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  • About
  • The Global ETD Search service is a free service for researchers to find electronic theses and dissertations. This service is provided by the Networked Digital Library of Theses and Dissertations.
    Our metadata is collected from universities around the world. If you manage a university/consortium/country archive and want to be added, details can be found on the NDLTD website.
11

CHARACTERIZING CONSUMPTION, DEPENDENCE, AND THE ROLE OF GLUCOCORTICOIDS IN AN ANIMAL MODEL OF VOLUNTARY ETHANOL CONSUMPTION

Sharrett-Field, Lynda 01 January 2013 (has links)
Alcohol abuse disorders (AUD) represent a serious worldwide health problem with far reaching social, financial, and interpersonal implications. One of the most devastating facets of these disorders is the propensity to relapse following periods of abstinence. Ethanol withdrawal (EWD) is believed to promote relapse by increasing anxiety and craving, and may contribute to the development of cognitive decline associated with long-term dependence. Clinical data suggest that stress also plays a main role in both the development of AUD as well as relapse to drinking. As a physiological stressor, EtOH elevates levels of stress hormones (cortisol in humans, corticosterone (CORT) in the rat). Both CORT and EtOH have been shown to alter the composition, function, and activity of the N-methyl-D-aspartate (NMDA) receptor, and in particular, the NR2B subunit of this receptor. These alterations have been suggested to mediate EWD, which may negatively impact abstinence rates. This synergistic interaction between EtOH and CORT may present a therapeutic target for the treatment of EWD. In fact, data suggest that blocking the glucocorticoid receptor, which is a main target for CORT, with RU-486 could promote abstinence, as treatment with the drug has been shown to reduce consumption and the development dependence, as well as the severity of EWD and the cognitive deficits following EWD. However, these latter effects have not been validated in models of voluntary EtOH consumption. As there is considerable evidence that active versus passive intake can significantly impact neuroadaptations to ethanol this is an important consideration. These studies sought to characterize consumption and evaluate the development of dependence in a chronic voluntary model of intermittent access (IA) to EtOH. CORT plasma levels and protein expression of the glucocorticoid and NR2B receptors were measured during and/or following exposure. Finally, to assess the role of CORT in EtOH consumption and the development of dependence, the glucocorticoid receptor antagonist ORG-34517 was administered during access to EtOH. IA access to 20% EtOH produced varying levels of consumption (2.0-6.7g/kg/24hr exposure) and blood EtOH levels (6.3-116.9 mg/dl), but did not significantly affect food consumption or weight gain. Baseline CORT levels were found to be predictive of subsequent EtOH consumption and levels of consumption were sufficient to elevate CORT levels following one hour of EtOH exposure. Further, IA to EtOH was sufficient to produce dependence, as measured by elevations in the acoustic startle reflex following 26 hours and five days of withdrawal. No alteration in protein expression was observed regarding either the NR2B or glucocorticoid receptors and exposure to ORG-34517 had no effect on consumption or withdrawal.
12

A bio-behavioural investigation into the role of the cholinergic system in stress / Ilse Groenewald

Groenewald, Ilse January 2006 (has links)
Posttraumatic stress disorder (PTSD) is an anxiety disorder that may follow exposure to severe emotional trauma and presents with various symptoms of anxiety, hyperarousal and cognitive anomalies. Interestingly, only 10-30% of an exposed population will go on to develop full-blown PTSD. Cholinergic neurotransmission is implicated in anxiety as well as other typical manifestations of PTSD, particularly cognitive changes. The frontal cortex and hippocampus regulate and in turn are affected by stress, and have also been implicated in the underlying neuropathology of PTSD. These areas are densely innervated by cholinergic neurons originating from the basal forebrain. In this study, the time dependent sensitization (TDS) model was used to induce symptoms of PTSD in animals. The study was designed to determine the long-term effects of an intense, prolonged aversive procedure on central muscarinic acetylcholine receptor (mAChR) characteristics and the correlation if any of those findings to cognitive aspects and general arousal as characteristics associated with PTSD. In order to achieve this goal, male Sprague-Dawley rats were exposed to the TDS stress paradigm with behavioral/neuro-receptor assessments performed on day 7 post re-stress (duration of each experiment in whole is 14 days). Acoustic startle reflex (ASR) was used to determine emotional state (hyperarousal), while the conditioned taste aversion (CTA) paradigm was implemented in order to assess aversive memory. Muscarinic receptor binding studies were performed in the frontal cortex and hippocampus. Moreover, both the stress-exposed and control animals were pre-tested in the acoustic startle chamber in order to attempt to separate stress sensitive from stress-resilient animals based on predetermined ASR criteria. The ASR niodel was previously validated in our laboratory, while the CTA model was validated in this project before application. In the CTA model, an i.p. injection with lithium chloride (LiCl) (associated with digestive malaise), was used as unconditioned stimulus (US) and was paired with a saccharinlcyclamate drinking solution as conditioned stimulus (CS) to induce aversion to the novel taste (CS) when presented in the absence of the US. Population data of animals tested in the ASR experiment indicated no statistical significant difference between stressed and control animals. However, when each animal was assessed individually, 22.5 % of the exposed population displayed all increase above the predetermined criteria of 35 % in startle response, indicating a state of heightened arousal. In contrast, only 4.2 O h of control animals (no stress) displayed an increase in arousal based on the above mentioned criteria. Muscarinic receptor densities (Bm,) in the total population of animals exposed to stress showed a statistical significant increase in both the hippocampus and frontal cortex when compared to controls, with no changes in & values observed in either one of the areas. In the CTA experiment, TDS stress was implemented as US paired with a saccharinlcyclamate drinking solution as CS. An acute session of prolonged stress (as used in the TDS model) effectively induced aversion to a novel taste and a subsequent reminder of the stress (restress) paired with the CS sustained the acquire adversive memory. Furthermore, LiCl was reintroduced as US in order to assess the effect of prior exposure to two types of stress (acute and TDS) on subsequently acquired CTA memory. Prior exposure to acute stress had no significant effect on subsequently acquired aversive memory when measured either 3- or 7 days post-conditioning (CS-US). Stress-restress (TDS) exposure, however, indicated a significant decrease in aversive memory from 3- to 7 days post-conditioning (CS-US) as well as a significant decrease in aversive memory between the control- and the TDS group 7 days post-conditioning. The mAChR density (B,,) in the frontal cortex; but not in the hippocampus, was elevated at the same point in time (7 days post CS-US pairing) that CTA memory was impaired following TDS stress (stress-restress). Ultimately, these data support an association between altered cholinergic receptors and hyperarousallanxiety in an animal model of PTSD. The data also support the phenomenon of individual susceptibility to stress in animals that parallels that observed in humans exposed to severe trauma. Impaired aversive memory (CTA) is a consequence of prior exposure to TDS stress, but not acute stress, and is likewise mediated by an altered central cholinergic transmission displayed as an increase in mAChRs in the frontal cortex. The lack of studies regarding the influence of the cholinergic system in PTSD related behavior earns ,this project value as inimitable PTSD research. / Thesis (M.Sc. (Pharmacology))--North-West University, Potchefstroom Campus, 2007.
13

A bio-behavioural investigation into the role of the cholinergic system in stress / Ilse Groenewald

Groenewald, Ilse January 2006 (has links)
Thesis (M.Sc. (Pharmacology))--North-West University, Potchefstroom Campus, 2007.
14

A bio-behavioural investigation into the role of the cholinergic system in stress / Ilse Groenewald

Groenewald, Ilse January 2006 (has links)
Posttraumatic stress disorder (PTSD) is an anxiety disorder that may follow exposure to severe emotional trauma and presents with various symptoms of anxiety, hyperarousal and cognitive anomalies. Interestingly, only 10-30% of an exposed population will go on to develop full-blown PTSD. Cholinergic neurotransmission is implicated in anxiety as well as other typical manifestations of PTSD, particularly cognitive changes. The frontal cortex and hippocampus regulate and in turn are affected by stress, and have also been implicated in the underlying neuropathology of PTSD. These areas are densely innervated by cholinergic neurons originating from the basal forebrain. In this study, the time dependent sensitization (TDS) model was used to induce symptoms of PTSD in animals. The study was designed to determine the long-term effects of an intense, prolonged aversive procedure on central muscarinic acetylcholine receptor (mAChR) characteristics and the correlation if any of those findings to cognitive aspects and general arousal as characteristics associated with PTSD. In order to achieve this goal, male Sprague-Dawley rats were exposed to the TDS stress paradigm with behavioral/neuro-receptor assessments performed on day 7 post re-stress (duration of each experiment in whole is 14 days). Acoustic startle reflex (ASR) was used to determine emotional state (hyperarousal), while the conditioned taste aversion (CTA) paradigm was implemented in order to assess aversive memory. Muscarinic receptor binding studies were performed in the frontal cortex and hippocampus. Moreover, both the stress-exposed and control animals were pre-tested in the acoustic startle chamber in order to attempt to separate stress sensitive from stress-resilient animals based on predetermined ASR criteria. The ASR niodel was previously validated in our laboratory, while the CTA model was validated in this project before application. In the CTA model, an i.p. injection with lithium chloride (LiCl) (associated with digestive malaise), was used as unconditioned stimulus (US) and was paired with a saccharinlcyclamate drinking solution as conditioned stimulus (CS) to induce aversion to the novel taste (CS) when presented in the absence of the US. Population data of animals tested in the ASR experiment indicated no statistical significant difference between stressed and control animals. However, when each animal was assessed individually, 22.5 % of the exposed population displayed all increase above the predetermined criteria of 35 % in startle response, indicating a state of heightened arousal. In contrast, only 4.2 O h of control animals (no stress) displayed an increase in arousal based on the above mentioned criteria. Muscarinic receptor densities (Bm,) in the total population of animals exposed to stress showed a statistical significant increase in both the hippocampus and frontal cortex when compared to controls, with no changes in & values observed in either one of the areas. In the CTA experiment, TDS stress was implemented as US paired with a saccharinlcyclamate drinking solution as CS. An acute session of prolonged stress (as used in the TDS model) effectively induced aversion to a novel taste and a subsequent reminder of the stress (restress) paired with the CS sustained the acquire adversive memory. Furthermore, LiCl was reintroduced as US in order to assess the effect of prior exposure to two types of stress (acute and TDS) on subsequently acquired CTA memory. Prior exposure to acute stress had no significant effect on subsequently acquired aversive memory when measured either 3- or 7 days post-conditioning (CS-US). Stress-restress (TDS) exposure, however, indicated a significant decrease in aversive memory from 3- to 7 days post-conditioning (CS-US) as well as a significant decrease in aversive memory between the control- and the TDS group 7 days post-conditioning. The mAChR density (B,,) in the frontal cortex; but not in the hippocampus, was elevated at the same point in time (7 days post CS-US pairing) that CTA memory was impaired following TDS stress (stress-restress). Ultimately, these data support an association between altered cholinergic receptors and hyperarousallanxiety in an animal model of PTSD. The data also support the phenomenon of individual susceptibility to stress in animals that parallels that observed in humans exposed to severe trauma. Impaired aversive memory (CTA) is a consequence of prior exposure to TDS stress, but not acute stress, and is likewise mediated by an altered central cholinergic transmission displayed as an increase in mAChRs in the frontal cortex. The lack of studies regarding the influence of the cholinergic system in PTSD related behavior earns ,this project value as inimitable PTSD research. / Thesis (M.Sc. (Pharmacology))--North-West University, Potchefstroom Campus, 2007.
15

Modulation du réflexe acoustique de sursaut par la musique stimulante et relaxante

Richard, Marie-Andrée 08 1900 (has links)
La musique a la capacité d’induire et moduler les émotions, décomposées en deux dimensions : le niveau d’activation (relaxant-stimulant) et la valence émotionnelle (déplaisant-plaisant). Une façon de mesurer objectivement la valence musicale est par le réflexe acoustique de sursaut, une réaction de défense qui consiste en un clignement de l’oeil provoqué par un bruit fort et inattendu. Le réflexe est renforcé par la musique déplaisante et inhibée par la musique plaisante. Cependant, l’effet du niveau d’activation émotionnelle lors de l’écoute musicale demeure inconnu. Cette étude a donc pour objectif d’examiner la modulation du réflexe acoustique de sursaut par la musique stimulante et relaxante jugée plaisante. Basée sur les résultats d’études antérieures avec des images, notre hypothèse était que le réflexe serait plus faible dans la condition stimulante que dans la condition relaxante. Dans un devis intrasujet, 47 participants ont écouté de la musique relaxante et stimulante. Des bruits blancs courts et forts ont été rajoutés par-dessus les extraits afin de provoquer le réflexe de sursaut, dont son amplitude et sa latence ont été mesurées par électromyographie. Les résultats ont ensuite été comparés à ceux d’une condition non-musicale, constituée de sons environnementaux plaisants, afin d’explorer si la musique est plus efficace pour inhiber le réflexe. Finalement, des caractéristiques acoustiques, telles que la clarté de la pulsation, la densité acoustique, la dissonance et l’énergie, ont été extraites puis comparées entre les trois conditions pour explorer leur relation avec les paramètres du réflexe. Les résultats rapportent une modulation de la latence du réflexe de sursaut, dans laquelle celle-ci est plus longue dans la condition stimulante comparée à la condition relaxante. Cependant, aucune différence au niveau de l’amplitude n’a été observée. Seule la latence serait donc sensible au niveau d’activation des émotions musicales lorsque la musique est plaisante. Ensuite, la latence dans la condition non-musicale était aussi longue que celle dans la condition stimulante, suggérant que la musique n’est pas plus efficace que les sons non-musicaux pour inhiber le réflexe de sursaut. Finalement, comme l’amplitude et la latence n’ont pas le même patron de réponses, cette étude suggère que le réflexe de sursaut est aussi modulé par le traitement des caractéristiques acoustiques et que ceux-ci ont un effet différent sur ces deux paramètres. En conclusion, la latence du réflexe acoustique de sursaut est une bonne méthode pour mesurer le niveau d’activation des émotions musicales. De futures recherches pourront utiliser le paradigme de la modulation affective du réflexe de sursaut pour mesurer les effets des émotions musicales selon des facteurs individuels tels que l’âge et la dépression. / Music has the capacity to evoke and modulate emotions, divided by two dimensions: arousal (relaxing-stimulating), and valence (unpleasant-pleasant). Musical valence can be objectively measured by the acoustic startle reflex, a defensive reaction consisting of an eye blink provoked by a short and loud noise. This reflex is facilitated by unpleasant music and inhibited by pleasant music. However, the arousal effect while listening to music on the startle reflex remains unknown. This study therefore aims to explore the affective startle modulation by stimulating and relaxing music. In a within-subjects design, 47 participants listened to stimulating music, relaxing music and non-musical sounds. White noises (50 ms, 105 dB(A)) were added over the excerpts to induce startle while eyeblink magnitude and latency were measured by electromyography. Excerpts’ acoustic features were then extracted and compared through experimental conditions to explore their effect on startle modulation. Startle latency was longer in the stimulating condition compared to the relaxing one, but no differences in magnitude were found, partially confirming our predictions. Exploratory analyses suggest that startle modulation is also attributed to bottom-up processes of acoustic features, and that these latter impact differently magnitude and latency. In conclusion, this study highlights startle latency measure efficiently emotional arousal while listening to music, allowing future research to use the paradigm of affective startle reflex modulation to evaluate the effect of music on emotions considering individual factors, such as age and depression. It also paves the way for comparisons of the effect of emotions and acoustic features processes on the startle reflex modulation.
16

Differential Pathologies Resulting From Sound Exposure: Tinnitus Vs. Hearing Loss

Longenecker, Ryan James 07 October 2015 (has links)
No description available.
17

Physiological Stress Reactivity in Late Pregnancy

Hellgren, Charlotte January 2013 (has links)
During pregnancy, the basal activity is increased in both of our major stress response systems: the sympathetic nervous system and the hypothalamic-pituitary-adrenal axis. At the same time, the reactivity towards stressors is reduced. These alterations sustain maternal and fetal homeostasis, and are involved in the regulation of gestational length. Although the feto-placental hormone synthesis produces the main endocrinological changes, also the central nervous system undergoes adaptation. Together, these profound adjustments have been suggested to make women’s mental health more vulnerable during pregnancy and postpartum period. The aim of this thesis was to examine factors connected to physiological stress responses during the late pregnancy in relation to pain, labour onset, emotional reactivity, and mental health. The first study examined the pain and sympathetic response during cold stress, in relation to time to delivery. Women with fewer days to spontaneous delivery had lower sympathetic reactivity, while no pain measure was associated with time to delivery. In the second study, acoustic startle response modulation was employed to study emotional reactivity during late gestation, and at four to six weeks postpartum. The startle response was measured by eye-blink electromyography, while the participants watched pleasant and unpleasant pictures, and positive and negative anticipation stimuli. A significant reduction in startle modulation by anticipation was found during the postpartum assessment. However, no startle modulation by pleasant, or unpleasant, pictures was detected at either time-point. The serum level of allopregnanolone, a neurosteroid implied in pregnancy-induced hyporeactivity, was analysed in relation to self-reported symptoms of anxiety and depression. Although the participants reported low levels of depression, the women with the highest depression scores had significantly lower levels of serum allopregnanolone. There was no correlation between allopregnanolone and anxiety scores. In the fourth study, the cortisol awakening response was compared between women with depression during pregnancy, women with depression prior to pregnancy, and women who had never suffered from depression. No group differences in cortisol awakening response during late pregnancy were found. The results are in line with the previously described pregnancy-induced hyporesponsiveness, and add to the knowledge on maternal stress hyporeactivity, gestational length, and maternal mental health.
18

Modulation du réflexe acoustique de sursaut et de l’inhibition par le prépulse : une comparaison entre les jeunes adultes et les âgés

Le Duc, Jolyanne 08 1900 (has links)
Une des théories actuellement prépondérante pour expliquer le déclin cognitif observé chez les personnes âgées est une perte généralisée de la fonction inhibitrice. En revanche, de plus en plus d’études révèlent un maintien et même un gain sur le plan émotionnel chez les âgés. Afin de caractériser l’effet de l’âge sur la fonction inhibitrice et sur les émotions, nous avons utilisé le paradigme bien connu du réflexe acoustique de sursaut et de son inhibition par le prépulse, un phénomène reconnu comme reflétant le filtrage sensorimoteur, soit une mesure pré-attentionnelle d’inhibition. Le réflexe acoustique de sursaut est une réponse du corps tout entier à un bruit fort et inattendu et a été mesuré via la magnitude et la latence du clignement des yeux. La présentation d’un son faible (prépulse) quelques millisecondes avant le bruit de sursaut réduit la réponse de sursaut. Deux groupes de participants (jeunes adultes et âgés) ont visionné des images plaisantes, neutres et déplaisantes issues du International Affective Picture System (IAPS), lesquelles étaient associées à des stimuli auditifs évaluant le réflexe acoustique de sursaut et son inhibition par le prépulse. Les résultats démontrent que le réflexe de sursaut est modulé différemment par les émotions chez les jeunes adultes et les âgés. Plus particulièrement, les adultes âgés ont un plus grand réflexe de sursaut que les jeunes adultes lorsqu’ils visionnent des images plaisantes et neutres. Le processus d’inhibition par le prépulse est également modulé différemment par les émotions chez les âgés et les jeunes adultes: les âgés ont une plus grande inhibition du réflexe de sursaut que les jeunes adultes lorsqu’ils visionnent des images plaisantes et déplaisantes, mais ils ne diffèrent pas des jeunes adultes pour les images neutres. Dans l’ensemble, les résultats obtenus ne sont pas compatibles avec une perte d’inhibition chez les adultes âgés, et supportent plutôt un biais émotionnel positif. / Aging is often characterized by a decline in cognitive abilities and a loss of inhibitory function. At the same time there is promising, yet limited to date, evidence of a better emotion regulation with aging. In order to characterize the effect of age on inhibitory function and emotions, in this study the well-known acoustic startle paradigm and its inhibition by a prepulse, a phenomenon known to engage sensorimotor gating, were used. The acoustic startle reflex, a whole-body reflex in response to a loud and unexpected sound, was measured through eye blink magnitude and latency. The inhibition of this acoustic startle response by the presentation of a weak sound, a prepulse, was also measured. Two groups of 30 adults (young and older adults) viewed pleasant, neutral, and unpleasant images from the International Affective Picture System (IAPS) while startle and prepulse trials were presented. The results show that the startle response is differently modulated in the two groups, with the elderly displaying a greater startle reflex while viewing pleasant and neutral pictures compared to young adults. Prepulse inhibition is also differently modulated by emotions in young adults and their older counterparts, with the latter exhibiting a greater inhibition of the startle reflex when viewing pleasant and unpleasant pictures (but not for neutral pictures) compared to young adults. In summary, the present data do not support a decline of the inhibitory function with increasing age, but rather support a positivism effect.
19

Modulation du réflexe acoustique de sursaut et de l’inhibition par le prépulse : une comparaison entre les jeunes adultes et les âgés

Le Duc, Jolyanne 08 1900 (has links)
No description available.

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