Effects of sphingomyelin hydrolysis on quantal release from rat adrenal chromaffin cells

Yin, Jihuan

Unknown Date

No description available.

sphingomyelin

quantal release

chromaffin cell

Effects of sphingomyelin hydrolysis on quantal release from rat adrenal chromaffin cells

Yin, Jihuan

11 1900

Sphingomyelin (SM), a sphingolipid that is concentrated in the extracellular leaflet of the plasma membrane, can interact with cholesterol to form more ordered raft domains. The hydrolysis of SM by sphingomyelinase (SMase) generates ceramide and may redistribute cholesterol molecules to other less ordered domains. I employed carbon fibre amperometry to examine whether SM hydrolysis affected the kinetics of release of catecholamines from individual granules of rat chromaffin cells when exocytosis was triggered by elevated extracellular [K+]. Similar to cholesterol overload, SMase treatment selectively increased the proportion of stand-alone foot signals and the duration of the pre-spike foot signals; both effects could be reduced by extraction of cellular cholesterol. In contrast, the application of an exogenous ceramide did not mimic the effects of SMase. My results suggest that SMase treatment liberated cholesterol from lipid rafts to increase the persistence of the semi-stable fusion pore before the onset of rapid dilation.

sphingomyelin

quantal release

chromaffin cell

PHYSIOLOGICAL AND ANATOMICAL ASSESSMENT OF SYNAPSES AT THE CRAYFISH NEUROMUSCULAR JUNCTION

Johnstone, Andrew Fredericks Moser

01 January 2006

The crayfish, Procambarus clarkii, has a multitude of ideal sites in which synaptic transmission may be studied. Its opener muscle, being innervated by a single excitatory neuron is a good model for studying the structure/function of neuromuscular junctions since the preparation is identifiable from animal to animal and the nerve terminals are visible using a vital dye. This allows ease in finding a suitable site to record from in each preparation and offers the ability to relocate it anatomically. Marking a recorded site and rebuilding it through electron microscopy gives good detail of synaptic struture for assesment.In the first of these studies, low output sites known as stems (which lie between varicosities) were used to reduce n (number of release sites) in order to minimize synaptic complexity so individual quantal events could be analyzed by their unique parameters (area, peak, tau, rise time and latency). This was in attempt to uncover specific quantal signatures that could be traced back to the structure of the area recorded. It was found that even at stem regions synaptic structure is still complex having multiple synapses each of which could harbor a number of AZs. This gives insight as to how quantal analysis should be treated. Even low output synapses n must be treated at the AZ level.Synaptic depression was studied at the crayfish extensor muscle. By depressing the phasic neuron and recording from the muscle it appears thatdepression is a presynaptic phenomenon. The use of 5-HT gave insight to vesicular dynamics within the nerve terminal, by delaying depression and increasing maximum EPSP amplitude. TEM of phasic nerve terminals reveals no change in numbers of dock or RRP vesicles. Short term facilitation and vesicular dynamics were studied with the use of 5-HT and a neurotoxin TBOA, which blocks the glutamate transporter. In this study I showed differential mechanisms that control RRP and RP vesicles. By blocking glutamate reuptake, the RRP is depleted as shown by reduced EPSPs, but recovered with 5-HT application. The understanding of vesicle dynamics in any system has relevance for all chemical synapses.

The return on social bonds: the effect of social contracts on international conflict and economics

Nieman, Mark David

01 January 2013

Hierarchical or asymmetrical power relationships among states have long been a focus of scholarly attention (e.g., asymmetrical alliances, trade dependencies). While the "power to hurt" is one expression of power, an alternative approach is to gain and exercise authority, or "rightful rule." One of the major impediments to the study of social concepts such as authority or legitimacy, however, is in their informal or intangible nature. This dissertation uses game theoretic and latent variable approaches to capture informal, social authority relationships, or social hierarchies, among international states and explores the effects of these hierarchies on security and economic behavior. I posit that states adopt one of two social roles--that of a dominant or a subordinate. Each subordinate chooses a degree of autonomy that it is willing to cede to the dominant in exchange for a corresponding degree of protection. Ranging from complete autonomy to complete control, these dyadic bargains make up a social international hierarchy. This hierarchy affects the relationships between each subordinate and the dominant, as well as the relationships among subordinates. In the security realm, the probability of conflict initiation is inversely related to the degree of subordination. When conflict does occur, dominants are more likely to intervene when the target is located at a higher position in the dominant's social hierarchy than the aggressor state. Economically, the probability that a state enacts illiberal policies is inversely related to its degree of subordination. Moreover, more subordinated states face a lower risk of economic sanction than states located lower in the hierarchy, even for similar illiberal actions. Empirical analysis of states within the US hierarchy (1950-2000) and UK hierarchy (1870-1913) using strategic probit models supports these theoretical predictions.

Censored Strategic Probit

Economic Sanctions

International Conflict

Quantal Response Equalibria

Social Hierarchy

Strategic Interaction

Political Science

Three essays on biases in decision making

Ferecatu, Alina

01 July 2014

Cette thèse est organisée en trois chapitres. Chaque article analyse les déviations systématiques des décideurs par rapport aux prédictions économiques classiques dans certaines expériences bien connues. Les agents s’écartent de la voie optimale et explorent ou exploitent de manière excessive dans le problème du bandit manchot, ils exigent des taux d’intérêt bien plus élevés par rapport aux taux du marché financier afin de reporter leurs dépenses lorsqu’ils prennent des décisions de choix intertemporel, et ils ne se contentent pas de recevoir des petites sommes d’argent, même si, objectivement, ils devraient accepter cette offre, dans des expériences de négociation comme le jeu de l’ultimatum. Ces soi-disant «irrégularités» sont documentées dans les trois essais de thèse. Le essaies représentent une première étape afin de formuler des stratégies adaptées au profile psychologique de chaque individu, nécessaires pour surmonter les biais de décision. / This dissertation is organized in three chapters. Each chapter analyzes decision makers’ systematic deviations from economic predictions in well-known experiments. People deviate from the optimal path and excessively explore or exploit in n-armed bandit games, demand interest rates well above financial market averages in order to defer consumption in intertemporal choice settings, and do not settle for receiving small amounts of money, even though they would be better off objectively, in bargaining games such as the ultimatum game. Such “irregularities” are documented in the three dissertation essays. The essays are intended as a first step to formulate individual specific, customized decision aids, useful to overcome such decision biases.

Inférence bayésienne

Théorie comportementale de la décision

Aversion au risque

Behavioral Decision Making

Hierarchical Bayes

Quantal Response Equilibrium

Inositol Trisphosphate and Cyclic Adenosine Diphosphate-Ribose Increase Quantal Transmitter Release at Frog Motor Nerve Terminals: Possible Involvement of Smooth Endoplasmic Reticulum

Brailoiu, E., Miyamoto, M. D.

01 December 1999

The release of chemical transmitter from nerve terminals is critically dependent on a transient increase in intracellular Ca2+.6,25 The increase in Ca2+ may be due to influx of Ca2+ from the extracellular fluid15 or release of Ca2+ from intracellular stores such as mitochondria.1,8,18 Whether Ca2+ utilized in transmitter release is liberated from organelles other than mitochondria is uncertain. Smooth endoplasmic reticulum is known to release Ca2+, e.g., on activation by inositol trisphosphate or cyclic adenosine diphosphate-ribose,2 so the possibility exists that Ca2+ from this source may be involved in the events leading to exocytosis. We examined this hypothesis by testing whether inositol trisphosphate and cyclic adenosine diphosphate-ribose modified transmitter release. We used liposomes to deliver these agents into the cytoplasmic compartment and binomial analysis to determine their effects on the quantal components of transmitter release. Administration of inositol trisphosphate (10-4M) caused a rapid, 25% increase in the number of quanta released. This was due to an increase in the number of functional release sites, as the other quantal parameters were unaffected. The effect was reversed with 40min of wash. Virtually identical results were obtained with cyclic adenosine diphosphate-ribose (10-4M). Inositol trisphosphate caused a 10% increase in quantal size, whereas cyclic adenosine diphosphate-ribose had no effect. The results suggest that quantal transmitter release can be increased by Ca2+ released from smooth endoplasmic reticulum upon stimulation by inositol trisphosphate or cyclic adenosine diphosphate-ribose. This may involve priming of synaptic vesicles at the release sites or mobilization of vesicles to the active zone. Inositol trisphosphate may have an additional action to increase the content of transmitter within the vesicles. These findings raise the possibility of a role of endogenous inositol phosphate and smooth endoplasmic reticulum in the regulation of cytoplasmic Ca2+ and transmitter release.

cyclic adenosine diphosphate-ribose

frog neuromuscular junction

inositol trisphosphate

neurosecretion

quantal transmitter release

smooth endoplasmic reticulum

Inositol Derivatives Modulate Spontaneous Transmitter Release at the Frog Neuromuscular Junction

Brailoiu, Eugen, Miyamoto, Michael D., Dun, Nae J.

01 January 2003

One of the consequences of G-protein-coupled receptor activation is stimulation of phosphoinositol metabolism, leading to the generation of IP 3 and its metabolites 1,3,4,5-tetrakisphosphate (IP4) and inositol 1,2,3,4,5,6-hexakisphosphate (IP6). Previous reports indicate that high inositol polyphosphates (IP4 and IP6) are involved in clathrin-coated vesicular recycling. In this study, we examined the effects of IP4 and IP6 on spontaneous transmitter release in the form of miniature endplate potentials (MEPP) and on enhanced vesicular recycling by high K+ at frog motor nerve endings. In resting conditions, IP4 and IP6 delivered intracellularly via liposomes, caused concentration-dependent increases in MEPP frequency and amplitude. Pretreatment with the protein kinase A (PKA) inhibitor H-89 or KT 5720 reduced the IP4-mediated MEPP frequency increase by 60% and abolished the IP6-mediated MEPP frequency increases as well as the enhancement in MEPP amplitude. Pretreatment with antibodies against phosphatidylinositol 3-kinase (PI 3-K), enzyme also associated with clathrin-coated vesicular recycling, did not alter the IP4 and IP6-mediated MEPP frequency increases, but reduced the MEPP amplitude increase by 50%. In our previous reports, IP3, but not other second messengers releasing Ca2+ from internal Ca2+ stores, is able to enhance the MEPP amplitude. In order to dissociate the effect of Ca2+ release vs. metabolism to IP4 and IP 6, we evaluated the effects of 3-deoxy-3-fluoro-inositol 1,4,5-trisphosphate (3F-IP3), which is not converted to IP 4 or IP6. 3F-IP3 produced an increase then decrease in MEPP frequency and a decrease in MEPP amplitude. In elevated vesicle recycling induced by high K+-Ringer solution, IP4 and IP6 have similar effects, except decreasing MEPP frequency at a higher concentration (10-4 M). We conclude that (1) high inositol polyphosphates may represent a link between IP3 and cAMP pathways; (2) the IP3-induced increase of MEPP amplitude is likely to be due to its high inositol metabolites; (3) PI 3-K is not involved in the IP 4 and IP6-mediated MEPP frequency increases, but may be involved in MEPP size.

inositol phosphates

liposomal delivery

phosphatidylinositol 3-kinase

quantal transmitter release

synaptic vesicle

Calmodulin Increases Transmitter Release by Mobilizing Quanta at the Frog Motor Nerve Terminal

Brailoiu, Eugen, Miyamoto, Michael D., Dun, Nae J.

01 January 2002

1. The role of calmodulin (CaM) in transmitter release was investigated using liposomes to deliver CaM and monoclonal antibodies against CaM (antiCaM) directly into the frog motor nerve terminal. 2. Miniature endplate potentials (MEPPs) were recorded in a high K+ solution, and effects on transmitter release were monitored using estimates of the quantal release parameters m (number of quanta released), n (number of functional transmitter release sites), p (mean probability of release), and vars p (spatial variance in p). 3. Administration of CaM, but not heat-inactivated CaM, encapsulated in liposomes (1000 units ml-1) produced an increase in m (25%) that was due to an increase in n. MEPP amplitude was not altered by CaM. 4. Administration of antiCaM, but not heat-inactivated antiCaM, in liposomes (50 μl ml-1) produced a progressive decrease in m (40%) that was associated with decreases in n and p. MEPP amplitude was decreased (15%) after a 25 min lag time, suggesting a separation in time between the decreases in quantal release and quantal size. 5. Bath application of the membrane-permeable CaM antagonist W7 (28 μM) produced a gradual decrease in m (25%) that was associated with a decrease in n. W7 also produced a decrease in MEPP amplitude that paralleled the decrease in m. The decreases in MEPP size and m produced by W7 were both reversed by addition of CaM. 6. Our results suggest that CaM increases transmitter release by mobilizing synaptic vesicles at the frog motor nerve terminal.

calmodulin

electrophysiology

neuromuscular junction

neurotransmitter secretion

quantal transmitter release

synaptic vesicles

Abl family kinases regulate neuronal nicotinic receptors and synapses in chick ciliary ganglion neurons

Jayakar, Selwyn S.

14 July 2009

No description available.

Neurology

Nicotinic Receptors

ABL Kinase

Ciliary Ganglion

Quantal Analysis

Confocal

Patch Clamp

Nitric oxide enhances transmitter release at the mammalian neuromuscular junction via a cGMP-mediated mechanism

Nickels, Travis John

24 April 2006

No description available.

nitric oxide

neuromuscular junction

quantal release

neurotransmission

adenosine

n-type calcium channels