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Modeling and treatment of rat cervical spinal cord injuryGensel, John Carib 05 January 2007 (has links)
No description available.
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Differential regulation of GABAB receptor trafficking by different modes of N-methyl-D-aspartate (NMDA) receptor signalingKantamneni, Sriharsha, Gonzàlez-Gonzàlez, I.M., Luo, J., Cimarosti, H., Jacobs, S.C., Jaafari, N., Henley, J.M. 2013 December 1924 (has links)
Yes / Inhibitory GABAB receptors (GABABRs) can down-regulate most excitatory synapses in the CNS by reducing postsynaptic excitability. Functional GABABRs are heterodimers of GABAB1 and GABAB2 subunits and here we show that the trafficking and surface expression of GABABRs is differentially regulated by synaptic or pathophysiological activation of NMDA receptors (NMDARs). Activation of synaptic NMDARs using a chemLTP protocol increases GABABR recycling and surface expression. In contrast, excitotoxic global activation of synaptic and extrasynaptic NMDARs by bath application of NMDA causes the loss of surface GABABRs. Intriguingly, exposing neurons to extreme metabolic stress using oxygen/glucose deprivation (OGD) increases GABAB1 but decreases GABAB2 surface expression. The increase in surface GABAB1 involves enhanced recycling and is blocked by the NMDAR antagonist AP5. The decrease in surface GABAB2 is also blocked by AP5 and by inhibiting degradation pathways. These results indicate that NMDAR activity is critical in GABABR trafficking and function and that the individual subunits can be separately controlled to regulate neuronal responsiveness and survival. / BBSRC, MRC and the European Research Council
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Die Bedeutung der Proteine 4.1G und 4.1N für den Aufbau und die Funktion glutamaterger Synapsen / The role of proteins 4.1G and 4.1N for the composition and function of glutamatergic synapsesWolk, Friederike 09 July 2009 (has links)
No description available.
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Neuroligin-4: Einfluss auf die synaptische Übertragung exzitatorischer Neurone der Schicht IV des Barrel-Kortex / Neuroligin-4: Effect on synaptic transmission of excitatory neurons in layer IV of barrel-cortexOlt, Stephen 20 November 2013 (has links)
Neuroligine (NL) sind vorwiegend postsynaptisch lokalisierte transmembrane Adhäsionsmoleküle, die in Wechselwirkung mit dem präsynaptisch lokalisierten Protein Neurexin eine wichtige Rolle in der Reifung und Funktion von Synapsen spielen. Es existieren verschiedene NL-Isoproteine (NL-1 – NL-4), die sich in ihrer Assoziation zu exzitatorischen und inhibitorischen Synapsen unterscheiden. Die funktionelle und klinische Relevanz der Neuroligine belegen beispielhaft Mutationen des Isotyps NL 4, welche mit neuropsychiatrischen Erkrankungen wie Autismus-Spektrum-Störungen assoziiert vorkommen.
Anhand eines durch Ausschalten des human-orthologen NL-4-Gens generierten Mausmodells (NL 4 Knockout, NL 4 KO) konnte in vorhergehenden Studien die Bedeutung einer immunhistochemisch beobachteten Lokalisation von NL 4 an glycinergen Synapsen der Retina für die inhibitorische synaptische Übertragung nachgewiesen werden. Im Unterschied dazu konnte kein Zusammenhang zwischen einer in Schicht IV des Barrel-Kortex nachweisbaren Lokalisation von NL-4 mit inhibitorischen Synapsen hergestellt werden. Deshalb, und aufgrund der in Schicht IV dominierenden exzitatorischen Verschaltung von thalamischen Projektionen und den kolumnenassoziierten Rückverschaltungen aus dem Neokortex, lässt sich eine Interaktion von NL-4 mit exzitatorischen Synapsen in diesem Areal vermuten. Im Rahmen der vorliegenden Arbeit wurde anhand der NL-4-KO-Modellmaus der Frage nachgegangen, inwiefern NL-4 die exzitatorische synaptische Übertragung im Barrel-Kortex beeinflusst. Dafür wurden mit Hilfe der Patch-Clamp-Technik abgeleitete AMPA-Rezeptor-vermittelte exzitatorische postsynaptische Ströme (EPSC) von bedornten Sternzellen, Sternpyramiden- und Pyramidenzellen der Schicht IV ausgewertet und zwischen NL-4-Wildtyp- (NL 4-WT) und NL 4 KO-Neuronen verglichen. Dabei zeigten NL 4-KO-Neurone signifikant veränderte Parameter der EPSC-Kinetik. Die Abfallszeit war in NL 4 KO-Neuronen signifikant länger, das maximale Gefälle und die maximale Steigung signifikant flacher gegenüber NL-4-WT-Kontrollen. Diese Veränderungen sprechen für eine funktionelle Relevanz von NL-4 für die AMPA-Rezeptor-vermittelte synaptische Übertragung auf exzitatorische Neurone in Schicht IV des Barrel-Kortex. Das Muster der in NL-4-KO-Neuronen veränderten EPSC-Kinetik weist dabei auf eine Modulation der biophysikalischen AMPA-Rezeptoreigenschaften hin und könnte mit Veränderungen der synaptisch exprimierten AMPA-Rezeptor-TARP-Subtypen in Zusammenhang stehen, die über Proteine der postsynaptischen Dichte (wie PSD-95 und S SCAM) mit Neuroliginen interagieren.
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Estrogens Rapidly Enhance Neural Plasticity and LearningPhan, Anna 24 July 2013 (has links)
This thesis examines the rapid, non-genomic effects of estrogens on neural plasticity and learning. Estrogens are classically known to affect gene transcription events, however they have more recently been found to also rapidly activate second messenger systems within 1hr of administration. Therefore, we first examined the rapid effects of 17β-estradiol, and an estrogen receptor (ER) α and ERβ agonist on three different learning paradigms: object placement, object recognition, and social recognition. We found that both systemic injections and intrahippocampal delivery of 17β-estradiol and the ERα agonist improved performance on all 3 learning paradigms within 40min of hormone administration. However, the ERβ agonist administered systemically or intrahippocampally, improved performance only on the object placement learning paradigm, while having no effect on object recognition, and impairing social recognition at high doses. To elucidate how estrogens might rapidly affect learning, we examined how estrogens rapidly affect the neural plasticity of CA1 hippocampal neurons. We found that 17β-estradiol and the ERα agonist increased dendritic spine density in CA1 hippocampal neurons within 40min of administration, suggesting that estrogens rapidly increase the density of synapses within this brain region. Conversely, the ERβ agonist did not affect spine density, or decreased spine density. In addition, by using whole-cell patch clamp recordings of CA1 pyramidal neurons, we were able to determine that 17β-estradiol and the ERα agonist rapidly reduced AMPA receptor (but not NMDA receptor) mediated membrane depolarizations after 15min of hormone application. Similar to above, the ERβ agonist had no effect on AMPA or NMDA receptor mediated membrane depolarizations. These data suggest that estrogens rapidly promote the development of immature synapses (which contain low levels of synaptic AMPA receptors) within the CA1 hippocampus. Immature spines provide synaptic sites at which new memories can be stored and are thought of as “learning spines” (Kasai et al, 2003). Therefore, estrogens (through ERα) may rapidly induce the formation of hippocampal immature spines to promote learning. / Funded by NSERC
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Sound encoding in mutant mice with disrupted action potential generationYamanbaeva, Gulnara 21 August 2017 (has links)
No description available.
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Evaluating a Novel Photochemical Tool for Labeling and Tracking Live, Endogenous Calcium-Permeable AMPARsCombs-Bachmann, Rosamund Elizabeth 13 July 2016 (has links)
The purpose of this research is to advance development of a photochemical tool designed to probe the role of ionotropic glutamate receptor signaling in neurodegenerative processes, and to delve more deeply into the biological processes underlying the role of these receptors in signaling and memory formation. This ligand-targeted nanoprobe was designed and developed in our lab to label endogenous calcium-permeable AMPARs (CP-AMPARs) in live cells with minimal disruption to native receptor activity. Nanoprobe is designed to use naphthyl acetyl spermine (NASPM) as a photocleavable ligand to target and covalently label native CP-AMPARs with a non-perturbing, fluorescent marker that then allows observation of these receptors using standard epifluorescence microscopy. My contribution to this work, outlined in the aims below, is the characterization of nanoprobe using electrophysiology and fluorescent imaging to evaluate its effectiveness as an endogenous CP-AMPAR label on live neurons.
Aim 1: To use whole cell patch clamp electrophysiology to test the labeling of CP-AMPARs with nanoprobe by recording changes in glutamate-evoked current through heterologously expressed GluA1-L497Y homomultimers during, pre- and post- nanoprobe labeling.
Aim 2: To use fluorescent imaging to evaluate nanoprobe labeling of glutamate receptors endogenously expressed in hippocampal neurons by co-labeling nanoprobe-treated neurons with traditional antibodies to AMPAR and synaptic targets.
Aim 3: To use nanoprobe to detect endogenously expressed CP-AMPARs on live neurons during the course of neuron development. Live neuronal cultures will be imaged before and after labeling with nanoprobe in young dissociated cultures (DIV 1-2) and in maturing cultures (DIV 14-17).
Conclusions: Whole cell patch clamp electrophysiology results provide evidence that nanoprobe will label CP-AMPARs in a minimally-perturbing fashion that allows the receptors to resume normal activity after photolytic-release of ligand as designed. Fixed cell imaging of CP-AMPAR nanoprobe labeling was largely ineffective, and live cell imaging was not conclusive, but provided supporting evidence that nanoprobe targets and labels NASPM-sensitive endogenous glutamate receptors on live dissociated hippocampal neurons
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Analysis of CPEB Family Protein Member CPEB4 Function in Mammalian Neurons: A DissertationKan, Ming-Chung 01 June 2008 (has links)
Local protein synthesis is required for long-term memory formation in the brain. One protein family, Cytoplasmic Polyadenylation Element binding Protein (CPEB) that regulates protein synthesis is found to be important for long-term memory formation possibly through regulating local protein synthesis in neurons. The well-studied member of this family, CPEB1, mediates both translational repression and activation of its target mRNAs by regulating mRNA polyadenylation. Mouse with CPEB1 KO shows defect in memory extinction but not long-term memory formation. Three more CPEB1 homologs (CPEB2-4) are identified in mammalian system. To test if CPEB2-4 may have redundant role in replacing CPEB1 in mediating local protein synthesis, the RNA binding specificity of these homologs are studied by SELEX. The result shows CPEB2-4 bind to RNAs with consensus sequence that is distinct from CPE, the binding site of CPEB1. This distinction RNA binding specificity between CPEB1 and CPEB2-4 suggests CPEB2-4 cannot replace CPEB1 in mediating local protein synthesis. For CPEB2-4 have distinct RNA binding specificity compared to CPEB1, they are referred as CPEB-like proteins. One of CPEB-like protein, CPEB3, binds GluR2 mRNA and represses its translation. The subcellular localization of CPEB family proteins during glutamate over stimulation is also studied. The CPEB family proteins are identified as nucleus/cytoplasm shuttling proteins that depend on CRM1 for nuclear export. CPEB-like proteins share similar nuclear export ciselement that is not present in CPEB1. Over-stimulation of neuron by glutamate induces the nuclear accumulation of CPEB family proteins possibly through disrupted nuclear export. This nuclear accumulation of CPEB family protein is induced by imbalance of calcium metabolism in the neurons. Biochemical and cytological results suggest CPEB4 protein is associated with ER membrane peripherally in RNA independent manner. This research provides general description of biochemical, cytological properties of CPEB family proteins.
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Exploring the effects of 5-HT2A and AMPA receptors on brain 5-HT via a mechanism-based pharmacodynamic modelZhou, Zhu 01 January 2014 (has links) (PDF)
Depression is a common mood disorder. Although major ethical challenges make it nearly impossible to invasively and directly measure serotonin (5-hydroxytryptamine, 5-HT) levels in human brains, neuroimaging technologies have shown macroscopic structural and functional abnormalities in the prefrontal cortex (PFC) of depressed patients. The monoamine hypothesis of depression is based on the neurotransmitter imbalance, such as deceased serotonin brain levels are implicated in the cause of depression. Research has focused on the control mechanisms involved in the dorsal raphé nucleus (DRN) which is the serotonergic control center located in the midbrain. We hypothesized that activation 5-HT 2A receptor in PFC would increase serotonin levels by an AMPA-dependent mechanism in both DRN and PFC. Enhancement of the 5-HT in DRN may inhibit 5-HT level in PFC by 5-HT 1A receptor. This becomes the full feedback loop system. While 5-HT levels in the PFC have been well studied, pathway that modulate this DRN pool through upstream cascade interactions leading to a downstream feedback loop have been difficult to elucidate. Developing a mechanism-based pharmacokinetics (PK) and pharmacodynamics (PD) model to quantitatively describe the effect of 5-HT 2A receptors regulation to serotonin in the DRN and PFC would help us to better understand the complex brain. 5-HT 2A receptor agonist and AMPA receptor agonist and antagonist were used to activate or block the related receptor. Male Wistar rats underwent neurosurgery for implantation of microdialysis (MD) probes. Three to five rats were randomly assigned to experimental arms. Using the MD method, the drug combination was examined to explore the drug effect on time course of 5-HT release in DRN and PFC. Based on the experiment results, a mechanism-based PD model was developed. Phoenix WinNonlin ® and Berkeley Madonna™ were used for model estimation, external validation with secondary data set, and simulation. The result supports the possibility of a 5-HT 2A /AMPA feedback control circuit that originates in the PFC and modulates DRN and PFC 5-HT levels through feedback coupling of 5-HT. The time-course profiles of 5-HT in both DRN and PFC was well modeled and model parameters were estimated with good precision (CV% ranged from 1.37% to 35.03%). The mechanism model was developed to characterize and better understand the neurotransmitter mechanisms, providing estimations of various parameters of the disease related receptor system.
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Estrogenic Modulation of Fear GeneralizationLynch, Joseph Francis, III 06 July 2016 (has links)
No description available.
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