Analyse des mécanismes cellulaires et moléculaires du guidage axonal sérotoninergique in vitro

Sharif Askari, Bahram

January 2006

Mémoire numérisé par la Direction des bibliothèques de l'Université de Montréal.

Rat

Neurobiologie

Développement

Guidage axonal

Raphé dorsal

Sérotonine

Culture cellulaire neurale

Protéines à ancre GPI

Éphrines

Récepteurs Eph

Transcriptional and epigenetic control of gene expression in embryo development

Boija, Ann

January 2016

During cell specification, temporal and spatially restricted gene expression programs are set up, forming different cell types and ultimately a multicellular organism. In this thesis, we have studied the molecular mechanisms by which sequence specific transcription factors and coactivators regulate RNA polymerase II (Pol II) transcription to establish specific gene expression programs and what epigenetic patterns that follows. We found that the transcription factor Dorsal is responsible for establishing discrete epigenetic patterns in the presumptive mesoderm, neuroectoderm and dorsal ectoderm, during early Drosophila embryo development. In addition, these different chromatin states can be linked to distinct modes of Pol II regulation. Our results provide novel insights into how gene regulatory networks form an epigenetic landscape and how their coordinated actions specify cell identity. CBP/p300 is a widely used co-activator and histone acetyltransferase (HAT) involved in transcriptional activation. We discovered that CBP occupies the genome preferentially together with Dorsal, and has a specific role during development in coordinating the dorsal-ventral axis of the Drosophila embryo. While CBP generally correlates with gene activation we also found CBP in H3K27me3 repressed chromatin. Previous studies have shown that CBP has an important role at transcriptional enhancers. We provide evidence that the regulatory role of CBP does not stop at enhancers, but is extended to many genomic regions. CBP binds to insulators and regulates their activity by acetylating histones to prevent spreading of H3K27me3. We further discovered that CBP has a direct regulatory role at promoters. Using a highly potent CBP inhibitor in combination with ChIP and PRO-seq we found that CBP regulates promoter proximal pausing of Pol II. CBP promotes Pol II recruitment to promoters via a direct interaction with TFIIB, and promotes transcriptional elongation by acetylating the first nucleosome. CBP is regulating Pol II activity of nearly all expressed genes, however, either recruitment or release of Pol II is the rate-limiting step affected by CBP. Taken together, these results reveal mechanistic insights into cell specification and transcriptional control during development. / <p>At the time of the doctoral defense, the following paper was unpublished and had a status as follows: Paper 4: Manuscript.</p><p> </p>

Epigenetics

Cell specification

Drosophila embryo

Dorsal morphogen

CBP/p300

Gene regulation

Chromatin

Promoter proximal Pol II pausing

Avaliação clínica, radiográfica e ultra-sonográfica da articulação fêmuro-tíbio-patelar pós desmotomia patelar medial experimental em eqüinos / Clinical, radiographic and ultrasonographic evaluation of the femurotibiopatellar joint after experimental medial patellar desmotomy in horses

Martins, Edivaldo Aparecido Nunes

22 November 2004

Este trabalho objetivou avaliar através do exame clínico, radiográfico e ultra-sonográfico a articulação fêmuro-tíbio-patelar pós desmotomia patelar medial. Foram utilizados oito equinos, machos e fêmeas, de peso, raça e idade variáveis. Todos animais foram submetidos a desmotomia patelar medial no membro pélvico direito. Os exames clínico e ultra-sonográfico foram realizados no 7&ordm;, 14&ordm;, 21&ordm;, 28&ordm;, 43&ordm;, 58&ordm;, 88&ordm; e 118&ordm; dia do pós-operatório. Os exames radiográficos e do líquido sinovial foram realizados no 15&ordm;, 30&ordm;, 60&ordm;, 90&ordm; e 120&ordm; dia do pós-operatório. No pós-operatório foi observado durante exame radiográfico do joelho direito, aumento do ângulo entre a superfície articular proximal da patela e a superfície cranial distal do fêmur, formação óssea na crista tibial, entesofitos na patela, deslocamento da patela e irregularidade óssea na superfície patelar lateral. No exame ultra-sonográfico foi observado aumento da espessura (p&lt;0,05) no segmento proximal e médio do ligamento patelar intermédio do membro pélvico direito, desmite do patelar intermédio, enteseofitos na patela, distensão do recesso articular medial do fêmur, efusão articular e irregularidade da cartilagem do sulco troclear femoral. Conclui-se que a desmotomia patelar medial causa alterações no joelho devido a instbilidade articular e deve ser indicada apenas nos casos que não responderam a outras forma de tratamento. / This study aimed the evaluation of the femurotibiopatellar joint trough clinical, radiographic and ultrasonographic examinations after experimental medial patellar desmotomy. Medial patellar desmotomy was performed on the right hindlimb in eight mixed-breed horses. The clinical and ultrasonographic evaluation was performed on day 7, 14, 21, 28, 43, 58, 88 e 118 after surgery. The radiographic and synovial fluid evaluation was performed on day 15, 30, 60, 90 e 120 after surgery. It was observed during radiographic evaluation of the right stifle, an increase of the angle between the patellar proximal articular surface and the cranial distal femur surface. During ultrasonographic evaluation it was observed thickening (p&lt;0,05) on the proximal and midlle segment of the midlle patellar ligament on the right hindlimb, entesophyte at the patella, femoral medial joint recess distending, joint effusion and cartilage irregularity of the femoral troclear groove. The medial patellar desmotomy causes stifle changes and must be performed only in animals non responsive to other treatment.

Desmotomia patelar medial

Eqüinos

Fixação dorsal da patela

Horses

Joelho

Medial patellar desmotomy

Stifle

Ultrasonografia

Ultrasonographic

Upward fixation of the patella

Envolvimento dos sítios de ligação benzodiazepínicos localizados na substância cinzenta periaquedutal dorsal de ratos nos efeitos ansiolítico e panicolítico causado pelo alprazolam / Involvement of the benzodiazepine binding sites in the dorsal periaqueductal gray matter of rats in the anxiolytic- and panicolytic-like effects promoted by alprazolam

Frias, Alana Tercino

06 February 2018

O transtorno do pânico (TP) é um transtorno de ansiedade caracterizado por ataques de pânico recorrentes e inesperados, com um prognóstico crônico. Entre as drogas utilizadas no tratamento do TP, os benzodiazepínicos (BZs) de alta potência, como o alprazolam e o clonazepam, apresentam a vantagem de serem eficazes logo no início do tratamento. Assim como outras drogas BZs, tais como o diazepam e o flurazepam, estes compostos também são empregados como ansiolíticos no tratamento de pacientes com transtorno de ansiedade generalizada. O mecanismo da ação primária dessas drogas ocorre pela interação com os sítios de ligação BZs presentes nos receptores do ácido gama-aminobutírico do tipo A (GABAA), facilitando a neutotransmissão GABAérgica. Entretanto, ainda permanecem desconhecidos os substratos neurais envolvidos no efeito panicolítico causado pelos BZs. Dentre os substratos em potencial, a substância cinzenta periaquedutal dorsal (SCPD), uma estrutura mesencefálica criticamente relacionada à fisiopatogênica do TP, apresenta alta densidade de receptores GABAA e de sítios de ligação BZs. Neste trabalho avaliamos o envolvimento do complexo receptor GABAA/BZ presente na SCPD no efeito panicolítico promovido pela administração sistêmica de alprazolam em ratos Wistar. Para isso, empregamos o labirinto em T elevado (LTE), que além da resposta de fuga, que é associada ao pânico, também permite avaliar a resposta de esquiva inibitória, associada à ansiedade. Neste modelo, o alprazolam inibe a expressão da resposta de fuga, indicando efeito panicolítico e inibe a aquisição da esquiva inibitória, sugestivo de efeito ansiolítico. Além do LTE, também empregamos os modelos experimentais da hipóxia e o de Vogel, associados ao pânico e a ansiedade, respectivamente. Os resultados obtidos mostraram que o efeito panicolítico promovido pela administração sistêmica de alprazolam, observado na resposta de fuga do LTE, foi bloqueado pela administração intra-SCPD de flumazenil, antagonista dos sítios de ligação BZs, ou de bicuculina, antagonista dos receptores 10 GABAA. No teste da hipóxia, o efeito panicolítico causado pela administração sistêmica de alprazolam foi inibido, porém não significativamente bloqueado, pela administração intra-SCPD de bicuculina. Já o efeito ansiolítico, observado na resposta de esquiva do LTE e no teste do beber punido de Vogel, não foi bloqueado pela administração intra-SCPD de flumazenil ou de bicuculina. No conjunto, nossos resultados sugerem que o complexo receptor GABAA/BZ da SCPD está envolvido no efeito panicolítico, mas não ansiolítico, promovido pela administração sistêmica de alprazolam. / Panic Disorder (PD) is an anxiety disorder characterized by recurrent and unexpected panic attacks with a chronic prognosis. Among the drugs used to treat PD, highpotency benzodiazepines (BZs), such as alprazolam and clonazepam, have the advantage of causing significant effects early in the treatment. Like others BZs, such as diazepam and flurazepam, these compounds are also used as anxiolytics in the treatment of patients with generalized anxiety disorder. The primary mechanism of action of these drugs is the interaction with BZs binding sites present at gammaaminobutyric acid type A receptors (GABAA), facilitating GABAergic neurotransmission. However, it remains yet unknown the neural substrates involved in the panicolytic-like action caused by BZs. Among the potential substrates, the dorsal periaqueductal gray matter (DPAG), a mesencephalic structure critically associated with the physiopathology of PD, presents a high density of GABAA receptors and of BZs binding sites. In this work, we evaluated the participation of the GABAA/BZ receptor complex present in the DPAG in the panicolytic-like effect caused by systemic administration of alprazolam in Wistar rats. For this, we use the elevated T-maze (ETM), that besides the escape response which is associated with panic, also allows the measurement of inhibitory avoidance acquisition, which has been related to anxiety. In this model, alprazolam inhibits the expression of escape, indicating a panicolytic-like effect and inhibits the acquisition of inhibitory avoidance, suggestive of an anxiolytic effect. In addition to the ETM, animals were also tested in the hypoxia and Vogel\'s conflict tests, which have been associated with panic and anxiety, respectively. The results showed that the panicolytic-like effect caused by alprazolam in ETM\'s escape response was blocked by intra-DPAG injection of flumazenil, a BZs binding site antagonist, or bicuculline, a GABAA receptor antagonist. In the hypoxia test, the panicolytic-like effect caused by alprazolam was inhibited, but not significantly blocked, by intra-DPAG injection of bicuculline. The anxiolytic effect observed in the 12 ETM\'s avoidance task or in the Vogel\'s conflict test was not blocked by intra-DPAG injection of flumazenil or bicuculline. Taken together, our results suggest that the GABAA/BZ receptor complex located in the DPAG is involved in the panicolytic, but not anxiolytic, effect caused by systemic administration of alprazolam.

Estudo da participação da matéria cinzenta periaquedutal dorsal no comportamento defensivo de camundongos através do emprego de diferentes modelos animais de ansiedade: a estimulação química e a exposição ao predador / Role of the midbrain dorsal periaqueductal gray on defensive behaviors of mice evaluated in different animal models of anxiety: the local chemical stimulation and the prey-predator exposure

Carvalho Netto, Eduardo Ferreira de

28 February 2007

O medo e a ansiedade são emoções que apresentam claro valor adaptativo, e que tem suas origens nas reações de defesa que os animais exibem em resposta a situações de ameaça que podem comprometer sua integridade física ou sobrevivência. Recentes estudos têm indicado que a matéria cinzenta periaquedutal dorsal (MCPD) está envolvida na organização e expressão de comportamentos intempestivos do tipo fuga e luta, os quais são relacionados ao estado de medo, e também participa, juntamente com estruturas prosencefálicas (ex. córtex pré-frontal, sistema septo-hipocampal e amígdala), do controle de comportamentos defensivos mais elaborados e orientados relacionados à ansiedade. O presente estudo investigou a participação da MCPD na modulação de diferentes comportamentos defensivos (p. ex. fuga, esquiva e avaliação de risco) induzidos por métodos artificial (estimulação química) e naturalístico (exposição ao predador) em camundongos. Na primeira etapa, investigamos o padrão de resposta comportamental induzida pela infusão do ácido D,L-homocistéico (DLH, estímulo aversivo químico) na MCPD em diferentes situações ou ambientes, com e sem grande disponibilidade de espaço - o Mouse Defense Test Battery (MDTB) e a Arena (Experimento 1), respectivamente. Além disso, o presente estudo avaliou a habilidade dos animais de reagirem a estímulos aversivos (predador) durante o período inicial (nos 60 s iniciais) do efeito do ácido DLH (fuga explosiva) (Experimento 3), e imediatamente após esse período, no qual o animal apresente comportamento de congelamento ou imobilidade (Experimento 2). Nossos resultados indicaram que a fuga desencadeada pela estimulação química é a resposta predominante de camundongos e que sua exibição depende da disponibilidade de espaço, uma vez que a maioria dos saltos observados na arena está intimamente relacionada ao contato tátil do animal com as paredes do aparato. Esse perfil de respostas de fuga explosiva e saltos parece não representar o padrão comportamental defensivo natural, tal como acontece diante de uma ameaça proximal (ex. um predador), uma vez que durante a estimulação química os camundongos apresentaram um déficit na estratégia antipredador. A segunda etapa do estudo avaliou os efeitos da injeção intra-MCPD do agonista glutamatérgico ácido N-metil-D-aspártico (NMDA), do inibidor da enzima de síntese do óxido nítrico neuronial (NOSn), N?-propil-L-arginina (NPLA) (Experimento 4), e do agonista não seletivo de receptores do fator de liberação de corticotrofina (CRF), CRF ovino (oCRF) (Experimento 5), no comportamento defensivo de camundongos submetidos ao MDTB e ao teste de exposição ao rato (Rat Exposure Test; RET). Os resultados da segunda etapa demonstraram que a ativação de receptores NMDA na MCPD de camundongos intensifica comportamentos relacionados à esquiva do predador. De maneira interessante, essas alterações produzidas pelo NMDA foram consistentemente revertidas pelo inibidor da NOSn, previamente microinjetado no mesmo sítio. Além disso, efeitos intrínsecos do NPLA atenuaram as respostas de esquiva e de avaliação de risco em camundongos submetidos ao RET. Por fim, os resultados da segunda etapa também apontaram para um efeito proaversivo (nas respostas de salto e de esquiva) do agonista de receptores CRF, indicando uma participação dos sistemas glutamatérgico, nitrérgico e CRFérgico, localizados na MCPD, na modulação de diferentes estratégias defensivas (ex. esquiva, avaliação de risco e saltos) de camundongos submetidos ao confronto com o predador. Em conjunto, nossos resultados corroboram a hipótese de que a MPCD está envolvida tanto na organização e expressão de comportamentos intempestivos do tipo fuga e luta como também no controle de comportamentos defensivos mais elaborados e orientados, tais como a avaliação de risco e a esquiva. / The midbrain dorsal periaqueductal grey (DPAG) is part of the brain defensive system involved in active defense reactions to threatening stimuli. Many lines of evidence suggest that besides fundamentally controlling fear-like responses (fight and flight) the DPAG also controls responses related to anxiety, such as avoidance and risk assessment. This study investigated the role of DPAG on different defensive strategies (i.e. flight, avoidance and risk assessment) elicited by artificial (chemical stimulation, Experiments 1-3) and naturalistic (exposure to predator, Experiments 4 and 5) paradigms in mice. Firstly, D,L-Homocysteic acid (DLH) was infused into the DPAG and behavioral responses of mice were evaluated in two different situations, a rectangular novel chamber and a large oval runway, the Mouse Defense Test Battery (MDTB) apparatus (Exp. 1). We also investigated the ability of mice to react to a threatening stimulus (ex. a predator) during (Exp. 3) and immediately after (Exp. 2) the hyperactive responses (ex. jumping and running) induced by DLH injection. Our results indicated that running as opposed to jumping is the primary response in mice injected with DLH into the DPAG when the environment enables flight. However, mice did not react the predator during the flight reaction induced by chemical stimulation, suggesting the behavioral profile induced by DLH infusion into the DPAG is not related to a normal antipredator flight. In the Experiments 4 and 5, we evaluated the effects of three different compounds, N-methyl-D-Aspartate (NMDA), a NMDA receptor agonist, N?-propyl-L-arginine (NPLA), an neuronal nitric oxide synthase (nNOS) inhibitor as well as ovine CRF (oCRF), a nonspecific corticotropin-releasing factor (CRF) receptor agonist, injected into the DPAG of mice, in two predator-stress situations, the Mouse Defense Test Battery (MDTB), and the Rat Exposure Test (RET). Firstly, our results demonstrated that NMDA receptor activation into the mouse DPAG enhances antipredator reactivity (avoidance), an effect that was attenuated by prior infusion of NPLA into the same site. Moreover, the results from the Experiment 4 indicated that the NPLA treatment per se induces consistent anti-aversive effects on defensive behaviors (avoidance and risk assessment) of mice confronted by predator. Finally, our results pointed out a proaversive effect (e.g. increased jump escapes and avoidance behaviors) following intra-DPAG infusion of oCRF, suggesting an important role of glutamatergic, nitrergic and CRFergic systems into the DPAG on the defensive behaviors (risk assessment, avoidance and jumps) elicited by the confront to the predator. Taken together, present results are compatible with previous studies which have emphasized the role of the periaqueductal gray in the modulation of behavioral responses related to anxiety such as risk assessment and avoidance besides fundamentally controlling fear-like responses.

chemical stimulation

Comportamento defensivo

defense behaviors

estimulação química

matéria cinzenta periaquedutal

MDTB e RET

midbrain dorsal periaqueductal grey

modelo presa-predador

Comparação entre posiçao prona e posiçao supina, associadas à ventilação oscilatória de alta frequência, em modelo experimental de lesão pulmonar aguda /

Pires, Rafaelle Batistella.

January 2013

Orientador: José Roberto fioretto / Banca: Mário Ferreira Carpi / Banca: Carlos Fernando Ronchi / Resumo: A Síndrome do Desconforto Respiratório Agudo (SDRA) cursa com alta mortalidade apesar do melhor entendimento de sua fisiopatologia e avanços no tratamento. A Ventilação Oscilatória de Alta Frequência (VOAF) é método protetor por utilizar baixos volumes correntes (VC). Existem terapias adjuvantes à ventilação, dentre as quais se destaca a posição prona, que possibilita homogeneização da distribuição do VC e promove recrutamento alveolar. O objetivo foi investigar o efeito da posição prona associada à VOAF sobre a oxigenação, inflamação, histologia e dano oxidativo pulmonares, comparando-a com a posição supina neste mesmo modo ventilatório em modelo experimental de lesão pulmonar aguda (LPA) induzida em coelhos. Trinta coelhos foram instrumentados com traqueostomia e acessos vasculares e ventilados. A LPA foi induzida por infusão traqueal de salina aquecida (30mL/Kg, 38°C). Os coelhos foram submetidos à VOAF e divididos em dois grupos (n=15), um ventilado em posição supina (GS) e outro em posição prona (GP). VOAF foi iniciada com pressão aérea média de 16 cmH2O, que foi diminuída a cada 30 minutos até 10-11 cmH2O. Nos últimos 30 minutos os coelhos foram reposicionados em posição supina. Parâmetros ventilatórios e hemodinâmicos foram registrados a cada 30 minutos durante 150 minutos. Os desfechos foram: oxigenação, avaliada pela relação PaO2/FiO2 e índice de oxigenação (IO); inflamação pulmonar, avaliada pela porcentagem de polimorfonucleares (PMN) no lavado broncoalveolar (BAL) e pelo nível de TNF-alfa medido no BAL e no tecido pulmonar nas áreas ventral e dorsal; estresse oxidativo tecidual pulmonar, determinado pelo método de peroxidação lipídica (malondialdeído); e lesão tecidual pulmonar, determinada por escore histológico de lesão por área pulmonar. O nível de significância avaliado... (Resumo completo, clicar acesso eletrônico abaixo) / Abstract: Acute respiratory distress syndrome (ARDS) has been associated to high mortality rate despite better understanding of its pathophysiology and advances in treatment. High-frequency oscillatory ventilation (HFOV) is a protective ventilatory method because of using low tidal volume (VT). There are also many adjunctive therapies, of which prone position is known to allow homogenization of VT distribution and to promote alveolar recruitment. The objective was to investigate the prone position and HFOV association effects on oxygenation, inflammation, oxidative damage and lung histology, comparing to the supine position in this same ventilation mode, in experimental acute lung injury (ALI) induced in rabbits. Thirty rabbits were instrumented with tracheotomy and vascular catheters and ventilated. ALI was induced by tracheal infusion of warm saline (30mL/Kg, 38°C). Rabbits were submitted to HFOV and divided in two groups (n=15), one ventilated in supine position (SG), and the other in prone position (PG). HFOV was initiated with mean airway pressure of 16 cmH2O, which was decreased each 30 minutes until 10-11 cmH2O. In the last 30 minutes, all rabbits were repositioned to supine position. Ventilatory and hemodynamic parameters were recorded every 30 minutes for 150 minutes. The outcomes were: oxygenation, measured by PaO2/FiO2 ratio and oxygenation index (OI); lung inflammation, assessed by the percentage of polymorphonuclear cells (PMN) in bronchoalveolar lavage fluid (BAL) and by the level of TNF- alpha measured in BAL and in lung tissue, in ventral and dorsal areas; lung tissue oxidative stress, determined by the method of lipid peroxidation (malondialdehyde); and lung tissue damage, as determined by a histological score of injury, in each lung area. A significance level of 5% was... (Complete abstract click electronic access below) / Mestre

Sindrome do desconforto respiratorio.

Insuficiência respiratória.

Respiração artificial.

Decúbito ventral.

Decúbito dorsal.

Coelho como animal de laboratorio.

Respiratory Distress Syndrome.

Neural drive to human respiratory muscles

Saboisky, Julian Peter, Clinical School - Prince of Wales Hospital, Faculty of Medicine, UNSW

January 2008

This thesis addresses the organisation of drive to human upper airway and inspiratory pump muscles. The characterisation of single motor unit activity is important as the discharge frequency or timing of discharge of each motor unit directly reflects the output of single motoneurones. Thus, the firing properties of a population of motor units is indicative of the neural drive to the motoneurone pool. The experiments presented in Chapter 2 measured the recruitment time of five inspiratory pump muscles (diaphragm, scalene, second parasternal intercostal, and third and fifth dorsal external intercostal muscles) during normal quiet breathing and quantified the timing and magnitude of drive reaching each muscle. Chapter 3 examined the EMG activity of a major upper airway muscle (the genioglossus). The single motor units of the genioglossus display activity that can be grouped into six types based on its association or lack of association with respiration. The types of activity are termed: Inspiratory Phasic, Inspiratory Tonic, Expiratory Phasic, Expiratory Tonic, Tonic, and Tonic Other. A new method is presented in Chapter 4 to illustrate large amounts of data from single motor units recorded from respiratory muscles in a concise manner. This single figure displays for each motor unit, the recruitment time and firing frequency, the peak discharge frequency and its time, and the derecruitment time and its frequency. This method, termed the time-and-frequency plot, is used to demonstrate differences in behaviour between populations of diaphragm (Chapter 2) and genioglossus (Chapter 3) motoneurones. In Chapter 5, genioglossus activity during quiet breathing is compared between a group of patients with severe OSA and healthy control subjects. The distribution of central drive is identical between the OSA and control subjects with the same proportion of the six types of motor unit activity in both groups. However, there are alterations in the onset time of Inspiratory Phasic and Inspiratory Tonic motor units in OSA subjects and their peak discharge rates are also altered. Single motor unit action potentials in OSA subjects showed an increased area. This suggests the presence of neurogenic changes and may provide a pathophysiological explanation for the increased multiunit electromyographic activity reported in OSA subjects during wakefulness.

Obstructive sleep apnoea

Motoneurones

Breathing

Time and Frequency Plot (TAFPLOT)

Genioglossus

Diaphragm

Scalene

Parasternal intercostal

Dorsal external intercostal

internal intercostal

Étude et évaluation d'une architecture de système pour les bases de données généralisées

Burnier, Marc

21 September 1984

Dans le cadre du projet TIGRE, on a mis en évidence les insuffisances de systèmes de gestion de données et plus particulièrement des systèmes de gestion de bases de données QUART à la manipulation de ces nouvelles informations volumineuses et structurellement complexes. Description des fondements de ces nouveaux types d'architectures et on aborde la phase d'expérimentation durant laquelle a été évaluée la machine base de données d'Intel, l'IDBP en l'opposant à une configuration plus traditionnelle définie autour de SOCRATE/CI.

base de données généralisées

machine base de données

nouvelle architecture de SGBD

nouvelle application

évaluation

DORSAL

Keeping Eye and Mind on the Road

Victor, Trent

January 2005

<p>This thesis is devoted to understanding and counteracting the primary contributing factor in traffic crashes: inattention. Foremost, it demonstrates the fundamental importance of proactive gaze in the road centre area for action guidance in driving. Inattention is explained with regard to two visual functions (vision-for-action and vision-for-identification), three forms of attentional selection (action-driven-, stimulus-driven-, and goal-directed attention), and two forms of prediction influences (extrapolation-based- and decision-based prediction influences). In Study I an automated eye-movement analysis method was developed for a purpose-built eye-tracking sensor, and was successfully validated. This analysis method was further developed, and several new measures of gaze concentration to the road centre area were created. Study II demonstrated that a sharp decrease in the amount of road centre viewing time is accompanied by a dramatic spatial concentration towards the road centre area in returning gaze during visual tasks. During cognitive tasks, a spatial gaze concentration to road centre is also evident; however contrary to visual tasks, road centre viewing time is increased because the eyes are not directed towards an object within the vehicle. Study III found that gaze concentration measures are highly sensitive to driving task demands as well as to visual and auditory in-vehicle tasks. Gaze concentration to the road centre area was found as driving task complexity increased, as shown in differences between rural curved- and straight sections, between rural and motorway road types, and between simulator and field motorways. Further, when task duration was held constant and the in-vehicle visual task became more difficult, drivers looked less at the road centre area ahead, and looked at the display more often, for longer periods, and for more varied durations. In closing, it is shown how this knowledge can be applied to create in-vehicle attention support functions that counteract the effects of inattention.</p>

Psychology

Vision

Eye-movements

Driving

Attention

Distraction

Ventral stream

Dorsal stream

Road safety

Traffic crashes

Evaluation methodology

Psykologi

Psychology

Psykologi

Ontogeny- and Sex-Dependent Contributions of the Neuronal Nitric Oxide Synthase (nNOS) Gene to Rewarding and Psychomotor Stimulating Effects of Cocaine

Balda, Mara A.

10 June 2009

Multiple interactions between dopamine (DA), glutamate, and nitric oxide (NO) in mesolimbic and corticostriatal circuits suggest that NO may play a critical role in cocaine-induced behavioral and neural plasticity. Clinical and preclinical studies have revealed that females and adolescents display unique vulnerabilities to the behavioral and neurochemical effects of cocaine as a result of sex-dependent and ontogeny-dependent differences in dopaminergic systems. Thus, my research objectives were to investigate the contributions of the neuronal nitric oxide synthase (nNOS) gene, ontogeny, and gender on the rewarding and sensitizing effects of cocaine. I found that nNOS significantly influences the rewarding aspects of cocaine in adolescent mice and adult male mice (i.e., major deficits in several phases of cocaine conditioned place preference (CPP) were detected in nNOS knockout (KO) adolescent mice and nNOS KO adult male mice). However, the contribution of nNOS was sex-dependent as CPP phases were normal in KO adult females. In contrast to CPP, I found a major ontogeny-dependent contribution of nNOS to the sensitizing effects of cocaine. Namely, while nNOS is essential for the development of behavioral sensitization in adult males, this type of behavioral plasticity develops independently of nNOS during adolescence. The contribution of nNOS was once again sex-dependent as behavioral sensitization was normal in adult KO females. Together, this line of investigation has revealed that the NO-signaling pathway has a) a sex-dependent role in the neuroplasticity underlying cocaine CPP and b) a sex-dependent and ontogeny-dependent influence on cocaine-induced behavioral sensitization. Stereological and western blot analysis revealed that a sensitizing regimen of cocaine resulted in an increase in nNOS and tyrosine hydroxylase (TH) immunoreactivity in the dorsal striatum (dST) of adult, but not adolescent, wild-type (WT) male mice. In the absence of nNOS, dopaminergic neurons in the ventral tegmental area (VTA) were severely reduced and cocaine caused a downregulation of dST TH suggesting that nitrergic levels modulate TH. Thus, the finding that nNOS is essential for the development of sensitization in adulthood, but not adolescence, together with the fact that cocaine upregulated nNOS and TH in the dST in adult, but not adolescent mice, strongly suggest that the nitrergic system underlies behavioral sensitization through modulation of the dopaminergic system in adulthood. These findings suggest different approaches in the clinical treatment of drug craving and drug-seeking behavior in adolescent and adult patients.