactive AKT signaling resulted in differential regulation of several pathways with potential role in invasion and metastasis and in cell death and survival. Subsequent in vivo experiments confirmed the role of NOTCH3 signaling in CRC progression. Treatment of AOM-induced Tp53ΔIEC; AktE17K mice with a NOTCH3 antagonistic antibody or the γ-secretase inhibitor DAPT significantly reduced invasion and metastasis. Importantly, NOTCH3 expression was also found to be associated with human CRC progression, suggesting that NOTCH3 represent a valid target for the treatment of CRC. This work, using genetically engineered mouse models and advanced in vitro techniques, has demonstrated a strong tumor promoting role for PI3K/AKT signaling in CRC progression and has identified NOTCH3 signaling as a potential therapeutic target downstream of the PI3K/AKT pathway.
Microsporidia are a group of parasites that infect a wide range of species, many of which play important roles in agriculture and human disease. At least 14 microsporidian species have been confirmed to cause potentially lifethreatening infectious diseases in both immunocompromised and immunocompetent humans. Approximately 1,400 species of microsporidia have been described. Depending on their host and habitat they are classified into three groups, the aquasporidia, the terresporidia and the marinosporidia.
Microsporidia were originally classified as fungi by Naegeli (1857). However, their lack of typical eukaryotic components – such as mitochondria, Golgi bodies or peroxisomes – suggested to place the microsporidia together with other amitochondriate protists within the Archezoa kingdom. This "microsporidia-early" hypothesis was further supported by molecular phylogenies inferred from individual genes. Despite this evidence, the placement of microsporidia as an early branching eukaryote remained a topic for debate. The phylogeny of microsporidia is prone to suffer from biases in their reconstruction. The high evolutionary rate of microsporidian proteins tends to place these proteins together with other fast evolving lineages, a phenomenon known as long-branch attraction. In 1996, the first molecular phylogenetic studies placed the microsporidia inside the fungi.
Subsequently, several further studies located the microsporidia at different positions inside the fungal clade. Since then, microsporidia have been considered as members of the Ascomycota, Zygomycota, Cryptomycota, or as a sister group to the Ascomycota and Basidiomycota, or even as the sister group of all fungi.
The difficulties in determining the evolutionary origin of microsporidia are not only caused by their lack of several cellular components but also by their reduced genomes and metabolism. Being obligate intracellular parasites, microsporidia successfully reduced their genome sizes, down to the range of bacteria. As the smallest eukaryotic genome described so far, the genome of Encephalitozoon intestinalis is just 2.3 Mbp, about half the size of the one of Escherichia coli. Due to their low number of protein coding genes (less than 4,000), microsporidia are thought to retain only genes essential for their survival and development. Furthermore, several key metabolic pathways are missing in the microsporidia, such as the citric acid cycle, oxidative phosphorylation, or the de novo biosynthesis of nucleotides. As a result they are in an obligatory dependence on many primary metabolites from the hosts. However, the presence of hsp70 protein suggests a more complex genome of the microsporidian ancestor. Consequently, the small microsporidian genomes and the reduced metabolism would be consequences of a secondary loss process that molded the contemporary microsporidia from a functionally more complex ancestral species. However, it remains unclear whether the last common ancestor (LCA) of the microsporidia was already reduced, or whether the genome compaction was lineage-specific and started from a more complex LCA.
We investigated the evolutionary history of the contemporary microsporidia through the reconstruction and analysis of their LCA. As a first step in our analysis, we have developed and implemented a software facilitating an intuitive data analysis of the large presence absence-patterns resulting from the tracing of microsporidian proteins in gene sets of many different species. These so called phylogenetic profiles can now be dynamically visualized and explored with PhyloProfile. The software allows the integration of other additional information layers into the phylogenetic profile, such as the similarity of feature architecture (FAS) between the protein under study and its orthologs. The FAS score can be displayed along the presence-absence pattern, which can help to identify orthologs that have likely diverged in function. PhyloProfile closes the methodological gap that existed between tools to generate large phylogenetic profiles to delineate the evolutionary history and the contemporary distribution of large – and ultimately complete – gene sets, and the more function-oriented analysis of individual protein. In the next step we tackled the problem of how to transfer functional annotation from one protein to another. We have developed HamFAS that integrates a targeted ortholog search based on the HaMStR algorithm with a weighted assessment of feature architecture similarities (FAS) between orthologs. In brief, for a seed protein we identify orthologs in reference species in which proteins have been functionally annotated based on manually curated assignments to KEGG Ortholog (KO) groups. The FAS scores between the orthologs and seed proteins are calculated. Subsequently, we compute pairwise FAS scores for all reference proteins within a KO group. A group's mean FAS score serves then as cutoff that must be exceeded to warrant transfer of its KO identifier to the seed. A benchmark using a manually curated yeast protein set showed that HamFAS yields the best precision (98.5%) when compared with two state-of-the-art annotation tools, KAAS and BlastKOALA. Furthermore, HamFAS achieves a higher sensitivity. On average HamFAS annotates almost 50% more proteins than KAAS or BlastKOALA.
With this extended bioinformatics toolbox at hand, we aimed at reconstructing the evolutionary history of the microsporidia. We generated a robust phylogeny of microsporidia using a phylogenomics approach. As a data basis, we identified a set of microsporidian proteins encoded by 80 core genes with one-to-one orthologs. A maximum likelihood analysis of this data
with 48 fungi and additionally in 13 species from more distantly related such as animals and plants combined in a supermatrix strongly supported the hypothesis that microsporidia form the sister group of the fungi. We confirmed that the data explains this microsporidia-fungi relationship significantly better than any other of the previously proposed phylogenetic hypotheses.
On the basis of this phylogeny, and of the phylogenetic profiles of microsporidian proteins, we then focused on reconstructing the dynamics microsporidian genome evolution. Between 2% of the proteins in the compact microsporidia Encephalitozoon intestinalis and up to 49% of the proteins of Edhazardia aedis are private for individual microsporidian species. A comparison of the sequence characteristics of these proteins to that of proteins with orthologs in other microsporidian species revealed individual differences. Yet, without further evidences it remains unclear whether these private genes are indeed lineage-specific innovations contributing to the adaptation of each microsporidium to its host, or whether these are artifacts introduced in the process of gene annotation. A total of 14,410 microsporidian proteins could then be grouped into 1605 orthologous groups that can be traced back to the last common ancestor of the microsporidia (LCA set). We found that 94% of the microsporidian LCA proteins could be tracked back to the last eukaryotic common ancestor. The high evolutionary age of these proteins, together with the resistance against gene loss in the microsporidia suggests that the corresponding functions are essential for eukaryotic life. Further 3% of the LCA proteins could be dated to the common ancestor microsporidia share with the fungi. Only 3% of the LCA proteins appear as microsporidia specific inventions. These proteins are potentially of importance for the evolutionary of the obligate parasitic lifestyle nowadays shared by all microsporidia.
The functional annotation and metabolic pathway analysis of the microsporidian LCA protein set gave us more insight into the adaptation of the microsporidia to their parasitic lifestyle and the origin of the microsporidian genome reduction. The presence of E1 and E3 components of the pyruvate dehydrogenase complex and the mitochondrial hsp70 protein support an ancestral presence of mitochondria in the ancestral microsporidia. In addition, several ancient proteins that complement gapped metabolic pathways were found in the microsporidian LCA. They suggested a more complex genome and metabolism in the LCA. However, our reconstruction of the metabolic network of the microsporidian LCA still lacks many main pathways. For example, the TCA cycle for effective energy production, and key enzymes that are required for in vivo synthesis of critical metabolites like purines and pyrimidines appear absent. We therefore find that the parasitic lifestyle and the genome reduction already occurred in the microsporidian LCA. This ancestral state was followed by further losses and gains during the evolution of each individual microsporidian lineage.
In conclusion, I described for the first time the in vivo functions of PAK2 during cardiac development and its requirement for heart contractility
AIM1 – Characterization of Pak2a and Pak2b functions during cardiovascular system development: description of the phenotype triggered by the loss of expression of pak2b in the pak2a mutant Firstly, in addition to the confirmation of the published data regarding the pak2a mutant and morphant phenotype, I showed that pak2bbns159 mutant does not exhibit morphological defects, neither in the ISV formation nor in the brain vascular patterning. More importantly, I analyzed in more details the phenotypic consequences of pak2a and pak2b loss of expression in the trunk and brain vasculatures. Indeed, the lack of blood flow in the embryos, was associated with central arteries migration defects and reduced lumen in these central arteries and the ISVs. Moreover, pak2a and pak2b loss of expression resulted in cardiac failure.
AIM2 – Role of Pak2 on cardiac contractility From 40 -46 hpf, I found a weaker heart contractility in the pak2ami149/mi149;pak2bbns159/bns159. Although, the PAK proteins have been shown to impact the actin cytoskeleton organization, the heart morphological defects associated with the altered contractility, were not associated with acto-myosin filament reorganization. However, by analyzing in more details the structure of the sarcomeres, I was able to demonstrate that the proteins constituting the sarcomeres were strongly affected and showed an altered spatial organization. Then, I also described the effects of the loss of expression of both paralogs on the junctional protein localization. I demonstrated the loss of Pak2 function resulted in junction protein rearrangement in the cardiomyocytes in the pak2ami149/mi149;pak2bbns159/bns159 mutants at 40 and 46 hpf.
Thus, I was able for the first time to demonstrate in vivo PAK2 functions during cardiac development and its requirement for proper cardiac contractility activity.
AIM3 – Decipher mechanism of Pak2 signaling cascade involved during cardiac development Both pak2a and pak2b WT mRNAs were able to rescue the pak2ami149/mi149;pak2bbns159/bns159 mutant heart defects and the results indicated that these paralogs share overlapping function during cardiac development. Moreover, although I was not able to examine the control transgenic lines, myocardial and endothelial specific pak2a overexpression did not ameliorate the mutant cardiac deficiency. Thus,the absence of rescue by reactivating pak2a in cardiomyocytes indicates a non-cell autonomous function of Pak2a on cardiomyocytes.
For the first time, this study allowed to follow PAK2 in vivo functions during cardiovascular development. More importantly, its role on heart contractility regulation would enable further investigations to generate new tools for the treatment of cardiomyopathies.
The fungal interaction with plants is a 400 million years old phenomenon, which presumably assisted in the plants’ establishment on land. In a natural ecosystem, all plant-ranging from large trees to sea-grasses-are colonized by fungal endophytes, which can be detected inter- and intracellularly within the tissues of apparently healthy plants, without causing obvious negative effects on their host. These ubiquitous and diverse microorganisms are likely playing important roles in plant fitness and development. However, the knowledge on the ecological functions of fungal root endophytes is scarce. Among possible functions of endophytes, they are implicated in mutualisms with plants, which may increase plant resistance to biotic stressors like herbivores and pathogens, and/or to abiotic factors like soil salinity and drought. Also, endophytes are fascinating microorganisms in regard to their high potential to produce a great spectrum of secondary metabolites with expected ecological functions. However, evidences suggest that the interactions between host plants and endophytes are not static and endophytes express different symbiotic lifestyles ranging from mutualism to parasitism, which makes difficult to predict the ecological roles of these cryptic microorganisms. To reveal the ecological function of fungal root endophytes, this doctoral thesis aims at assessing fungal root endophytes interactions with different plants and their effects on plant fitness, based on their phylogeny, traits, and competition potential in settings encompassing different abiotic contexts. To understand the cryptic implication of nonmycorrhizal endophytes in ecosystem processes, we isolated a diverse spectrum of fungal endophytes from roots of several plant species growing in different natural contexts and tested their effects on different model plants under axenic laboratory conditions. Additionally,we aimed at investigating the effect of abiotic and biotic variables on the outcome of interactions between fungal root endophytes and plants.
In summary, the morphological and physiological traits of 128 fungal endophyte strains within ten fungal orders were studied and artificial experimental systems were used to reproduce their interactions with three plant species under laboratory conditions. Under defined axenic conditions, most endophytes behaved as weak parasites, but their performance varied across plant species and fungal taxa. The variation in the interactions was partly explained by convergent fungal traits that separate groups of endophytes with potentially different niche preferences. According to my findings, I predict that the functional complementarity of strains is essential in structuring natural root endophytic communities. Additionally, the responses of plant-endophyte interactions to different abiotic factors, namely nutrient availability, light intensity, and substrate’s pH, indicate that the outcome of plant-fungus relationships may be robust to changes in the abiotic environment. The assessment of the responses of plant endophyte interactions to biotic context, as combinations of selected dominant root fungal endophytes with different degrees of trait similarity and shared evolutionary history, indicates that frequently coexisting root-colonizing fungi may avoid competition in inter-specific interactions by occupying specific niches, and that their interactions likely define the structure of root-associated fungal communities and influence the microbiome impacts on plant fitness.
In conclusion, my findings suggest that dominant fungal lineages display different ecological preferences and complementary sets of functional traits, with different niche preferences within root tissues to avoid competition. Also, their diverse effects on plant fitness is likely host-isolate dependent and robust to changes in the abiotic environment when these encompass the tolerance range of either symbiont.
Colorectal cancer (CRC) has the third highest incidence and the fourth highest mortality rate worldwide and represents a substantial health care burden and affects the life of millions of people. CRC is a genetic disease caused by the stepwise accumulation of genetic alterations. The initiating event in colorectal carcinogenesis is the aberrant activation of the WNT pathway, but other pathways are also commonly deregulated, including the PI3K/AKT pathway. A number of previous studies using genetically engineered mouse models aimed at dissecting the exact role of PI3K/AKT pathway in CRC, but have yielded in rather conflicting results. Despite the inconsistent results, these studies already put forward the idea that PI3K/AKT signaling in combination with other genetic events might substantially contribute to tumor progression.
Since the PI3K/AKT pathway is frequently activated in CRC, it represents an ideal candidate for therapeutic intervention. Although extensive efforts had led to the development of numerous inhibitors targeting the PI3K/AKT pathway, the diversity of genetic alterations can challenge the identification of the most effective therapeutic targets. Therefore, the discovery of shared tumor-promoting mechanisms downstream of these genetic alterations might unravel new biomarkers and druggable targets. The aim of this study was to elucidate the precise role of PI3K/AKT pathway during the course of colorectal carcinogenesis and to decipher novel pro-tumorigenic molecular mechanisms downstream of PI3K/AKT activation that can be used for therapeutic intervention.
To obtain a better insight into the role of the PI3K/AKT pathway during colorectal carcinogenesis, mice expressing an oncogenic variant of AKT1 (AktE17K) specifically in the intestinal epithelial cells (IEC) were used. At the age of 6 months untreated AktE17K mice showed clearly perturbed intestinal homeostasis, but no tumor formation. To induce colonic tumorigenesis, AktE17K mice were subjected to treatment with the colonic carcinogen azoxymethane (AOM). In response to AOM, AktE17K mice developed invasive but nonmetastatic tumors, which showed strong nuclear accumulation of TP53. To investigate the role of PI3K/AKT signaling specifically in CRC progression, AktE17K mice were crossed to TP53- deficient mice (Tp53ΔIEC). Unlike AktE17K mice, untreated Tp53ΔIECAktE17K, developed highly invasive small intestinal tumors by the age of 6 months. To investigate the role of AKT hyperactivation in colonic tumor progression, Tp53ΔIECAktE17K mice were subjected to AOM treatment. AKT hyperactivation significantly enhanced tumor progression and induced metastatic dissemination.
To get a better insight how AKT signaling can promote tumor progression, whole tumor tissues from AOM-treated Tp53ΔIEC and Tp53ΔIECAktE17K mice were subjected to next generation mRNA sequencing and phospho-proteomic analysis by mass spectrometry. Both analyses indicated that AKT hyperactivation expands the inflammatory tumor microenvironment and upregulates pathways associated with invasion and metastasis. Importantly, Gene Set Enrichment Analysis revealed that AOM-induced colon tumors of Tp53ΔIECAktE17K animals, are highly similar in their gene expression profile to the CMS4 subtype of human CRC, which is associated with worse overall- and relapse-free survival7 . Gene expression analysis also suggested elevated NOTCH signaling in the Tp53ΔIECAktE17K tumors. Interestingly, while the expression of Notch3 mRNA was increased in the tumors of Tp53ΔIECAktE17K mice, the expression of the other NOTCH receptors was unaffected by AKT hyperactivation. In vitro experiments using TP53-deficient mouse tumor organoids with hyperactive AKT signaling confirmed the direct, tumor cell-intrinsic link between AKT activation and increased Notch3 expression. Moreover, inhibition of EZH2 mimicked the effect of AKT hyperactivation on Notch3 expression, suggesting that AKT regulates Notch3 via an epigenetic mechanism.
Knock-down of Notch3 in TP53-deficient mouse tumor organoids with hyperactive AKT signaling resulted in differential regulation of several pathways with potential role in invasion and metastasis and in cell death and survival. Subsequent in vivo experiments confirmed the role of NOTCH3 signaling in CRC progression. Treatment of AOM-induced Tp53ΔIECAkt E17K mice with a NOTCH3 antagonistic antibody or the γ-secretase inhibitor DAPT significantly reduced invasion and metastasis. Importantly, NOTCH3 expression was also found to be associated with human CRC progression, suggesting that NOTCH3 represent a valid target for the treatment of CRC. This work, using genetically engineered mouse models and advanced in vitro techniques, has demonstrated a strong tumor promoting role for PI3K/AKT signaling in CRC progression and has identified NOTCH3 signaling as a potential therapeutic target downstream of the PI3K/AKT pathway.