Strukturelle Korrelate des Gesangslernens bei Vögeln

Nixdorf-Bergweiler, Barbara Emilie

28 June 2006

Das Gesangssystem der Vögel hat sich als ein hervorragendes Modellsystem erwiesen, um Fragen zu Mechanismen entwicklungsbedingter neuronaler Plastizität von Lernprozessen zu erarbeiten. Bei Singvögeln haben sich im Laufe der Phylogenese neuronale Zentren entwickelt, die sich auf das Gesangslernen und die Gesangsproduktion spezialisiert haben. Zebrafinkenmännchen, wie viele andere Singvögel auch, erlernen ihren Gesang, indem sie von einem Tutor ihr artspezifisches Gesangsmuster schon in früher Jugend im Gedächtnis abspeichern und dann ganz allmählich ihr eigenes Vokalisationsmuster über auditorische Rückkopplung an das im Gehirn abgespeicherte Muster angleichen. Parallel zu diesen Verhaltensänderungen, finden auch auf neuronaler Ebene zahlreiche Veränderungen in den Gesangskernen statt, die in der hier vorliegenden Arbeit detailliert untersucht wurden, indem Zebrafinken zum einen mit einem Gesangstutor aufwuchsen oder ohne ein Gesangsvorbild. Die Folgen dieser unterschiedlichen Aufzuchtsbedingungen wurden dann im Gesang und in den neuronalen Strukturen der Gesangskerne mit einer Vielzahl von Techniken analysiert, einschließlich der Golgi-Technik, Elektronenmikroskopie, Immunhistochemie, verschiedener neuronaler Tracersubstanzen und quantitativer Stereologie, sowie intrazellulärer Ableitungen am in vitro Hirnschnittpräparat. Die Daten zeigen u.a., dass dendritische Spines an der Gedächtnisbildung für Gesang maßgeblich beteiligt sind und zwar in einer Vorderhirnregion, der eine wichtige Rolle bei frühen sensorischen Lernprozessen zukommt, dem lateralen magnocellularen Nucleus des anterioren Nidopalliums (LMAN). Zebrafinkenweibchen singen nicht und haben weitaus kleinere Gesangskerne als die Männchen. Zebrafinkenweibchen, die nie einen artspezifischen Gesang hören, weisen im Vergleich zu denen, die mit einem solchen aufgewachsen sind, signifikante Unterschiede in der neuronalen Struktur im Nucleus robustus arcopallii (RA) auf. Diese Befunde zeigen, dass die Gesangskerne bei Weibchen trotz ihrer kleineren Größe dennoch eine wichtige Rolle bei der Gedächtnisbildung eines artspezifischen Gesangsmusters spielen. Man beachte, dass die Nomenklatur des Vogelgehirns 2004 revidiert wurde (Reiner et al, J Comp Neurol 473:377-414, 2004; http://avianbrain.org/papers/RevisedNomenclature.pdf). / The song system of birds has been used extensively as a model system for studying basic mechanisms of neuronal plasticity and development underlying a learned behavior. Discrete sets of interconnected nuclei in the avian brain have evolved and are a prerequisite for song learning processes and the production of song. Zebra finch males, like many other song birds, learn their song by memorizing a tutor song model early in life and then gradually matching their vocal output by auditory feedback to the stored memory of that tutor song. In parallel to these behavioural changes, various changes in neuronal structures of song system nuclei take place. These structural correlates of song learning processes have been investigated in great detail in the current research by raising zebra finches with and without a song tutor model and then studying the consequences for song and for neuronal structure in the song system by using a variety of techniques including Golgi-technique, electron microscopy, immunohistochemistry, various neuronal tracer and quantitative stereology, intracellular recordings in the in vitro slice preparation and analyzing sonograms at the behavioral approach. There is strong evidence that, among other findings, dendritic spines are very much involved in memory formation of song in the lateral magnocellular nucleus of the anterior nidopallium (LMAN), a forebrain region particularly involved in sensory learning processes early in life. Female zebra finches do not sing and have much smaller song nuclei than males. Rearing females either with being exposed to species-specific song early in life or deprived of hearing song, exhibit significant differences in neuronal structure particularly in nucleus robustus arcopallii (RA). These data give further evidence that, despite their smaller sizes, song system nuclei in female birds do play an important role in memorization of song. Please note that in 2004 the nomenclature of the avian brain has been revised (Reiner et al, J Comp Neurol 473:377-414, 2004; http://avianbrain.org/papers/RevisedNomenclature.pdf).

Entwicklung

Lernen und Gedächtnis

Gesangssystem

Gehirnstrukturen

dendritische Spines

Synapsen

quantitative Morphometrie

development

learning and memory

song system

brain structure

dendritic spines

synapses

quantitative morphometry

590 Tiere (Zoologie)

32 Biologie

WT 4530

ddc:590

Rôle de Scribble1 dans la formation des synapses glutamatergiques et le trafic des récepteurs NMDA / Role of Scribble1 in glutamatergic synapse formation and trafficking of NMDA receptors

Piguel, Nicolas

20 December 2010

Les neurones établissent entre eux de nombreux contacts synaptiques, et l'on estime qu’en moyenne un neurone peut avoir dix mille contacts avec les neurones de son voisinage. L'une des synapses les plus importantes et les plus étudiées, dont les dysfonctionnements conduisent à des pathologies du cerveau, est la synapse excitatrice glutamatergique. Dans l’hippocampe, les synapses excitatrices présentent une structure postsynaptique particulière, sous la forme d’un renflement de la dendrite appelé épine dendritique. Cette épine possède un domaine particulier, la densité postsynaptique, concentrant de nombreux récepteurs aux glutamates, des protéines d’adhésion ainsi que des protéines d’échafaudage faisant le lien avec les cascades moléculaires intracellulaires et le cytosquelette d’actine. La morphologie de l’épine dendritique ainsi que le nombre de récepteurs présents dans la PSD sont des éléments clés dans la transmission synaptique et les phénomènes de potentiation et de dépression à long terme (LTP & LTD). Lors de ma thèse, j’ai identifié Scribble1 comme une nouvelle protéine régulant le trafic des récepteurs NMDA. Scribble1 est surtout connue pour son implication dans des processus de polarité, division et migration cellulaire. En modulant le taux de Scribble1, j’ai montré que je pouvais affecter le nombre et la morphologie des épines des neurones hippocampaux, ainsi que la polymérisation de l’actine. Ensuite, j’ai démontré que Scribble1 interagissait directement avec les récepteurs NMDA et permettait leur recyclage à la membrane. Enfin, chez le neurone immature, Scribble1 est impliqué dans la migration du cône axonal. Chez un animal mutant, qui n’exprime que 50% de la protéine (circletail) les performances mnésiques et sociales de l’animal sont perturbées, validant le rôle de la protéine au niveau du système nerveux. / One of the most studied and more important synapse is the glutamatergic excitatory synapse, which dysfunctions lead to brain pathologies. In the hippocampus, the most represented synapses are glutamatergic synapses using glutamate as neurotransmitter. Postsynaptic structures, such as dendritic spines, concentrate many glutamate receptors, adhesion proteins and scaffold proteins bridging receptors to molecular cascades and intracellular actin cytoskeleton. The morphology of the dendritic spine and the number of glutamate receptors at the surface of the spine are key-elements in synaptic transmission, such as of long-term potentiation (LTP). In this study, I identify Scribble1 as an important regulator of NMDA receptors trafficking. Scribble1 is well known for its roles in cell polarity, division and migration processes. First, I show that Scribble1 gain- and loss-of-function affect the number and morphology of spines, as well as the actin polymerization. Next, I showed that Scribble1 interacts directly with the NMDA receptor and stimulates its recycling to the membrane. Finally, in immature neuron, Scribble1 is involved in axon growth cone migration. In a Scribble1 mutant animal model, circletail, we observed disruption of synaptic transmission and memory and social performance defects, compatible with a role of the protein in central nervous system function.

Scribble1

Récepteurs NMDA

Recyclage

Neurones hippocampales

Épines dendritiques

Cônes de croissance

Scribble1

NMDA receptors

Recycling

Hipocampal neurons

Dendritic spines

Growth cones

EFFECTS OF ALTERNATIVE PREY AS A BUFFER TO PREDATION OF CHANNEL CATFISH (ICTALURUS PUNCTATUS) BY LARGEMOUTH BASS (MICROPTERUS SALMOIDES)

Nellis, Shelley

23 July 2010

Channel catfish have pectoral spines that lock to defend against gape-limited predators such as largemouth bass. Previous work indicated that spines increase survival of channel catfish exposed to bass but did not determine whether bass avoid catfish if less dangerous species are available. We presented bass with channel catfish and two alternatives, bluegill and goldfish, and compared order of ingestion, ingestion time, percent of successful strikes, and time spent chasing each prey species. We also presented the three species in a jar study that standardized position in the water column as well as in a net-pen study. The order of ingestion was suggestive of a preference for goldfish, then bluegill and finally channel catfish. Handling time was greater for channel catfish, less for bluegill, and the least for goldfish. Fewer catfish were eaten when other prey were available. Bass appear to avoid channel catfish if alternative prey is available.

channel catfish

largemouth bass

predation

pectoral spines

anti-predator adaptation

anti-predator morphology

survivability

Biology

Life Sciences

Regulation of AKAP79/150 targeting to dendritic spines /

Horne, Eric Andrew.

January 2007

Thesis (Ph.D. in Pharmacology) -- University of Colorado Denver, 2007. / Typescript. Includes bibliographical references (leaves 132-151). Free to UCD affiliates. Online version available via ProQuest Digital Dissertations;

Investigating glial dynamics in the developing hippocampus

Haber, Michael.

January 2008

Glial cells represent the most abundant cell population in the central nervous system (CNS), and yet, have historically been thought of as merely support cells for neurons. Over the past few decades, however, the number of identified roles that glial cells play in the CNS has expanded at an exponential rate, revealing new and exciting functions in neuron-glial communication. At synapses, astrocytes are now recognized as part of a "tripartite" complex with pre- and postsynaptic structures and can modulate synaptic transmission and plasticity. Accumulating evidence has also revealed new roles for oligodendrocytes in regulating axon diameter and integrity, and ion channel clustering. Despite our knowledge of the physiological connections between neurons and glia, relatively little is known about the morphological interplay of these cells during development and in the mature brain. The results presented in this thesis reveal the extent and time-course of rapid remodelling of astrocytes and oligodendrocytes in close proximity to dendritic spines and axons respectively. These findings provide further evidence that glia play an important role in regulating the structural plasticity of the brain. The methodology developed also provides a powerful system for the study of neuron-glial structural dynamics and may contribute to the development of novel therapeutic strategies for diseases affecting the central nervous system.

Hippocampus -- growth & development.

Hippocampus -- physiology.

Astrocytes -- physiology.

Oligodendroglia -- physiology.

Dendritic Spines -- physiology.

Axons -- physiology.

Cell Communication -- physiology.

The developmental functions of BDNF and MECP2 on dendritic and synaptic structure

Chapleau, Christopher Allen.

January 2008

Thesis (Ph. D.)--University of Alabama at Birmingham, 2008. / Title from first page of PDF file (viewed Sept. 16, 2008). Includes bibliographical references.

Rôle de CHMP2B et du complexe ESCRT-III dans le remodelage dans membranes cellulaires : cas des épines dendritiques / Role of CHMP2B and ESCRT-III in in the remodeling of cellular membranes : example of dendritic spines

Chassefeyre, Romain

16 December 2013

CHMP2B est une sous-unité du complexe ESCRT-III, un complexe cytosolique très conservé, responsable du remodelage des membranes biologique, dans divers processus cellulaires. Des mutations de CHMP2B sont associées à une forme familiale de démence frontotemporale. Une étude précédente a mis en évidence que les mutants pathogènes de CHMP2B altèrent la morphologie des épines dendritiques, un phénomène potentiellement à l'origine de la maladie. Ce travail de recherche a pour objectif de décrire le rôle de CHMP2B, et du complexe ESCRT-III, dans la structure et le fonctionnement des épines dendritiques. Dans des lignées cellulaires, nous avons démontré que CHMP2B a la propriété de s'associer préférentiellement à la membrane plasmique, de se polymériser en filaments hélicoïdaux et de former de longs et fins tubes membranaires. Ce résultat indique que CHMP2B est directement impliqué dans le remodelage de la membrane plasmique. Dans les neurones, CHMP2B se concentre dans des régions sous-membranaires proches de la PSD. Une analyse biochimique a montré que CHMP2B et CHMP4B sont associées à d'autres sous-unités, pour former un complexe ESCRT-III postsynaptique particulièrement stable. Nous avons identifié par spectrométrie de masse que ce complexe interagit également avec des protéines d'échafaudage postsynaptiques et des protéines de remodelage du cytosquelette d'actine. La déplétion de CHMP2B par RNAi, dans des neurones en culture, affecte la complexité de l'arborisation dendritique, la morphologie des épines dendritiques et empêche le gonflement des épines associé à la LTP. Des expériences de récupération, avec des mutants pontuels, indiquent que le rôle de CHMP2B dans le maintien de l'arborisation dendritique est dépendant à la fois de de son association avec ESCRT-III et la bicouche phospholipidique. Nous proposons une nouvelle fonctionnalité pour un complexe ESCRT-III contenant CHMP2B, dans les processus de remodelage de la membrane postsynaptique associés à la maturation et à la plasticité des épines dendritiques. / CHMP2B is a subunit of ESCRT-III, a highly conserved cytosolic protein machinery, responsible for membrane remodeling in diverse cellular mechanisms. Mutations in CHMP2B are responsible for a familial form of frontotemporal dementia. A previous study highlighted that FTD-related mutants of CHMP2B impair the morphological maturation of dendritic spines, a process that may underlie neurodegeneration in this disease. The goal of this research work id directed towards understanding the role of CHMP2B and ESCRT-III in dendritic spines structure and function. In cell lines, we demonstrated that CHMP2B associates preferentially with the plasma membrane, polymerizes in helical filaments and forms long and thin membrane protrusions. This result indicates that CHMP2B is directly involved in plasma membrane remodeling. In neurons, CHMP2B concentrates in specific sub-membrane microdomains close to the PSD. Biochemical analysis revealed that CHMP2B and CHMP4B associate with other subunits to form a remarkably stable postsynaptic ESCRT-III complex. Mass-spectrometry indicated that this complex also interacts with postsynaptic scaffolds and proteins involved in actin cytoskeleton remodelling. RNAi depletion of CHMP2B, in cultured neurons, alters stability of dendrite branching and morphology of dendritic spines, and impairs spine head growth, normally associated with LTP. Rescue experiments, with point mutants, indicated that CHMP2B activity in dendrite branching is dependent on its capacity to both bind phospholipids and oligomerization with ESCRT-III. We propose a novel functionality for an ESCRT-III complex containing CHMP2B, in maturation-dependent and plasticity-dependent processes of dendritic spine morphogenesis.

ESCRT

Epines dendritiques

Déformation membranaire

Démence frontotemporale

Arborisation dendritique

ESCRT

Dendritic spines

Membrane deformation

Frontotemporal dementia

Dendritic arborization

610

A Novel Methodology to Probe the Structural and Functional Correlates of Synaptic Plasticity

Laura Andrea Roa Gonzalez (12873056)

15 June 2022

<p>Dendritic spines are mushroom-shaped appendages on the dendritic branches of neurons. They are invaluable to the function of the brain as they form the major site for excitatory signal transmission in the mammalian brain. These ubiquitous structures have several invaluable and unique characteristics – namely that their morphological and functional characteristics are activity-dependent and undergo remodeling as the spine experiences stimulation. This activity-dependent regulation then in turn modulates the excitatory postsynaptic potential that propagates into the adjacent parent dendrite, and which ultimately reaches the somatic compartment. The mediation of this modulatory effect on the postsynaptic signal by dendritic spines renders them invaluable to the brain’s ability to change neuronal circuits as it learns. The relationship between the structural and functional change in dendritic spines as plasticity is induced remains poorly understood; while efforts have been made to examine the morphology of dendritic spines during plasticity as well as the change to receptor insertion on the postsynaptic density, a comprehensive methodology to interrogate the concomitant changes to several aspects of dendritic spine structure and function as plasticity occurs has not been established. In this study, such a methodology was developed in order to facilitate future study of how a dendritic spine’s diffusional neck resistance, head volume, calcium-sensitive channels (on the postsynaptic density), and excitatory postsynaptic potential amplitude change concurrently as the spine undergoes activity-dependent regulation. This activity-dependent regulation also occurs in groups of spines called “clusters” <em>in vivo</em>, and the structural and functional dynamics of spines as these groups are formed also remains unknown. In order to to facilitate future <em>in vivo</em> studies on how clustered dendritic spines may change dynamically in both structure and function, a methodology for surgically accessing and recording calcium-based activity from the primary auditory cortex was developed, as the frequency-specific tuning of dendritic spines in this cortical area forms a compelling environment in which to study the relationship between spine form and function. </p>

Central nervous system

dendritic spines

FRAP

calcium imaging

electrical compartmentalization

biochemical compartmentalization

calcium channel variance

EPSP

primary auditory cortex

Effect of amyloid precursor protein and tau on dendritic spines and cell survival in an ex vivo model of Alzheimer s disease

Tackenberg, Christian

11 December 2009

Alzheimer s disease is characterized by synaptic alterations and neurodegeneration. Histopathological hallmarks represent amyloidplaques composed of amyloid-beta (Abeta) and neurofibrillary tangles containing hyperphosphorylated tau. To determine whether synaptic changes and neurodegeneration share common pathways we established an ex vivo model using organotypic hippocampal slicecultures from amyloid precursor protein transgenic mice combined with virus-mediated expression of EGFP-tagged tau constructs. Confocal high-resolution imaging, algorithm-based evaluation of spines and live imaging was employed to determine spine changes and neurodegeneration. We report that Abeta but not tau induces spine loss and shifts spine shape from mushroom to stubby through a mechanism involving NMDA receptor (NMDAR), calcineurin and GSK-3beta activation. In contrast, Abeta alone does not cause neurodegeneration but induces toxicity by phosphorylation of wt tau in a NMDAR-dependent pathway. We show thatGSK-3beta levels are elevated in APP transgenic cultures and that inhibiting GSK-3beta activity or use of phosphorylation-blocking tau mutations prevent Abeta-induced toxicity of tau. FTDP-17 tau mutants are differentially affected by Abeta. While R406W tau shows increased toxicity in the presence of Abeta, no change is observed with P301L tau. While blocking NMDAR activity abolishes toxicity of both wt and R406W tau, the inhibition of GSK-3beta only protects against toxicity of wt tau but not of R406W tau induced by Abeta. Tau aggregation does not correlate with toxicity. We propose that Abeta-induced spine pathology and tau-dependent neurodegeneration are mediated by divergent pathways downstream of NMDA receptor activation and suggest that Abeta affects wt and R406W tau toxicity by different pathways downstream of NMDAR activity.

Alzheimer´s disease

FTDP-17

amyloid-beta

tau

dendritic spines

neurodegeneration

NMDA receptor

GSK-3beta

32 - Biologie

ddc:610

Investigating glial dynamics in the developing hippocampus

Haber, Michael

January 2008

No description available.

Oligodendroglia -- physiology.

Hippocampus -- growth & development.

Astrocytes -- physiology.

Hippocampus -- physiology.

Axons -- physiology.

Dendritic Spines -- physiology.

Cell Communication -- physiology.