11 |
Conception de nouvelles molécules à activité sérotoninergique par des méthodes QSAR et des études de dynamique moléculaire de complexe ligands /récepteurMarot, Christophe 29 November 1995 (has links) (PDF)
Désireux de mettre au point de nouvelles substances pouvant présenter une activité biologique potentielle au niveau du Système Nerveux Central, nous avons envisagé d'étudier les Relations Quantitatives Structure-Activité (QSAR) sur plusieurs familles de composés 5-HT1A. L'objectif était de prédire l'activité et la sélectivité biologique de nouveaux ligands 5-HT1A vis-à-vis de certains neurorécepteurs transmembranaires (5-HT1A, alpha1, alpha2, D2). Pour ce faire, 382 composés issus de différentes familles chimiques (indole, tétraline, chromane, thiochromane, pipérazine, etc...) ont été modélisés et superposés aux pharmacophores 5-HT1A. Nous avons ensuite, pour chaque molécule, calculé et comparé différents descripteurs moléculaires représentatifs de l'aspect électrostatique, lipophilique, stérique et topologique. Les différentes tables constituées des composés et des descripteurs ont ensuite été étudiées par des analyses statistiques comme l'analyse en composantes principales, l'analyse discriminante, la régression multiple et l'analyse Partial Least Square. A partir des meilleurs modèles statistiques, l'activité biologique de nouveaux ligands a été prédite. Après la synthèse et les tests pharmacologiques, ces prédictions se sont révélées précises (écart moyen de 1 unité de pIC50). En parallèle, une étude de dynamique moléculaire du récepteur sérotoninergique transmembranaire 5-HT1A a été entreprise afin de rendre compte de l'importance fonctionnelle de ces ligands au niveau des interactions électrostatiques, stériques et lipophiliques mises en jeu au sein du site actif du récepteur. Ces études sur un nombre limité de complexes ligand/récepteur ont aussi été menées afin de comprendre le rôle de certaines parties fonctionnelles de ces ligands, rôle mal défini jusqu'alors par les autres techniques. Nous avons aussi obtenu des informations qualitatives sur les interactions et la mobilité de certaines parties du récepteur, entre autres sur les hélices transmembranaires TMH5, 6 et 7.
|
12 |
L’internalisation du récepteur 5-HT1A dans les neurones centraux : Développement de modèles cellulaires pour l’étude des mécanismes sous-jacents et des corrélats fonctionnels / The internalization of the 5-HT1A receptor in central neurons : Development of cellular models for studying the underlying mechanisms and functional correlatesAmar, Elodie 05 July 2012 (has links)
La sérotonine (5-HT) joue un rôle majeur dans la modulation de nombreuses fonctions physiologiques et des déficits de la neurotransmission sérotoninergique sont associés à la dépression. Les récepteurs de type 5-HT1A sont impliqués dans la régulation de l’humeur, et le délai d’action thérapeutique d’un traitement par antidépresseur inhibiteur sélectif de la recapture de la 5-HT (ISRS) serait en relation avec leur désensibilisation qui se développe progressivement dans les neurones du raphé au cours du traitement. De fait, il a été rapporté que l’accélération de la désensibilisation des (auto)récepteurs 5-HT1A dans le raphé induit une réduction du délai d’action des antidépresseurs ISRS. Des données indirectes suggèrent que l’internalisation des récepteurs 5-HT1A pourrait être impliquée dans leur désensibilisation. L’objectif de ma thèse a été d’étudier le lien entre l’internalisation des récepteurs 5-HT1A et leur désensibilisation. A cette fin, j’ai développé des outils permettant d’étudier les mécanismes d’internalisation des récepteurs 5-HT1A dans des lignées cellulaires puis dans des neurones de raphé ou d’hippocampe en culture primaire. Nous avons produit un vecteur pour l’expression du récepteur 5-HT1A étiqueté avec un site de liaison de la bungarotoxine (BBS-5-HT1A), et le suivi de son trafic en microscopie confocale et vidéomicroscopie dans les lignées cellulaires et les neurones. Notre construction a permis de montrer que le récepteur BBS-5-HT1A est internalisé constitutivement dans la lignée LLC-PK1 et dans les neurones de raphé et d’hippocampe. Cette internalisation implique la voie clathrine-dépendante, et est suivie du recyclage de la plus grande partie du récepteur internalisé à la membrane plasmique. Enfin, nous avons également montré que, suite à un traitement chronique avec le 8-OH-DPAT, le récepteur 5-HT1A présente aussi une internalisation agoniste-dépendante spécifiquement dans les neurones sérotoninergiques du raphé. De fait, ce phénomène n’intervient ni dans les neurones non-sérotoninergiques du raphé ni dans les neurones de l’hippocampe. Ces résultats suggèrent que l’internalisation du récepteur 5-HT1A, qui est induite par sa stimulation prolongée, dépend du phénotype du neurone qui l’exprime et met en jeu des mécanismes intracellulaires spécifiques. Le parallèle entre les différences régionales (raphé versus hippocampe) de l’internalisation agoniste-dépendante du récepteur 5-HT1A et celles qui concernent sa désensibilisation fonctionnelle sous traitement ISRS au long cours laisse à penser que l’endocytose du récepteur 5-HT1A pourrait jouer un rôle majeur dans sa propre régulation et dans celle de la neurotransmission sérotoninergique centrale. / Pas de résumé en anglais
|
13 |
Étude par la TEP au [18F]MPPF des récepteurs cérébraux sérotoninergiques 5-HT1A dans l’épilepsie du lobe temporal / Brain serotoninergic 5-HT1A receptor study using [18F]MPPF PET neuroimaging in the context of temporal lobe epilepsyDidelot, Adrien 23 June 2010 (has links)
Chez un patient épileptique, aucun examen ne permet la délimitation exacte de la zone épileptogène (ZE) qui est définie par la zone corticale nécessaire à la genèse des crises. Dans les épilepsies du lobe temporal (ELT), près d’un tiers des patients ne sont pas libres de crises après la chirurgie en dépit d’un bilan préopératoire concluant. La tomographie par émission de positons (TEP) au [18F]MPPF permet la mise en évidence de zones d’hypofixation qui sont, à l’échelle du groupe, corrélées à l’épileptogénicité du parenchyme cérébral. Afin d’évaluer la validité de la TEP au [18F]MPPF pour identifier la ZE au plan individuel, tout d'abord nous avons comparé l’analyse visuelle et statistique par SPM de la TEP au [18F]FDG à la TEP au [18F]MPPF en termes de sensibilité et de spécificité chez 42 patients souffrant d’une ELT en cours de bilan préchirurgical. Dans une seconde étude nous avons développé une méthode d’analyse statistique d’un index d’asymétrie (IA) de la fixation du [18F]MPPF [BPND] et comparé les rendements de cette nouvelle approche à l’analyse standard SPM des images TEP en utilisant deux seuils statistiques différents (p< 0,05, corrigé au niveau du voxel et p< 0,05, corrigé au niveau du cluster) chez 24 patients opérés et guéris de leur ELT. Dans une troisième étude nous avons évalué, au niveau du groupe, l’influence d’un état dépressif sur le BPND du [18F]MPPF chez 24 patients souffrant d’une ELT. Ces trois études ont permis les conclusions suivantes : i) dans des conditions d’analyse identiques, La TEP au [18F]MPPF est supérieure au [18F]FDG pour identifier le lobe épileptogène chez des patients souffrant d’une ELT, ii) L’analyse de l’IA, avec un seuil à p< 0,05 corrigé au niveau du cluster, est la meilleure technique d’analyse de la TEP au [18F]MPPF et permet l’identification de la ZE avec une sensibilité de 96% et une spécificité de 88% dans l’ELT, iii) A l’échelle du groupe, un état dépressif est responsable d’une augmentation du BPND du [18F]MPPF dans les noyaux du raphé et l’insula controlatérale à la ZE. / In patients suffering from epilepsy, no neuroimaging method has proved able to delineate the epileptogenic zone (EZ), which is defined by the area of cortex required to generate the epileptic seizures. About one third of patient suffering from temporal lobe epilepsies (TLE) are not seizure free after surgery after removal of the cortical area supposed to included the EZ according to the presurgical evaluation. Data from previous studies carried out in our departement suggested that decreases of the [18F]MPPF binding potential (BPND) correlated, at the group level, with cortical epileptogenicity. Our aim was to validate the relevance of [18F]MPPF PET at the individual level for identifying the EZ in TLE. In a first study, the [18F]MPPF PET of 42 patients suffering from TLE were visually and statistically analyzed and compared with [18F]FDG PET, which were performed in the same group of patients during their presurgical evaluation. In a second study, we developed a voxel based analysis of asymmetry index (AI) of [18F]MPPF binding and compared the sensibility and specificity of this method to those of conventional SPM analysis of [18F]MPPF PET data. This second study was carried out in 24 patients, who have been operated and remained seizure-free after surgery. Two statistical thresholds (p< 0.05 corrected at the voxel level and p< 0.05 corrected at the cluster level) were used for each method. In a last study, the correlation between the depressive symptoms and the BPND of [18F]MPPF was studied in 24 patients suffering from TLE. These three studies lead to the following conclusions: i) [18F]MPPF PET is more performant than [18F]FDG PET for identifying the epileptogenic lobe in patients suffering from TLE, ii) AI analysis with a statistical threshold of p< 0.05 corrected at the cluster is the method of analysis of [18F]MPPF PET that allowed EZ identification with the best sensitivity [96%] and specificity [88%] in TLE, iii) at the group level, depressive symptoms positively correlate with an increase of the BPND of [18F]MPPF BPND within the raphe nuclei and the insula controlateral to the EZ.
|
14 |
Apports de la TEP dans l’imagerie moléculaire des récepteurs sérotoninergiques 5-HT1A et 5-HT7 / Contributions of PET in molecular imaging of 5-HT1A and 5-HT7 serotonin receptorsLemoine, Laëtitia 04 March 2011 (has links)
Le système sérotoninergique, impliqué dans plusieurs pathologies du système nerveux central, peut être exploré in vivo par l’imagerie TEP (tomographie par émission de positons). La recherche et la validation préclinique de radiotraceurs ciblant spécifiquement les récepteurs sérotoninergiques est donc cruciale. Au cours de ce travail, nous nous sommes intéressés à deux récepteurs sérotoninergiques pour lesquels nous avons développé des outils moléculaires pour leur imagerie fonctionnelle: (i) les récepteurs 5-HT1A et (ii) les récepteurs 5-HT7. (i) Les récepteurs 5-HT1A sont parmi les récepteurs à sérotonine les mieux décrits à l’heure actuelle. Cependant, si des radiotraceurs TEP sont déjà disponibles, ceux-ci sont des antagonistes qui se fixent indifféremment aux récepteurs 5-HT1A, couplés aux protéines G et fonctionnels, et aux récepteurs 5-HT1A, découplés et non fonctionnels. Nous avons donc proposé une stratégie originale de développement d’un agoniste 5- HT1A radiomarqué au fluor afin d’accéder à une imagerie des récepteurs fonctionnels. Deux molécules, le F15599 et le F13714, initialement développées pour leurs propriétés antidépressives par un partenaire industriel, ont été radiomarquées au fluor 18 puis ont été évaluées in vitro, ex vivo et in vivo chez le rat et le chat. Nos résultats montrent que le [18F]F13714 permet de visualiser de manière inédite les récepteurs 5- HT1A couplés aux protéines G. (ii) Le deuxième axe de cette thèse concerne les récepteurs 5-HT7, de découverte récente et proposés comme cible thérapeutique antidépressive. A l’inverse des récepteurs 5-HT1A, les récepteurs 5-HT7 ne disposent pas encore de radiotraceur TEP. Notre approche a consisté à sélectionner, à partir du pharmacophore du récepteur, quatre structures d’antagonistes 5-HT7, synthétisées par un laboratoire partenaire de chimie : le 2FP3, le 4FP3, le 2FPMP et le 4FPMP. Nos études radiopharmacologiques in vitro, ex vivo et in vivo nous ont conduit à retenir un radiotraceur, le [18F]2FP3. À l’issue de ce travail de thèse CIFRE, nous pouvons donc proposer deux radiotraceurs TEP originaux, ouvrant des perspectives inédites d’imagerie moléculaires de la neurotransmission 5-HT1A et 5-HT7 et dont nous envisageons la poursuite du développement comme radiopharmaceutiques cliniques / The serotonergic system, implicated in several diseases of central nervous system, can be explored in vivo by PET imaging (positron emission tomography). The research and the preclinical validation of radiotracers that specifically target serotonin are crucial. In this work, we focused on two serotonin receptors for which we have developed molecular tools for functional imaging: (i) the 5-HT1A and (ii) the 5-HT7. (i) 5-HT1A receptors are among the serotonin receptors the best described at present. However, if PET radiotracers are already available, they are antagonists and bind either to 5-HT1A receptors, G protein-coupled and functional, and to 5-HT1A receptors decoupled and non-functional. We therefore proposed an original strategy to develop a 5-HT1A agonist labeled with fluorine to access imagery of functional receptors. Two molecules, the F15599 and F13714, initially developed for their antidepressant properties by an industrial partner, were radiolabeled with fluorine-18 and were evaluated in vitro, ex vivo and in vivo in rats and cats. Our results show that the [18F] F13714 may view in a new way the 5-HT1A G protein-coupled (ii) The second focus of this thesis for the 5-HT7, recently discovered and proposed as a therapeutic target antidepressant. Unlike the 5-HT1A, 5-HT7 receptors do not yet have PET radiotracer. Our approach was to select, from the pharmacophore of the receptor, four structures of 5-HT7 antagonists, synthesized by a lab partner in chemistry: the 2FP3, the 4FP3, the 2FPMP and 4FPMP. Our radiopharmacology in vitro, ex vivo and in vivo led us to retain a radiotracer, the [18F] 2FP3. At the conclusion of this thesis CIFRE, we can propose two originals PET radiotracers , opening new perspectives for molecular imaging of neurotransmission of 5-HT1A and 5-HT7 receptors and which we plan further development as clinical radiopharmaceuticals
|
15 |
Efeitos do canabidiol no comportamento agressivo induzido por isolamento social em camundongos / Cannabidiol effects on agressive-like behaviors induced by social isolation in miceAlice Hartmann dos Santos 28 January 2016 (has links)
O Canabidiol (CBD), principal composto não-psicotomimético da Cannabis sativa, possui diversas propriedades farmacológicas, incluindo a indução de efeitos tipoantidepressivos e ansiolíticos em roedores após administração sistêmica. O isolamento social aumenta comportamentos agressivos em camundongos, condição denominada agressão induzida pelo isolamento social ou agressão territorial. Drogas ansiolíticas e antidepressivas podem atenuar comportamentos agressivos. Desse modo, o objetivo do presente trabalho foi avaliar se o CBD atenuaria comportamentos agressivos induzidos pelo isolamento social em camundongos. Camundongos Suíços machos (7-8 semanas de idade no dia do isolamento, 30-40 g no dia do teste) foram mantidos isolados (camundongos residentes) para indução dos comportamentos agressivos. Paralelamente, camundongos co-específicos (camundongos intrusos) foram mantidos agrupados (oito por caixa). Neste modelo, um camundongo intruso da mesma linhagem, sexo e idade foi colocado na caixa moradia do residente. As interações entre os camundongos residente e intruso foram gravadas por 20 min e a latência para a primeira mordida contra o intruso, o número de ataques e o tempo total de ataques foram analisados por um observador cego aos grupos experimentais. Após 10 dias de isolamento social, foi testado se a administração aguda (i.p.) de CBD (5, 15, 30 ou 60 mg/kg), 30 min antes do teste, atenuaria comportamentos agressivos dos camundongos residentes contra os intrusos. Para avaliar a participação de receptores 5-HT1A e CB1 nos efeitos do CBD, grupos independentes de animais receberam 1 injeção prévia de WAY 100635 (antagonista dos receptores 5-HT1A, 0,3 mg/kg) ou AM251 (antagonista dos receptores CB1, 1 mg/kg), 30 min antes do CBD (15 mg/kg). Para controlar possíveis efeitos motores da droga, grupos independentes de animais tratados com doses efetivas de CBD ou não efetivas de WAY100635 ou AM251 foram submetidos ao actímetro para avaliação da atividade locomotora total. O CBD (15 mg/kg) aumentou a latência para o residente atacar o intruso e este efeito foi atenuado tanto pela administração prévia de AM251 (VEI+VEI: 186,62±83,16; VEI+CBD: 956,25±150,77; AM+VEI: 271,71±156,18; AM+CBD: 395,86±208,24; p=0,030) quanto WAY100635 (VEI+VEI: 116,33±29,38; VEI+CBD: 860,87±177,36; WAY+VEI: 305,12±159,16; WAY+CBD: 302,57±154,68; p=0,011). Além disso, o CBD reduziu o número de ataques em todas as doses testadas (VEI: 23,00±3,66; CBD 5: 12,25±2,43; CBD 15: 6,62±2,43; CBD 30: 7,71±3,24; CBD 60: 8,16±2,36; p=0,002) e as doses intermediárias (15 e 30 mg/kg) foram capazes de diminuir o tempo total de ataques (VEI: 114,37±22,65; CBD 5: 80,87±23,83; CBD 15: 40,00±14,58; CBD 30: 25,86±12,88; CBD 60: 54,67±9,68; p=0,018), ambos os efeitos sendo atenuados pelo AM251 (Número de ataques - VEI+VEI: 19,25±2,56; VEI+CBD: 3,25±2,36; AM+VEI: 22,86±4,97; AM+CBD: 14,14±4,10; p=0,028; Tempo total de ataques - VEI+VEI: 66,62±9,19; VEI+CBD: 11,75±9,56; AM+VEI: 118,86±31,00; AM+CBD: 58,71±17,45; p=0,049) e WAY100635 (Número de ataques - VEI+VEI: 30,83±6,77; VEI+CBD: 7,87±4,68; WAY+VEI: 22,50±5,06; WAY+CBD: 23,57±6,74; p=0,059; Tempo total de ataques - VEI+VEI: 151,17±32,65; VEI+CBD: 16,75±10,88; WAY+VEI: 113,75±24,66; WAY+CBD: 76,29±21,36; p=0,002). Não foi observado efeito motor do CBD em nenhuma das doses testadas, bem como do WAY100635 e AM251. Esses resultados evidenciam que o CBD atenua comportamentos agressivos em camundongos e nos permitem sugerir um mecanismo misto, visto que há o envolvimento de receptores CB1 e 5-HT1A. Desse modo, este fitocanabinoide poderia ser uma alternativa terapêutica para tratar comportamentos agressivos associados a transtornos psiquiátricos / Cannabidiol (CBD), a major non-psychotomimetic compound from Cannabis sativa plant, induces anxiolytic- and antidepressant-like effects in rodents after systemic administration. Long-term individual housing increases aggressive behavior in mice, a condition named isolation-induced aggression or territorial aggression, which can be attenuated by anxiolytic and antidepressant drugs. Thus, the aim of the present study was to verify whether CBD would attenuate the aggressive behavior induced by social isolation. Male Swiss mice (7-8 weeks of age on the isolation day, 30-40 g on the test day) were individually housed (resident mice) to induce aggressive behavior, while conspecific mice (intruder mice) were grouped housed (eight per cage). In this model, an intruder mouse of the same strain, sex and age is placed in the resident home cage. The resident-intruder interactions were videotaped for 20 min and the latency to the first bite against the intruder, the number of attacks and the total duration of aggressive encounters were recorded and later analyzed by an observer blind to the treatment groups. After 10 days of social isolation, we tested if acute intraperitoneal CBD administration (5, 15, 30 and 60 mg/kg) to the resident mice 30 min prior to the test would attenuate aggressive-like behavior towards the intruder animal. To evaluate the involvement of 5-HT1A and CB1 receptors in the CBD effects, independent groups of animals were injected with WAY100635 (0.3 mg/kg) or AM251(1 mg/kg) 30 min prior to CBD (15 mg/kg). To control possible motor effects, independent animals treated with effective doses of CBD or ineffective doses of WAY100635 or AM251 were submitted to the actimeter to evaluate the total locomotor activity. CBD (15 mg/kg) increased latency to attack the intruder and this effect was attenuated by the prior administration of AM251 (VEI+VEI: 186.62±83.16; VEI+CBD: 956.25±150.77; AM+VEI: 271.71±156.18; AM+CBD: 395.86±208.24; p=0.030) or WAY100635 (VEI+VEI: 116.33±29.38; VEI+CBD: 860.87±177.36; WAY+VEI: 305.12±159.16; WAY+CBD: 302.57±154.68; p=0.011). Moreover, CBD reduced the number of attacks in all tested doses (VEI: 23.00±3.66; CBD 5: 12.25±2.43; CBD 15: 6.62±2.43; CBD 30: 7.71±3.24; CBD 60: 8.16±2.36; p=0.002) as well as the duration of aggressive behavior encounters in the intermediary doses (15 and 30 mg/kg; VEI: 114.37±22.65; CBD 5: 80.87±23.83; CBD 15: 40.00±14.58; CBD 30: 25.86±12.88; CBD 60: 54.67±9.68; p=0.018), both effects were attenuated by AM251 (Number of attacks - VEI+VEI: 19.25±2.56; VEI+CBD: 3.25±2.36; AM+VEI: 22.86±4.97; AM+CBD: 14.14±4.10; p=0.028; Total time of attacks - VEI+VEI: 66.62±9.19; VEI+CBD: 11.75±9.56; AM+VEI: 118.86±31.00; AM+CBD: 58.71±17.45; p=0.049) and WAY100635 (Number of attacks - VEI+VEI: 30.83±6.77; VEI+CBD: 7.87±4.68; WAY+VEI: 22.50±5.06; WAY+CBD: 23.57±6.74; p=0.059; Total time of attacks - VEI+VEI: 151.17±32.65; VEI+CBD: 16.75±10.88; WAY+VEI: 113.75±24.66; WAY+CBD: 76.29±21.36; p=0.002). CBD, in all tested doses, as well as WAY100635 and AM251, did not induce locomotor changes. These findings suggest that CBD decreases aggressive behaviors in mice and allow us to suggest that this effect involves CB1 and 5-HT1A receptors. Therefore, this phytocannabinoid may be therapeutically useful to treat aggressive behaviors that are usually associated with psychiatric disorders
|
16 |
Efeitos do canabidiol no comportamento agressivo induzido por isolamento social em camundongos / Cannabidiol effects on agressive-like behaviors induced by social isolation in miceSantos, Alice Hartmann dos 28 January 2016 (has links)
O Canabidiol (CBD), principal composto não-psicotomimético da Cannabis sativa, possui diversas propriedades farmacológicas, incluindo a indução de efeitos tipoantidepressivos e ansiolíticos em roedores após administração sistêmica. O isolamento social aumenta comportamentos agressivos em camundongos, condição denominada agressão induzida pelo isolamento social ou agressão territorial. Drogas ansiolíticas e antidepressivas podem atenuar comportamentos agressivos. Desse modo, o objetivo do presente trabalho foi avaliar se o CBD atenuaria comportamentos agressivos induzidos pelo isolamento social em camundongos. Camundongos Suíços machos (7-8 semanas de idade no dia do isolamento, 30-40 g no dia do teste) foram mantidos isolados (camundongos residentes) para indução dos comportamentos agressivos. Paralelamente, camundongos co-específicos (camundongos intrusos) foram mantidos agrupados (oito por caixa). Neste modelo, um camundongo intruso da mesma linhagem, sexo e idade foi colocado na caixa moradia do residente. As interações entre os camundongos residente e intruso foram gravadas por 20 min e a latência para a primeira mordida contra o intruso, o número de ataques e o tempo total de ataques foram analisados por um observador cego aos grupos experimentais. Após 10 dias de isolamento social, foi testado se a administração aguda (i.p.) de CBD (5, 15, 30 ou 60 mg/kg), 30 min antes do teste, atenuaria comportamentos agressivos dos camundongos residentes contra os intrusos. Para avaliar a participação de receptores 5-HT1A e CB1 nos efeitos do CBD, grupos independentes de animais receberam 1 injeção prévia de WAY 100635 (antagonista dos receptores 5-HT1A, 0,3 mg/kg) ou AM251 (antagonista dos receptores CB1, 1 mg/kg), 30 min antes do CBD (15 mg/kg). Para controlar possíveis efeitos motores da droga, grupos independentes de animais tratados com doses efetivas de CBD ou não efetivas de WAY100635 ou AM251 foram submetidos ao actímetro para avaliação da atividade locomotora total. O CBD (15 mg/kg) aumentou a latência para o residente atacar o intruso e este efeito foi atenuado tanto pela administração prévia de AM251 (VEI+VEI: 186,62±83,16; VEI+CBD: 956,25±150,77; AM+VEI: 271,71±156,18; AM+CBD: 395,86±208,24; p=0,030) quanto WAY100635 (VEI+VEI: 116,33±29,38; VEI+CBD: 860,87±177,36; WAY+VEI: 305,12±159,16; WAY+CBD: 302,57±154,68; p=0,011). Além disso, o CBD reduziu o número de ataques em todas as doses testadas (VEI: 23,00±3,66; CBD 5: 12,25±2,43; CBD 15: 6,62±2,43; CBD 30: 7,71±3,24; CBD 60: 8,16±2,36; p=0,002) e as doses intermediárias (15 e 30 mg/kg) foram capazes de diminuir o tempo total de ataques (VEI: 114,37±22,65; CBD 5: 80,87±23,83; CBD 15: 40,00±14,58; CBD 30: 25,86±12,88; CBD 60: 54,67±9,68; p=0,018), ambos os efeitos sendo atenuados pelo AM251 (Número de ataques - VEI+VEI: 19,25±2,56; VEI+CBD: 3,25±2,36; AM+VEI: 22,86±4,97; AM+CBD: 14,14±4,10; p=0,028; Tempo total de ataques - VEI+VEI: 66,62±9,19; VEI+CBD: 11,75±9,56; AM+VEI: 118,86±31,00; AM+CBD: 58,71±17,45; p=0,049) e WAY100635 (Número de ataques - VEI+VEI: 30,83±6,77; VEI+CBD: 7,87±4,68; WAY+VEI: 22,50±5,06; WAY+CBD: 23,57±6,74; p=0,059; Tempo total de ataques - VEI+VEI: 151,17±32,65; VEI+CBD: 16,75±10,88; WAY+VEI: 113,75±24,66; WAY+CBD: 76,29±21,36; p=0,002). Não foi observado efeito motor do CBD em nenhuma das doses testadas, bem como do WAY100635 e AM251. Esses resultados evidenciam que o CBD atenua comportamentos agressivos em camundongos e nos permitem sugerir um mecanismo misto, visto que há o envolvimento de receptores CB1 e 5-HT1A. Desse modo, este fitocanabinoide poderia ser uma alternativa terapêutica para tratar comportamentos agressivos associados a transtornos psiquiátricos / Cannabidiol (CBD), a major non-psychotomimetic compound from Cannabis sativa plant, induces anxiolytic- and antidepressant-like effects in rodents after systemic administration. Long-term individual housing increases aggressive behavior in mice, a condition named isolation-induced aggression or territorial aggression, which can be attenuated by anxiolytic and antidepressant drugs. Thus, the aim of the present study was to verify whether CBD would attenuate the aggressive behavior induced by social isolation. Male Swiss mice (7-8 weeks of age on the isolation day, 30-40 g on the test day) were individually housed (resident mice) to induce aggressive behavior, while conspecific mice (intruder mice) were grouped housed (eight per cage). In this model, an intruder mouse of the same strain, sex and age is placed in the resident home cage. The resident-intruder interactions were videotaped for 20 min and the latency to the first bite against the intruder, the number of attacks and the total duration of aggressive encounters were recorded and later analyzed by an observer blind to the treatment groups. After 10 days of social isolation, we tested if acute intraperitoneal CBD administration (5, 15, 30 and 60 mg/kg) to the resident mice 30 min prior to the test would attenuate aggressive-like behavior towards the intruder animal. To evaluate the involvement of 5-HT1A and CB1 receptors in the CBD effects, independent groups of animals were injected with WAY100635 (0.3 mg/kg) or AM251(1 mg/kg) 30 min prior to CBD (15 mg/kg). To control possible motor effects, independent animals treated with effective doses of CBD or ineffective doses of WAY100635 or AM251 were submitted to the actimeter to evaluate the total locomotor activity. CBD (15 mg/kg) increased latency to attack the intruder and this effect was attenuated by the prior administration of AM251 (VEI+VEI: 186.62±83.16; VEI+CBD: 956.25±150.77; AM+VEI: 271.71±156.18; AM+CBD: 395.86±208.24; p=0.030) or WAY100635 (VEI+VEI: 116.33±29.38; VEI+CBD: 860.87±177.36; WAY+VEI: 305.12±159.16; WAY+CBD: 302.57±154.68; p=0.011). Moreover, CBD reduced the number of attacks in all tested doses (VEI: 23.00±3.66; CBD 5: 12.25±2.43; CBD 15: 6.62±2.43; CBD 30: 7.71±3.24; CBD 60: 8.16±2.36; p=0.002) as well as the duration of aggressive behavior encounters in the intermediary doses (15 and 30 mg/kg; VEI: 114.37±22.65; CBD 5: 80.87±23.83; CBD 15: 40.00±14.58; CBD 30: 25.86±12.88; CBD 60: 54.67±9.68; p=0.018), both effects were attenuated by AM251 (Number of attacks - VEI+VEI: 19.25±2.56; VEI+CBD: 3.25±2.36; AM+VEI: 22.86±4.97; AM+CBD: 14.14±4.10; p=0.028; Total time of attacks - VEI+VEI: 66.62±9.19; VEI+CBD: 11.75±9.56; AM+VEI: 118.86±31.00; AM+CBD: 58.71±17.45; p=0.049) and WAY100635 (Number of attacks - VEI+VEI: 30.83±6.77; VEI+CBD: 7.87±4.68; WAY+VEI: 22.50±5.06; WAY+CBD: 23.57±6.74; p=0.059; Total time of attacks - VEI+VEI: 151.17±32.65; VEI+CBD: 16.75±10.88; WAY+VEI: 113.75±24.66; WAY+CBD: 76.29±21.36; p=0.002). CBD, in all tested doses, as well as WAY100635 and AM251, did not induce locomotor changes. These findings suggest that CBD decreases aggressive behaviors in mice and allow us to suggest that this effect involves CB1 and 5-HT1A receptors. Therefore, this phytocannabinoid may be therapeutically useful to treat aggressive behaviors that are usually associated with psychiatric disorders
|
17 |
La neuroimagerie TEP-IRM pour l'exploration de l'agonisme des récepteurs 5-HT1A / Exploration of 5-HT1A agonism through PET-MRI neuroimagingVidal, Benjamin 07 November 2017 (has links)
Depuis des années, l’imagerie TEP des récepteurs 5-HT1A a permis une compréhension accrue du rôle physiopathologique de ces récepteurs. Toutefois les radiotraceurs actuels ne permettent pas d’évaluer le couplage entre récepteurs 5-HT1A et protéines G, susceptible d’être altéré au cours de pathologies. Les travaux effectués au cours de cette thèse visent à promouvoir l’utilisation de techniques d’imagerie translationnelles pour explorer le couplage des récepteurs 5-HT1A in vivo. La première partie a consisté à évaluer un agoniste des récepteurs 5-HT1A, le F13640, comme potentiel radiotraceur TEP. L’ensemble des résultats suggère que le [18F]F13640 est spécifique des récepteurs 5-HT1A couplés, avec des propriétés inédites par rapport aux radiotraceurs classiques.La deuxième partie a consisté à évaluer l’intérêt de l’imagerie des récepteurs 5-HT1A couplés. Les variations de densité de récepteurs couplés et totaux ont été comparées en autoradiographie postmortem au cours de la maladie d’Alzheimer. La fixation du [18F]F13640 dans l’hippocampe est diminuée dès les premiers stades, tandis que la fixation du [18F]MPPF n’est réduite qu’aux stades avancés. Ces observations démontrent la complémentarité entre traceurs agonistes et antagonistes des récepteurs 5-HT1A en imagerie TEP.La dernière partie s’est focalisée sur le concept d’agonisme biaisé, impliquant la possibilité de cibler différentes populations de récepteurs 5-HT1A en fonction de leur couplage aux protéines G. Le F13640 a été comparé au F15599 à doses pharmacologiques en imagerie TEP et en IRMf. Chez le rat, ces deux agonistes produisent des réponses hémodynamiques et métaboliques différentes. Chez le chat, ils diffèrent également en termes d’occupation des récepteurs et de réponse hémodynamique conséquente. L’ensemble des données est en faveur d’une stimulation préférentielle des récepteurs postsynaptiques par le F15599 par rapport aux autorécepteurs, contrairement au F13640 / Since the 1990s, PET imaging of 5-HT1A receptors has led to an increased understanding of the pathophysiological role of these receptors. However, the coupling between 5-HT1A receptors and G-proteins, which may be altered during pathologies, cannot be explored using current radiotracers. The work carried out in this thesis aims to promote the use of translational imaging techniques to explore the coupling of 5-HT1A receptors in vivo. In the first part, we evaluated the 5-HT1A receptor agonist F13640 as a PET radiotracer candidate. Taken together, the results suggest that [18F]F13640 binds specifically to coupled 5-HT1A receptors and displays novel properties and distribution pattern compared to classical 5-HT1A radiotracers. The second part was a proof-of-concept study regarding the interest of coupled 5-HT1A receptors imaging. Densities of coupled and total receptors were compared in postmortem autoradiography during Alzheimer’s disease. [18F]F13640 binding in hippocampus was decreased in the early stages, whereas [18F]MPPF binding was reduced in the advanced stages only. These results confirm the complementarity between 5-HT1A receptor agonists and antagonist tracers in PET imaging.In the last part we focused on the concept of biased agonism, which implies the possibility of targeting different populations of 5-HT1A receptors depending on their coupling with G-proteins. F13640 and F15599 were compared at pharmacological doses using PET and fMRI imaging. The two agonists produce different hemodynamic and metabolic responses in rat brain. They also differ in cat brain in terms of receptor occupancy and subsequent hemodynamic responses. Taken together, the results are consistent with a preferential stimulation of postsynaptic receptors over autoreceptors for F15599, in contrast with F13640
|
18 |
Validation de la résignation apprise chez la souris : étude de modèles animaux de dépression / Learned helplessness validation in mice : study of animal models of depressionBougarel, Laure 30 September 2010 (has links)
Les études sur modèle animal sont essentielles pour l'élaboration de nouveaux antidépresseurs, à la compréhension de leurs mécanismes d'action et aux mécanismes de la physiopathologie de la dépression. Des facteurs génétiques jouent un rôle important dans l'étiologie des troubles de l'humeur. Notre équipe de recherche a créé un modèle basé sur la reproduction dirigée de souris présentant un trait comportemental relatif à la symptomatologie dépressive en se basant sur les performances obtenues dans l'épreuve de suspension par la queue, obtenant ainsi une lignée résignée et une lignée non résignée . Au cours de ces travaux, nous avons validé un protocole de résignation apprise (RA) chez la souris CD1. Cette épreuve consiste en i) une période de conditionnement, ii) une période de test. Il a été montré que 4 périodes de conditionnement avec des chocs à 0,3 mA sont nécessaires à l'obtention d'une résignation. Un second protocole de RA, sur 3 semaines, a également été validé chez la souris CD1 consistant en 4 périodes de conditionnement suivies de tests à J5, J10, J15 et J20. L'introduction d'un « rappel » de choc en J8 a permis d'entretenir la résignation jusqu'en J20 contrairement à un protocole identique sans rappel. Ce nouveau protocole s'avère être particulièrement adapté pour étudier les effets de traitements chroniques. Deux autres modèles animaux de dépression (issues de 8 souches de souris différentes) ont été également crées dans le laboratoire sur la base de performances dans l'épreuve de suspension par la queue (TST) ou l'épreuve de nage forcée (FST). Les résultats révèlent que les modèles issus de 8 souches criblés au TST ou au FST présentent des caractéristiques neurochimiques différentes, qui en plus d'un comportement différent dans l'épreuve de résignation apprise, confirment que ceux sont bien deux modèles animaux distincts / Studies on animal models are essential to the development of new antidepressants, to the understanding of their mechanisms of action and to the mechanisms underlying depressive disorders. Genetics factors play an important role in the etiology of mood disorders. Our research team elaborated a model based on the selective breeding of mice displaying a behavioural trait of the depression symptomatology. On the basis of the behaviour in the TST, two strains of mice with “helpless” or “non helpless” phenotype were developed. During this work, we validated a learned helplessness protocol in CD1 mice. This paradigm consists in i) a conditioning period. ii) an escape test. It has been found that 4 conditioning periods with 0.3 mA shocks were necessary to induce helplessness. A second learned helplessness protocol was developed in CD1 mice, consisting in 4 conditioning periods followed by escape test in D5, D10, D15 and D20. A “shock reminder” at D8 allowed to maintain helplessness up to D20. This new protocol is particularly appropriate for investigating effects of chronic treatments. The selective breeding lines (from 8 strains of mice) were based on their performance in either the tail suspension test or the forced swimmed test. The results confirmed that lines models (bred from 8 lines) have not only behavioural differences but also display different biochemical characteristics
|
19 |
Envolvimento do núcleo leito da estria terminal nos efeitos ansiolíticos do canabidiol / Involvement of the bed nucleus of the stria terminalis in the anxiolytic effects of cannabidiolGomes, Felipe Villela 26 January 2011 (has links)
O canabidiol (CBD), um componente não-psicotomomético presente na planta Cannabis sativa, induz efeitos ansiolíticos em roedores e humanos após administração sistêmica. Entretanto, poucos estudos foram feitos para identificar as estruturas cerebrais envolvidas nesses efeitos do CBD. Dados prévios do nosso laboratório apontam para um possível envolvimento do núcleo leito da estria terminal (NLET) nos efeitos ansiolíticos do CBD, como evidenciado pelos níveis alterados (reduzidos) de imunorreatividade para proteína c-Fos (marcador de ativação neuronial) em animais tratados com administração sistêmica de CBD no modelo da resposta emocional condicionada (REC) contextual. Os mecanismos de ação pelos quais o CBD produz seus também são ainda pouco compreendidos, mas pode envolver a ativação de receptores 5-HT1A. Assim, o presente trabalho investigou se a administração de CBD diretamente no NLET atenuaria a expressão da REC contextual. Além disso, nós também avaliamos o envolvimento do NLET nos efeitos ansiolíticos do CBD em outros dois modelos animais de ansiedade amplamente utilizados, o labirinto em cruz elevado e o teste do lamber punido de Vogel e, se os efeitos ansiolíticos do CBD envolveriam a ativação local de receptores 5-HT1A. Os resultados mostraram que o CBD reduziu significativamente o tempo de congelamento e atenuou as respostas cardiovasculares induzidas pela re-exposição ao contexto aversivo no modelo da REC contextual. Além disso, o CBD também aumentou a exploração dos braços abertos do LCE, bem como o número de lambidas punidas no teste de Vogel, sugerindo um efeito ansiolítico. Adicionalmente, o CBD não alterou o número de entradas nos braços fechados do LCE e não interferiu no consumo de água ou no limiar nociceptivo, descartando potenciais interferentes nesses dois modelos. Nós também observamos que o pré-tratamento local com WAY100635, um antagonista de receptores 5-HT1A, foi capaz de bloquear os efeitos do CBD injetado no NLET nos três modelos animais utilizados. Logo, estes resultados dão suporte à proposta que NLET está envolvido nos efeitos ansiolíticos do CBD observado após a administração sistêmica, e que este efeito parece envolver a neurotransmissão mediada por receptores 5-HT1A. / Cannabidiol (CBD), a major non-psychotomimetic compound from Cannabis sativa, induces anxiolytic effects in rodents and humans following systemic administration. Despite the brain structures of CBD acts remain poorly understood, previous results from our laboratory suggest that the bed nucleus of the stria terminalis (BNST) may be involved in the anxiolytic effects of CBD, as evidenced by changed levels (decreased) in c-Fos protein expression (a marker of neuronal activation) in animals treated with systemic administration of CBD in the contextual fear conditioning. The mechanisms of CBD effects are still poorly understood but may involve activation of 5-HT1A receptors. Thus, in the present study, we have investigated the anxiolytic-like effects of intra-BNST administration of CBD in rats submitted to contextual fear conditioning. Moreover, we also evaluated the involvement of the BNST in the anxiolytic effects of CBD in other two widely used animal models of anxiety, the elevated plus-maze and the Vogel conflict test, and if these effects are mediated by local activation of 5-HT1A receptors. The results showed that CBD significantly decreased the freezing time and attenuated the cardiovascular responses induced by contextual fear conditioning. Moreover, CBD has also increased the exploration of open arms in EPM, and the number of punished licks in the Vogel test, suggesting an anxiolytic effect. Additionally, the CBD did not alter the number of entries in closed arms of the EPM and did not affect water consumption or pain threshold, eliminating potential interferences of these two models. We also found that local pretreatment with WAY100635, a 5-HT1A receptor antagonist, was able to block the effects of CBD injected into the BNST in the three animal models of anxiety used. Hence, these results support the proposal that BNST is involved in anxiolytic effects of CBD observed after systemic administration, and this effect seems to involve the neurotransmission mediated by 5-HT1A receptors.
|
20 |
Papel dos receptores 5-HT1A do Núcleo Mediano da Rafe de ratos nas consequências comportamentais da exposição ao estresse de nado forçado / Role of 5-HT1A receptors of the Median Raphe Nucleus of rats in the behavioral consequences of exposure to forced swim stressTokumoto, Alline Mayumi 26 February 2010 (has links)
A exposição a estressores incontroláveis leva a alterações comportamentais e bioquímicas significativas que parecem envolver um mau funcionamento da via serotoninérgica Núcleo Mediano da Rafe (NMnR)-Hipocampo Dorsal, mediada por receptores de tipo 5-HT1A (5-HT1aR), sugerindo que as associações aprendidas, relacionadas à exposição ao estresse e suas conseqüências emocionais, não foram desconectadas. Estudos na literatura sugerem que processos de memória são tempo-dependentes e podem ser alterados pela administração de drogas no momento de sua formação ou evocação. Assim, o objetivo do trabalho foi investigar se a interferência na neurotransmissão serotoninérgica mediada por 5-HT1aR, no NMnR, em diferentes momentos com relação à exposição ao estresse de nado forçado pode prevenir ou atenuar os efeitos desse estressor. Ratos Wistar machos (n=5-13/grupo) receberam duas injeções intra-NMnR de Salina (Sal), 8-OH-DPAT (DPAT; 3nmoles/0,2µL; agonista 5-HT1aR) e/ou WAY100635 (WAY; 0,3nmoles/0,2µL; antagonista 5-HT1aR) compondo os grupos experimentais: Sal+Sal, Sal+DPAT, WAY+Sal, WAY+DPAT. As drogas foram administradas em três condições experimentais distintas: antes da pré-exposição ao nado forçado; antes do teste em animais submetidos à pré-exposição; ou antes do teste em animais não pré-expostos. O teste ocorreu 24 horas após a pré-exposição. O tempo de latência para o primeiro episódio de imobilidade (LAT) e o tempo total gasto imóvel (IMO) foram registrados. Somente animais com sítios de injeção confirmados foram usados na análise (ANOVA de uma via seguida por teste post hoc de Duncan). Nossos resultados sugerem que o tratamento com 8-OH-DPAT antes da pré-exposição ou do teste em animais estressados previne ou atenua, respectivamente, as consequências comportamentais da exposição prévia ao estresse de nado forçado. Além disso, nossos dados sugerem que tanto a interferência no processo de aquisição da memória aversiva quanto da evocação da mesma são em parte mediados por 5-HT1aR. / Exposure to uncontrollable stressors leads to significant behavioral and biochemical changes which has been associated to mal functioning of the Median Raphe Nucleus (NMnR) Dorsal Hippocampus serotonergic pathway, mediated by receptor type 5-HT1A (5-HT1aR), suggesting that learned associations related to exposure to stress and emotional consequences from such exposure were not disconnected. Published studies suggest that memory processes are time-dependent and can be changed by the administration of drugs at the time of its formation or retrieval. The objective of the present study was to investigate whether interference with serotonergic neurotransmission mediated by 5-HT1aR in NMnR at different times in relation to exposure to forced swim stress could prevent or reduce the effects of this stressor. Male Wistar rats (n = 5-13/grupo) received two intra-NMnR injections of Saline (Sal), 8-OH-DPAT (DPAT; 3nmoles / 0.2 mL; 5-HT1aR agonist) and / or WAY100635 (WAY; 0.3 nmol / 0.2 mL; 5-HT1aR antagonist) composing the experimental groups: Sal + Sal, Sal + DPAT, WAY + Sal, WAY + DPAT. The drugs were administered in three different experimental conditions: before preexposure to forced swim; before testing in animals subjected to preexposure; or before testing in animals not preexposed. The test occurred 24 hours after preexposure. The latency to the first episode of immobility (LAT) and the total time spent immobile e (IMO) were registered. Only animals who had their sites of injection confirmed were used in the analysis (one-way ANOVA followed by post hoc test Duncan). Our results suggest that treatment with 8-OH-DPAT before preexposure or testing in stressed animals prevents or attenuates, respectively, the behavioral consequences of prior exposure to forced swim stress. Furthermore, our data suggest that both the interference in the acquisition of aversive memory, and the retrieval of the same are partly mediated by 5-HT1aR.
|
Page generated in 0.0607 seconds