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  • 1
    Keywords: Forschungsbericht ; Mekongdelta ; Wasseraufbereitung ; Nährstoffkreislauf
    Type of Medium: Online Resource
    Pages: Online-Ressource (52 S., 425 KB) , Ill., graph. Darst
    Language: German
    Note: Förderkennzeichen BMBF 02WD0413 - 02WD0414 - 02WD0415. - Verbund-Nr. 01023340. - Engl. Titel: Closing nutrient cycles by hygienically safe substrates in decentralised water management systems in the Mekong Delta, Vietnam (SANSED) , Unterschiede zwischen dem gedruckten Dokument und der elektronischen Ressource können nicht ausgeschlossen werden , Auch als gedr. Ausg. vorhanden , Teilprojekt 1: Rheinische Friedrich-Wilhelm Universität Bonn, Institut für Pflanzenernährung (02WD0413) / Joachim Clemens; Teilprojekt 2: Ruhr-Universität Bochumg, Institut f. Umweltechnik u. Ökologie im Bauwesen (02WD0414) / Harro Stolpe und Teilprojekt 3: Ith - Ingenieurbüro für technische Hydrologie (02WD0415) / Thilo Herrmann , Systemvoraussetzungen: Acrobat reader.
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  • 2
    Publication Date: 2015-03-20
    Description: Background: Using auditory discrimination learning in gerbils, we have previously shown that activation of auditory-cortical D1/D5 dopamine receptors facilitates mTOR-mediated, protein synthesis-dependent mechanisms of memory consolidation and anterograde memory formation. To understand molecular mechanisms of this facilitatory effect, we tested the impact of local pharmacological activation of different D1/D5 dopamine receptor signalling modes in the auditory cortex. To this end, protein patterns in soluble and synaptic protein-enriched fractions from cortical, hippocampal and striatal brain regions of ligand- and vehicle-treated gerbils were analysed by 2D gel electrophoresis and mass spectrometry 24 h after intervention. Results: After auditory-cortical injection of SKF38393 – a D1/D5 dopamine receptor-selective agonist reported to activate the downstream effectors adenylyl cyclase and phospholipase C – prominent proteomic alterations compared to vehicle-treated controls appeared in the auditory cortex, striatum, and hippocampus, whereas only minor changes were detectable in the frontal cortex. In contrast, auditory-cortical injection of SKF83959 – a D1/D5 agonist reported to preferentially stimulate phospholipase C – induced pronounced changes in the frontal cortex. At the molecular level, we detected altered regulation of cytoskeletal and scaffolding proteins, changes in proteins with functions in energy metabolism, local protein synthesis, and synaptic signalling. Interestingly, abundance and/or subcellular localisation of the predominantly presynaptic protein α-synuclein displayed dopaminergic regulation. To assess the role of α-synuclein for dopaminergic mechanisms of memory modulation, we tested the impact of post-conditioning systemic pharmacological activation of different D1/D5 dopamine receptor signalling modes on auditory discrimination learning in α-synuclein-mutant mice. In C57BL/6JOlaHsd mice, bearing a spontaneous deletion of the α-synuclein-encoding gene, but not in the related substrains C57BL/6JCrl and C57BL/6JRccHsd, adenylyl cyclase-mediated signalling affected acquisition rates over future learning episodes, whereas phospholipase C-mediated signalling affected final memory performance. Conclusions: Dopamine signalling modes via D1/D5 receptors in the auditory cortex differentially impact protein profiles related to rearrangement of cytomatrices, energy metabolism, and synaptic neurotransmission in cortical, hippocampal, and basal brain structures. Altered dopamine neurotransmission in α-synuclein-deficient mice revealed that distinct D1/D5 receptor signalling modes may control different aspects of memory consolidation.
    Electronic ISSN: 1477-5956
    Topics: Medicine
    Published by BioMed Central
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