Reversão dos efeitos reforçadores da morfina através do prejuízo da reconsolidação da memória do condicionamento de preferência por local e da sensibilização locomotora

Boos, Flávia Zacouteguy

January 2016

A dependência de drogas é um transtorno multifatorial complexo que se desenvolve em uma minoria de indivíduos que fazem uso dessas substâncias. Memórias associativas entre a droga e o contexto funcionam como gatilho para disparar comportamentos não adaptativos de busca e consumo, além de recaídas após períodos de abstinência. Subjacentes a essas mudanças comportamentais, existem modificações nas subunidades de receptores glutamatérgicos do tipo AMPA em estruturas envolvidas com memória (Hipocampo) e recompensa (Núcleo Accumbens). Por isso, estratégias que enfraqueçam a associação do contexto com a droga e que aprofundem o conhecimento dos circuitos envolvidos nesses comportamentos são de extrema relevância terapêutica. A memória quando evocada pode passar por dois processos pós-evocação: a extinção, em que uma nova memória é formada inibindo uma prévia associação, e a reconsolidação, em que a memória original entra em um estado lábil e suscetível a modificações, em que é possível enfraquecê-la através da inibição de sua reconsolidação. A reconsolidação da memória mostra-se uma estratégica mais eficaz e duradoura em relação à extinção, já que a memória original é modificada. Como modelo animal para o estudo da memória na dependência de drogas, o condicionamento de preferência por local (CPL) é bastante utilizado e sabe-se que é possível enfraquecer a preferência através do bloqueio da reconsolidação. Porém, são escassos os estudos que investigaram a existência da reconsolidação no modelo de sensibilização locomotora, que parece ocorrer, na maioria dos casos, em condição dependente do contexto de aquisição do comportamento, embora existam exemplos que demonstrem sua independência. As questões a serem respondidas neste trabalho são (a) se é possível reverter conjuntamente a preferência por local e a sensibilização locomotora à morfina (5 mg/kg) em ratos Wistar adultos machos, inibindo-se a síntese proteica com cicloheximida (CHX) i.p. logo após uma sessão de reativação contextual da memória no CPL, (b) se a reversão dos comportamentos reflete alterações (já descritas por outros autores) em GluA1, GluA1p (Ser845) e GluA2, no Hipocampo dorsal (HPCd) e no Núcleo Accumbens (NAc), e (c) se o mesmo tratamento em ambas estruturas reverte os dois parâmetros avaliados – comportamental e neuroquímico – de forma diferente ou igual. Nossos resultados mostraram ser possível reverter a preferência por local e a sensibilização locomotora por inibição sistêmica de síntese proteica, e que o condicionamento com exposição à morfina induz alterações nas subunidades analisadas de AMPA, conforme verificado no HPCd e NAc, embora a CHX não tenha produzido um efeito tão bem definido. Os animais que receberam infusões centrais no HPCd e NAc (central) não exibiram preferência por local, nem sensibilização. Em conjunto, nossos resultados mostraram, pela primeira vez em um mesmo desenho experimental, que é possível reverter diferentes aspectos da memória de recompensa (preferência e sensibilização) por meio do bloqueio da reconsolidação. / Drug addiction is a complex and multifactorial disorder that develops in a few people who use these substances. Associative memories between the drug and context of use act as a trigger for maladaptive behavior such as drug seeking and drug use, in addition to relapse after an extended period of withdrawal. Underlying these behavioral changes are modifications in glutamatergic reception (AMPA) in structures involved with memory (Hippocampus) and reward (Nucleus Accumbens). Therefore, strategies that weaken the drug and context association and deepen knowledge of circuits involved in these behaviors are extremely relevant therapeutically. When retrieved, a memory can undergo two distinct processes post-retrieval: extinction, in which a new memory inhibiting a previous association is generated, and reconsolidation, in which the original memory can enter a labile state and is susceptible to modifications, when it can be weakened by inhibition of its reconsolidation. Reconsolidation of memory has been shown to be a more effective and long lasting strategy in relation to extinction, since the original memory is modified. An animal model for studying drug addiction, conditioned place preference (CPP) is largely used and it is well known that it is possible to weaken preference by disrupting reconsolidation. However, there are few studies that investigate the existence of reconsolidation in a locomotor sensitization paradigm, which seems to occur in a condition dependent on context of acquisition, although some works report its independence. The questions answered in this work were (a) if it is possible to reverse both, context preference and locomotor sensitization to morphine (5mg/kg) by protein synthesis inhibition (CHX) after a contextual memory reactivation session in CPP, (b) if the disruption of behaviors reflects a reversal of changes of GluA1, GluA1p (Ser845) e GluA2 in dorsal Hippocampus (dHPC) and Nucleus Accumbens (NAc) and (c) if the same treatment in these structures differentially reverts the two parameters assessed. Our results indicate that it is possible to revert context preference and locomotor sensitization via systemic disruption of protein synthesis and that morphine conditioning induces changes in AMPA subunits in dHPC and NAc, although CHX did not have an evident effect on molecular reversal. Animals cannulated in dHPC and NAc core did not induce preference or sensitization. Taken together, our results demonstrated, for the first time, using the same experimental design that is possible to revert different aspects of reward memory (preference and sensitization) by disrupting the reconsolidation process.

Memória

Hipocampo

Núcleo accumbens

Locomoção

Morfina

Morphine

Conditioned place preference

Locomotor sensitization

Memory

Reconsolidation

Dorsal hippocampus

Nucleus accumbens

Cicloheximide

GluA1

GluA2

La mémoire hippocampo-dépendante : altérations dans un modèle de vieillissement accéléré et régulation par le système nociceptinergique chez la souris / Hippocampus-dependent memory : alteration in a model of accelerated aging and regulation by the nociceptinergic system in mice

Rekik, Khaoula

13 December 2017

La mémoire est définie comme une activité biologique et psychique qui permet d'emmagasiner, de conserver et restituer des informations. La formation de la mémoire à long terme a lieu en plusieurs étapes : acquisition, consolidation. Une fois consolidée, la mémoire peut être réactivée puis reconsolidée. C'est un processus dynamique qui au cours de la vie d'un individu peut subir des altérations physiologiques (vieillissement) ou pathologiques (maladies neurodégénératives, syndrome de stress post traumatique (PTSD)). Dans un premier temps nous avons caractérisé du point de vue comportemental les souris Werner (WRN), un modèle de vieillissement accéléré. Nos résultats ont montré que les souris WRN de différents âges (3, 5 et 8 mois) ne présentaient aucun problème moteur ni d'anxiété, deux paramètres altérés chez des souris âgées de 21 mois. Ces souris ne montrent pas non plus de déficit de mémoire non hippocampo-dépendante mais par contre présentent des déficits de mémoire hippocampo-dépendante. En termes d'intégrité fonctionnelle de l'hippocampe, les souris Werner sont capables de stocker l'information après un apprentissage mais à partir de 8 mois, elles présentent un déficit de flexibilité comportementale dans les tests de mémoire spatiale et contextuelle, un défaut caractéristique des animaux agés. Nos résultats montrent qu'au niveau comportemental, les souris WRN sont un bon modèle pour étudier le vieillissement car elles présentent dès 8 mois des déficits comparables à des souris normales âgées sans effets confondants liés à des troubles de la locomotion ou de l'anxiété. Dans un second temps nous avons évalué l'effet d'un système neuropeptidergique, le système nociceptine (peptide N/OFQ, récepteur NOP), sur la mémoire à long terme. Nous avons tout d'abord montré que différents agonistes du récepteur NOP inhibaient spécifiquement la reconsolidation de la mémoire aversive de type contextuelle dans le test du conditionnement de peur. Cet effet inhibiteur a également été observé dans un test hippocampo-dépendant non aversif, le test de localisation d'objet. Puisque l'activation des récepteurs NOP produit un effet amnésiant on peut émettre l'hypothèse que leur inhibition par des antagonistes pourrait favoriser l'apprentissage et la mémoire. Nos premiers résultats montrent en effet que l'injection d'un antagoniste NOP améliore les performances dans le test de localisation d'objet chez des souris Tg2576, modèles d'une forme familiale de la maladie d'Alzheimer. L'ensemble de ces résultats valident l'intérêt du système nociceptinergique en tant que cible thérapeutique pour atténuer les formes pathologiques de mémoire aversive comme dans le cas du PTSD ou au contraire améliorer les performances mnésiques chez les patients Alzheimer. / Memory can be defined as a biological and psychic activity that allows the acquisition, storage and retrieval of information. Long-term memory formation takes place in several stages: acquisition, consolidation. Once consolidated, the memory can be reactivated and then reconsolidated. Memory is a dynamic process that can undergo physiological (aging) or pathological alterations (neurodegenerative diseases, post-traumatic stress disorder (PTSD)) during the life of an individual. In a first step, we characterized the behavior of Werner mice (WRN), a model of accelerated aging. Our results showed that WRN mice of different ages (3, 5 and 8 months) showed no motor problems or anxiety, two parameters altered in 21-month-old mice. These mice also showed no non hippocampus-dependent memory deficit but showed hippocampus- dependent memory deficits. In terms of functional integrity of the hippocampus, Werner mice are able to store information after learning, but from 8 months onwards, they lack behavioral flexibility in spatial and contextual memory tests, a feature also observed in physiological aging. Our results show that at the behavioral level, WRN mice are a good model for studying aging because they show from 8 months deficits comparable to normal elderly mice without confounding effects related to locomotion or anxiety. Secondly, we evaluated the effect of a neuropeptidergic system, the nociceptin system (N/OFQ peptide, NOP receptor) on long-term memory. We first showed that differentagonists of the NOP receptor inhibit the reconsolidation of aversive memory in the fear conditioning paradigm.. This inhibitory effect was also observed in a non- aversive hippocampus-dependent task, the object location test. Since activation of NOP receptors produces an amnestic effect, it can be hypothesized that their inhibition by antagonists could promote learning and memory. Indeed, our first results show that the injection of a NOP antagonist improves the performance in the object location test in Tg2576 mice, a model of familial Alzheimer's disease. All these results validate the interest of the nociceptinergic system as a therapeutic target to attenuate pathological forms of aversive memory as in the case of PTSD, or on the contrary improve memory performance in Alzheimer patients.

Vieillissement

Souris Werner

Mémoire hippocampo-dépendante

Reconsolidation de la mémoire

Nociceptine/orphanine FQ

Trouble de stress post traumatique

Maladie d'Alzheimer

Aging

Werner mice

Hippocampus-dependent memory

Non-hippocampus-dependent memory

Le blocage de la reconsolidation des souvenirs, une avenue possible pour le traitement du trouble de stress post-traumatique?

Poundja, Joaquin

06 1900

La présente thèse porte sur l’évaluation de l’efficacité d’un nouveau traitement pour le trouble de stress post-traumatique (TSPT). Le traitement a été développé selon les prémisses de la théorie de la reconsolidation des souvenirs. Il consiste en six courtes séances de remémoration de l’événement traumatique réalisées sous l’effet du propranolol, un bêtabloquant. La population de l’étude est constituée de patients souffrant d’un TSPT chronique. La thèse comporte cinq chapitres. Le premier chapitre est l’introduction, on y retrouve une description du TSPT, des traitements validés empiriquement, de diverses théories de la mémoire, d’un modèle étiologique du TSPT, d’études sur la consolidation et la reconsolidation, de la pharmacocinétique et du mécanisme d’action du propranolol,ainsi que des objectifs de la thèse. Le second chapitre est une revue critique de littérature sur la théorie de la reconsolidation. Comme l’étude du phénomène de la reconsolidation est récente, nous tentons de faire le point sur l’état des connaissances dans le domaine, dans un effort de réflexion sur la validité de la théorie. Nous proposons une série de critères permettant de différencier la reconsolidation d’autres processus connexes. Nous concluons que la théorie paraît valide, bien que d’autres études soient nécessaires afin de rendre compte de résultats négatifs publiés par le passé. Le troisième chapitre est un essai ouvert, et vise à évaluer l’efficacité d’un traitement basé sur la reconsolidation à diminuer la sévérité et l’incidence du TSPT, auprès de 42 patients souffrant d’un TSPT chronique. Le traitement consiste en six séances de remémoration de l’événement traumatique sous propranolol. Lors d’un suivi à trois mois, nous rapportons une diminution des symptômes de TSPT de 41%-56%, ainsi qu’une diminution de l’incidence du TSPT de 74%. En comparaison, seulement 2/25 patients du groupe contrôle (ayant participé uniquement aux évaluations) ne souffrent plus d’un TSPT. Dans le groupe traitement, les tailles d’effet (d de Cohen)varient entre 1.32-2.19. Le quatrième chapitre a comme objectif d’identifier des caractéristiques des patients prédisant l’efficacité du traitement, et d’explorer s’ils s’améliorent dans des domaines de santé autres que le TSPT. Nous rapportons que les femmes s’améliorent davantage que les hommes, mais que d’autres facteurs, tels que la sévérité des traits de personnalité borderline ou le type de trauma (enfance versus adulte), n’influent pas sur l’efficacité. Également, les patients s’améliorent dans les domaines de santé suivants : la qualité de vie, la symptomatologie dépressive, l’intensité des émotions négatives au rappel de l’événement traumatique et dans la vie courante. Le cinquième chapitre contient la discussion générale de la thèse. Nous effectuons une synthèse et interprétation des résultats, nous examinons les hypothèses alternatives à l’amélioration clinique et abordons des pistes de recherches futures. Nous concluons que le traitement à l’étude a été efficace dans notre échantillon de patients souffrant d’un TSPT chronique. Étant donné la méthodologie employée (essai ouvert), nous ne pouvons statuer sur le mécanisme d’action du traitement, à savoir si l’amélioration clinique a été réellement causée par un blocage de la reconsolidation des souvenirs. / This dissertation aims at exploring the efficacy of a new treatment for posttraumatic stress disorder (PTSD). The treatment was developed in accordance with an emerging theory in neuroscience, the reconsolidation theory, and it consists in six short reactivation sessions of a traumatic memory under the influence of propranolol (a ß-blocker), with patients suffering from longstanding PTSD. This dissertation includes five chapters. Chapter I is the introduction, it includes a discussion on the following topics : definition and prevalence of PTSD,empirically validated treatments in the field, memory theories, etiology of PTSD, studies on consolidation and reconsolidation, pharmacokinetics of propranolol and its mechanism of action in reconsolidation, and the objectives of the dissertation. Chapter II is a critical literature review on reconsolidation theory. We discuss some of the contradicting findings in reconsolidation, as some researchers have reported negative results in the field. We address the possibility to reconcile these discrepancies,within the scope of evaluating the validity of the theory. We also discuss a series of criterion which could provide guidance in differentiating reconsolidation from other processes. We conclude that reconsolidation theory seems valid, although more research is needed in order to shed light on some negative results that were published in the past. Chapter III is an open label trial comprising six sessions of treatment (trauma reactivation under propranolol) with 42 patients suffering from chronic PTSD. At a three-month follow-up, we report that patients have a 41% - 56% reduction in PTSD symptoms, and that 31 / 42 patients no longer meet the diagnostic threshold for PTSD. In comparison, only 2 / 25 patients from the control group (assessments only) don’t meet the diagnostic threshold for PTSD. In the treatment group, effect sizes (Cohen’s d) range between 1.32 -2.19. Chapter IV follows on the previous chapter’s study, and aims at identifying predictors of treatment outcome (i.e., predictors of the improvement in PTSD symptoms), and whether patients also improve in health domains other than PTSD. We report that women improve more than men during the treatment, but that other factors such as borderline personality severity traits or type of trauma (childhood versus adulthood) do not influence treatment outcome. Patients also improve in diverse health domains during the treatment; they have a better quality of life, less depressive symptoms, less intense negative emotions in daily life and during trauma recollection. Chapter V contains a general discussion and a conclusion. We summarize and interpret the results, we explore alternative hypotheses to the clinical improvement as well as future research directions. We conclude that this treatment yielded interesting results in our sample of patients suffering from chronic PTSD. However, our methodology (open label study) doesn’t provide any information on the mechanism of action of the treatment used in this dissertation, i.e. whether the clinical improvement was caused or not by reconsolidation blockade.

Trouble de stress post-traumatique

Traitements

Reconsolidation

Mémoire

Propranolol

Effets du sexe

Extinction

Exposition

Posttraumatic stress disorder

Treatments

Memory

Gender effects

Exposure

Temporal variability of soil hydraulic properties under different soil management practices

Gill, Shahid Maqsood

20 December 2012

Agricultural management practices including tillage and irrigation have a considerable effect on soil physical and hydraulic properties in space and time. Tillage practices initially alter the soil physical and hydraulic properties depending on the type and depth of tillage. These changes are reverted back to original conditions due to reconsolidation during cycles of wetting and drying. Irrigation techniques can manipulate the reversion process dynamically due to different modes of wetting. The combined effects of tillage and irrigation have rarely been investigated. Therefore, two experiments were conducted to investigate the effect of different tillage practices and irrigation techniques on soil physical properties and temporal variations in soil hydraulic properties, one on wheat and second on the following maize crop grown on the same plots. The tillage and irrigation treatments implemented for the wheat crop were repeated for the subsequent maize crop restoring the same treatment layout plan. Intact soil core samples were collected, in the middle of the wheat crop before irrigation and the end of the maize crop season, for the determination of soil physical and hydraulic properties. Field saturated hydraulic conductivity (K_fs) was determined using the Guelph pressure infiltrometer method and volumetric soil water content (θ_v) and potential (ψ_m) was measured in the field using water content sensors and tensiometers, respectively. The wheat crop received rain showers from time to time, while in maize, a heavy spell of monsoon rains following tillage caused most of the soil reconsolidation. So, the greater intensity of rains, rather than the cycles of wetting and drying, became primarily responsible for the differences in soil physical and hydraulic properties between the two crops. Moldboard plow resulted in an increase in yield and improvement of soil hydraulic properties during both crop seasons. Flood irrigation reverted back the effects of tillage on soil hydraulic properties greater than sprinkler irrigation, while it did not affect the yield significantly. The dynamics of volumetric soil water content (θ_v) differed, depending on tillage type, irrigation technique and crop season. Moldboard plow was the wettest after rain or irrigation events but it dried quicker than other tillage treatments. Flood irrigation caused higher wetting than sprinkler irrigation. These wetting effects were greater in wheat as compared to maize crop. Temporal variability calculated as time averaged relative difference in θ_v was greater during wheat as compared to maize, while temporal stability calculated as standard deviation of temporal stability decreased with flood irrigation in both crops. Soil bulk density (ρ_b) and water retention characteristics (θ_v (ψ_m )) measured on the intact soil cores and total porosity (φ), plant available water capacity (θ_PAWC) and pore size distribution calculated from water retention data depended on the time of sampling. During wheat, the ρ_b was lower resulting in a higher φ than after maize. Moldboard plow decreased ρ_b increasing φ, while the effect of flood irrigation was opposite in both crops with greater magnitude in wheat. Similarly, the effects of tillage on θ_v (ψ_m ) were observed in both crops, while those of irrigation were observed in maize only. Cultivator treatment retained higher θ_v at higher ψ_m (−30 and −100 kPa), followed by chisel and moldboard plow. Plant available water capacity (θ_PAWC) was greater in maize as compared to the wheat crop. Cultivator had higher θ_PAWC than chisel and moldboard plow in both crops. Wheat had greater volume of larger pores (> 10 μm, φ_(>10)), whereas extraordinary rains as well as irrigations after tillage caused these larger pores to decrease in maize. Moldboard plow had higher φ_(>10) at 10 cm depth in both crops with greater magnitude in wheat. Field saturated hydraulic conductivity (K_fs) determined before irrigations and at the end of both crop seasons was greater in wheat than in maize especially in the first determination. Moldboard plow exhibited greater K_fs followed by chisel plow and cultivator in both crops and it decreased significantly with time in wheat but not in maize. Flood irrigation was responsible for a reduction in K_fs and the effect was greater in wheat as compared to maize. It was concluded that a greater intensity of water application in the form of rains or irrigations can revert the changes in soil physical and hydraulic properties induced by tillage more effectively than the cycles of wetting and drying. Soil hydraulic properties may be optimized with the combination of suitable tillage and irrigation for efficient utilization of water resources.

Reversão dos efeitos reforçadores da morfina através do prejuízo da reconsolidação da memória do condicionamento de preferência por local e da sensibilização locomotora

Boos, Flávia Zacouteguy

January 2016

A dependência de drogas é um transtorno multifatorial complexo que se desenvolve em uma minoria de indivíduos que fazem uso dessas substâncias. Memórias associativas entre a droga e o contexto funcionam como gatilho para disparar comportamentos não adaptativos de busca e consumo, além de recaídas após períodos de abstinência. Subjacentes a essas mudanças comportamentais, existem modificações nas subunidades de receptores glutamatérgicos do tipo AMPA em estruturas envolvidas com memória (Hipocampo) e recompensa (Núcleo Accumbens). Por isso, estratégias que enfraqueçam a associação do contexto com a droga e que aprofundem o conhecimento dos circuitos envolvidos nesses comportamentos são de extrema relevância terapêutica. A memória quando evocada pode passar por dois processos pós-evocação: a extinção, em que uma nova memória é formada inibindo uma prévia associação, e a reconsolidação, em que a memória original entra em um estado lábil e suscetível a modificações, em que é possível enfraquecê-la através da inibição de sua reconsolidação. A reconsolidação da memória mostra-se uma estratégica mais eficaz e duradoura em relação à extinção, já que a memória original é modificada. Como modelo animal para o estudo da memória na dependência de drogas, o condicionamento de preferência por local (CPL) é bastante utilizado e sabe-se que é possível enfraquecer a preferência através do bloqueio da reconsolidação. Porém, são escassos os estudos que investigaram a existência da reconsolidação no modelo de sensibilização locomotora, que parece ocorrer, na maioria dos casos, em condição dependente do contexto de aquisição do comportamento, embora existam exemplos que demonstrem sua independência. As questões a serem respondidas neste trabalho são (a) se é possível reverter conjuntamente a preferência por local e a sensibilização locomotora à morfina (5 mg/kg) em ratos Wistar adultos machos, inibindo-se a síntese proteica com cicloheximida (CHX) i.p. logo após uma sessão de reativação contextual da memória no CPL, (b) se a reversão dos comportamentos reflete alterações (já descritas por outros autores) em GluA1, GluA1p (Ser845) e GluA2, no Hipocampo dorsal (HPCd) e no Núcleo Accumbens (NAc), e (c) se o mesmo tratamento em ambas estruturas reverte os dois parâmetros avaliados – comportamental e neuroquímico – de forma diferente ou igual. Nossos resultados mostraram ser possível reverter a preferência por local e a sensibilização locomotora por inibição sistêmica de síntese proteica, e que o condicionamento com exposição à morfina induz alterações nas subunidades analisadas de AMPA, conforme verificado no HPCd e NAc, embora a CHX não tenha produzido um efeito tão bem definido. Os animais que receberam infusões centrais no HPCd e NAc (central) não exibiram preferência por local, nem sensibilização. Em conjunto, nossos resultados mostraram, pela primeira vez em um mesmo desenho experimental, que é possível reverter diferentes aspectos da memória de recompensa (preferência e sensibilização) por meio do bloqueio da reconsolidação. / Drug addiction is a complex and multifactorial disorder that develops in a few people who use these substances. Associative memories between the drug and context of use act as a trigger for maladaptive behavior such as drug seeking and drug use, in addition to relapse after an extended period of withdrawal. Underlying these behavioral changes are modifications in glutamatergic reception (AMPA) in structures involved with memory (Hippocampus) and reward (Nucleus Accumbens). Therefore, strategies that weaken the drug and context association and deepen knowledge of circuits involved in these behaviors are extremely relevant therapeutically. When retrieved, a memory can undergo two distinct processes post-retrieval: extinction, in which a new memory inhibiting a previous association is generated, and reconsolidation, in which the original memory can enter a labile state and is susceptible to modifications, when it can be weakened by inhibition of its reconsolidation. Reconsolidation of memory has been shown to be a more effective and long lasting strategy in relation to extinction, since the original memory is modified. An animal model for studying drug addiction, conditioned place preference (CPP) is largely used and it is well known that it is possible to weaken preference by disrupting reconsolidation. However, there are few studies that investigate the existence of reconsolidation in a locomotor sensitization paradigm, which seems to occur in a condition dependent on context of acquisition, although some works report its independence. The questions answered in this work were (a) if it is possible to reverse both, context preference and locomotor sensitization to morphine (5mg/kg) by protein synthesis inhibition (CHX) after a contextual memory reactivation session in CPP, (b) if the disruption of behaviors reflects a reversal of changes of GluA1, GluA1p (Ser845) e GluA2 in dorsal Hippocampus (dHPC) and Nucleus Accumbens (NAc) and (c) if the same treatment in these structures differentially reverts the two parameters assessed. Our results indicate that it is possible to revert context preference and locomotor sensitization via systemic disruption of protein synthesis and that morphine conditioning induces changes in AMPA subunits in dHPC and NAc, although CHX did not have an evident effect on molecular reversal. Animals cannulated in dHPC and NAc core did not induce preference or sensitization. Taken together, our results demonstrated, for the first time, using the same experimental design that is possible to revert different aspects of reward memory (preference and sensitization) by disrupting the reconsolidation process.

Memória

Hipocampo

Núcleo accumbens

Locomoção

Morfina

Morphine

Conditioned place preference

Locomotor sensitization

Memory

Reconsolidation

Dorsal hippocampus

Nucleus accumbens

Cicloheximide

GluA1

GluA2

A MELHORA DA RECONSOLIDAÇÃO DA MEMÓRIA INDUZIDA POR ESPERMIDINA ENVOLVE A PROTEÍNA CINASE DEPENDENTE DE CÁLCIO / SPERMIDINE-INDUCED IMPROVEMENT OF RECONSOLIDATION OF MEMORY INVOLVES CALCIUM-DEPENDENT PROTEIN KINASE

Girardi, Bruna Amanda

21 July 2015

Coordenação de Aperfeiçoamento de Pessoal de Nível Superior / The reactivation of a memory results in its destabilization, requiring a process of memory reconsolidation to maintain it. Spermidine is an endogenous aliphatic amine with polycationic structure that modulates N-methyl-D-aspartate (NMDA) receptor activity and improves memory. Recent evidence suggests that systemic administration of spermidine improves the reconsolidation of fear memory. Here we determined whether the calcium-dependent protein kinase (PKC) signaling pathway is involved in the improvement of fear memory reconsolidation induced by intrahippocampal (ih) administration of spermidine in rats. Male Wistar rats were trained in a fear conditioning apparatus using a 0.4 mA footshock as unconditioned stimulus. Twenty-four hours after training, animals were re-exposed to the apparatus in the absence of shock (reactivation session). Immediately after the reactivation session, spermidine (2-200 ρmol/site); the PKC inhibitor, 3-[1- (dimethylaminopropyl)indol-3-yl]-4-(indol-3-yl) maleimide hydrochloride (GF 109203X, 0.3 - 30 ρg/site); the antagonist of the polyamine-binding site at the NMDA receptor, arcaine (0.2 - 200 ρmol/site) or the PKC activator, phorbol 12-myristate 13-acetate (PMA, 0.02 - 2 nmol/site) were injected intra-hipocampally (i.h.). Testing was carried out in the same apparatus, twenty-four hours after reactivation. Freezing scores at testing were considered a measure of memory. While the post-reactivation administration of spermidine (20 and 200 ρmol/site) improved, GF 109203X (1, 10 and 30 ρg/site) impaired memory reconsolidation. GF 109203X (0.3 ρg/site) prevented spermidine (200 ρmol/site)-induced improvement of memory reconsolidation. The post-reactivation administration of arcaine (200 pmol/site) impaired and PMA (2 nmol/site) improved memory reconsolidation. PMA (0.2 nmol/site) prevented arcaine (200 ρmol/site)-induced impairment of memory reconsolidation. The protein synthesis inhibitor anisomycin (2 μg/site) prevented spermidine (200 ρmol/site)-induced improvement of memory reconsolidation. These drugs had no effect on memory if they were administered in the absence of reactivation. These results suggest that the enhancement of memory reconsolidation induced by the administration of spermidine involves PKC activation. / A reativação de uma memória resulta na sua desestabilização, que exigem um processo de reconsolidação de memória para mantê-la. A espermidina é uma amina alifática endógena com estrutura policatiônica que modula a atividade do receptor Nmetil- D-aspartato (NMDA) e melhora a memória. Evidências recentes sugerem que a administração sistêmica de espermidina melhora a reconsolidação da memória de medo. No entanto não se sabe se a administração intra hipocampal de espermidina melhora a reconsolidação da memória e nem se a proteína cinase dependente de cálcio (PKC) e síntese proteica estão envolvidas neste efeito. Portanto, no presente estudo verificou-se o envolvimento da PKC e da síntese proteica na melhora da reconsolidação da memória do medo induzida pela administração intrahipocampal (ih) de espermidina em ratos. Ratos Wistar machos foram treinados na tarefa de medo condicionado contextual utilizando-se choque de 0,4 mA como estímulo incondicionado. Vinte e quatro horas após o treino, os animais foram re-expostos ao aparelho na ausência de choque (sessão reativação). Imediatamente após a sessão de reativação foram administradas, por via ih, espermidina (2-200 ρmol/sítio); o inibidor da PKC, 3- [1- (dimetilaminopropil) indol-3-il] -4- (indol-3-il) maleimida (GF 109203X, 0,3-30 ρg/sítio); o antagonista do sítio de ligação das poliaminas no receptor de NMDA, arcaína (0,2-200 ρmol/sítio) ou o ativador de PKC, 12-miristato 13-acetato de forbol (PMA, 0,02-2 nmol/sítio). Os testes foram realizados no mesmo aparelho, 24 horas após a sessão de reativação. O tempo de imobilidade dos animais durante o teste foi considerado como medida de memória. Enquanto a administração de espermidina (20 e 200 ρmol/sítio) melhorou, GF 109203X (1, 10 e 30 ρg/sítio) prejudicou a reconsolidação da memória. O GF 109203X (0,3 ρg/sítio) preveniu a melhora da reconsolidação da memória induzida por espermidina (200 ρmol/sítio). A administração da arcaína (200 pmol/sítio) prejudicou e PMA (2 nmol/sítio) melhorou a reconsolidação da memória. O PMA (0,2 nmol/sítio) preveniu o prejuízo na reconsolidação da memória induzido por arcaína (200 ρmol/sítio). O inibidor de síntese de proteica, anisomicina (2 ug/sítio) preveniu a melhora da reconsolidação da memória induzida por espermidina (200 ρmol/sítio). Estas drogas não tiveram nenhum efeito sobre a memória quando foram administrados na ausência da sessão de reativação. Estes resultados sugerem que a melhora da reconsolidação da memória induzida pela administração ih de espermidina envolve a síntese proteica e a ativação de PKC.

Poliaminas

Hipocampo

Reconsolidação da memória

Proteína cinase C

Medo condicionado contextual

Polyamines

Hippocampus

Memory reconsolidation

Protein kinase C

Contextual fear conditioning

CNPQ::CIENCIAS BIOLOGICAS::FARMACOLOGIA

Reversão dos efeitos reforçadores da morfina através do prejuízo da reconsolidação da memória do condicionamento de preferência por local e da sensibilização locomotora

Boos, Flávia Zacouteguy

January 2016

A dependência de drogas é um transtorno multifatorial complexo que se desenvolve em uma minoria de indivíduos que fazem uso dessas substâncias. Memórias associativas entre a droga e o contexto funcionam como gatilho para disparar comportamentos não adaptativos de busca e consumo, além de recaídas após períodos de abstinência. Subjacentes a essas mudanças comportamentais, existem modificações nas subunidades de receptores glutamatérgicos do tipo AMPA em estruturas envolvidas com memória (Hipocampo) e recompensa (Núcleo Accumbens). Por isso, estratégias que enfraqueçam a associação do contexto com a droga e que aprofundem o conhecimento dos circuitos envolvidos nesses comportamentos são de extrema relevância terapêutica. A memória quando evocada pode passar por dois processos pós-evocação: a extinção, em que uma nova memória é formada inibindo uma prévia associação, e a reconsolidação, em que a memória original entra em um estado lábil e suscetível a modificações, em que é possível enfraquecê-la através da inibição de sua reconsolidação. A reconsolidação da memória mostra-se uma estratégica mais eficaz e duradoura em relação à extinção, já que a memória original é modificada. Como modelo animal para o estudo da memória na dependência de drogas, o condicionamento de preferência por local (CPL) é bastante utilizado e sabe-se que é possível enfraquecer a preferência através do bloqueio da reconsolidação. Porém, são escassos os estudos que investigaram a existência da reconsolidação no modelo de sensibilização locomotora, que parece ocorrer, na maioria dos casos, em condição dependente do contexto de aquisição do comportamento, embora existam exemplos que demonstrem sua independência. As questões a serem respondidas neste trabalho são (a) se é possível reverter conjuntamente a preferência por local e a sensibilização locomotora à morfina (5 mg/kg) em ratos Wistar adultos machos, inibindo-se a síntese proteica com cicloheximida (CHX) i.p. logo após uma sessão de reativação contextual da memória no CPL, (b) se a reversão dos comportamentos reflete alterações (já descritas por outros autores) em GluA1, GluA1p (Ser845) e GluA2, no Hipocampo dorsal (HPCd) e no Núcleo Accumbens (NAc), e (c) se o mesmo tratamento em ambas estruturas reverte os dois parâmetros avaliados – comportamental e neuroquímico – de forma diferente ou igual. Nossos resultados mostraram ser possível reverter a preferência por local e a sensibilização locomotora por inibição sistêmica de síntese proteica, e que o condicionamento com exposição à morfina induz alterações nas subunidades analisadas de AMPA, conforme verificado no HPCd e NAc, embora a CHX não tenha produzido um efeito tão bem definido. Os animais que receberam infusões centrais no HPCd e NAc (central) não exibiram preferência por local, nem sensibilização. Em conjunto, nossos resultados mostraram, pela primeira vez em um mesmo desenho experimental, que é possível reverter diferentes aspectos da memória de recompensa (preferência e sensibilização) por meio do bloqueio da reconsolidação. / Drug addiction is a complex and multifactorial disorder that develops in a few people who use these substances. Associative memories between the drug and context of use act as a trigger for maladaptive behavior such as drug seeking and drug use, in addition to relapse after an extended period of withdrawal. Underlying these behavioral changes are modifications in glutamatergic reception (AMPA) in structures involved with memory (Hippocampus) and reward (Nucleus Accumbens). Therefore, strategies that weaken the drug and context association and deepen knowledge of circuits involved in these behaviors are extremely relevant therapeutically. When retrieved, a memory can undergo two distinct processes post-retrieval: extinction, in which a new memory inhibiting a previous association is generated, and reconsolidation, in which the original memory can enter a labile state and is susceptible to modifications, when it can be weakened by inhibition of its reconsolidation. Reconsolidation of memory has been shown to be a more effective and long lasting strategy in relation to extinction, since the original memory is modified. An animal model for studying drug addiction, conditioned place preference (CPP) is largely used and it is well known that it is possible to weaken preference by disrupting reconsolidation. However, there are few studies that investigate the existence of reconsolidation in a locomotor sensitization paradigm, which seems to occur in a condition dependent on context of acquisition, although some works report its independence. The questions answered in this work were (a) if it is possible to reverse both, context preference and locomotor sensitization to morphine (5mg/kg) by protein synthesis inhibition (CHX) after a contextual memory reactivation session in CPP, (b) if the disruption of behaviors reflects a reversal of changes of GluA1, GluA1p (Ser845) e GluA2 in dorsal Hippocampus (dHPC) and Nucleus Accumbens (NAc) and (c) if the same treatment in these structures differentially reverts the two parameters assessed. Our results indicate that it is possible to revert context preference and locomotor sensitization via systemic disruption of protein synthesis and that morphine conditioning induces changes in AMPA subunits in dHPC and NAc, although CHX did not have an evident effect on molecular reversal. Animals cannulated in dHPC and NAc core did not induce preference or sensitization. Taken together, our results demonstrated, for the first time, using the same experimental design that is possible to revert different aspects of reward memory (preference and sensitization) by disrupting the reconsolidation process.

Memória

Hipocampo

Núcleo accumbens

Locomoção

Morfina

Morphine

Conditioned place preference

Locomotor sensitization

Memory

Reconsolidation

Dorsal hippocampus

Nucleus accumbens

Cicloheximide

GluA1

GluA2

AGENTES POLIAMINÉRGICOS MODULAM A RECONSOLIDAÇÃO DA MEMÓRIA DE MEDO EM RATOS / POLYAMINERGIC AGENTS MODULATE THE FEAR MEMORY RECONSOLIDATION IN RATS

Ribeiro, Daniela Aymone

19 August 2013

Coordenação de Aperfeiçoamento de Pessoal de Nível Superior / The memory may be studied according with memory's phases, which is acquisition, consolidation and recall. Memories once consolidated, are no more susceptible to interventions, but when reactivated, some of these memories again become labile and vulnerable, and to persist need to have a new stabilization process called reconsolidation. Previous studies described that endogenous polyamines, spermine and spermidine, which bind and modulate the activity of NMDA receptors are involved in memory acquisition and consolidation. However there are no studies showing the effect of these drugs on memory reconsolidation. Accordingly, the aim of this study was investigate the effect of polyamines on fear memory reconsolidation in rats. Male Wistar rats were trained in a fear conditioning apparatus using a 0.4 mA footshock as unconditioned stimulus. Twenty four hours after training, animals were re-exposed to the apparatus in the absence of shock (reactivation session). Immediately after the reactivation session, SPD (1 30 mg/kg, i.p.), the antagonist of the polyamine binding site at the NMDA receptor, arcaine (0.1 10 mg/kg, i.p.) or spermidine plus arcaine were injected, and the animals were tested in the same apparatus 24 h later. Freezing scores at testing were considered a measure of memory. While SPD (3 and 10 mg/kg) improved, arcaine (1 and 10 mg/kg) impaired memory reconsolidation. These drugs had no effect on memory if they were administered in the absence of reactivation, or 6 h after reactivation session. Arcaine (0.1 mg/kg, i.p.) prevented SPD (3 mg/kg)-induced improvement of memory reconsolidation. Accordingly, SPD (1 mg/kg) prevented arcaine (10 mg/kg)-induced impairment of memory reconsolidation. The amnesic effect of arcaine was not reversed by arcaine administration prior to test, ruling out state dependence in this effect. These results suggest that systemic administration of polyamine binding site ligands modulate memory reconsolidation, however further studies are required to elucidate the mechanism by which polyamines modulate memory reconsolidation. / A memória pode ser estudada de acordo com as suas fases, que são a aquisição, a consolidação e a evocação. As memórias, uma vez consolidadas, não podem mais ser modificadas, porém quando reativadas, ou seja, quando recuperadas, muitas destas voltam a se tornar instáveis e vulneráveis e para que persistam precisam passar por um novo processo de estabilização, chamado reconsolidação. Têm sido descrito que as poliaminas endógenas, espermidina e espermina, que se ligam e modulam a atividade do receptor NMDA, estão envolvidas na aquisição e na consolidação da memória. Contudo, não há trabalhos mostrando o efeito destas substâncias na reconsolidação da memória. Desta forma, o objetivo deste estudo foi verificar o efeito das poliaminas na reconsolidação da memória de medo em ratos. Para isso, ratos machos adultos foram treinados na tarefa de medo condicionado contextual, onde receberam três choque de 0,4 mA, com intervalo de 40 seg entre cada choque e, 24 horas após, os animais foram recolocados no aparelho do treino por um período de 3 min, na ausência de choque, para reativar a memória. Após a reativação foi administrado, pela via intraperitoneal, salina, espermidina (1-30 mg/kg), arcaína (0,1-10 mg/kg) ou espermidina mais arcaína e vinte e quatro horas após, os animais foram testados, onde foi avaliado a imobilidade destes durante 6 min. Foram realizados experimentos controles para avaliar a especificidade das drogas no processo de reconsolidação. Além disso, foi avaliado se o possível efeito da arcaína na reconsolidação poderia ser explicado por dependência de estado. Assim, enquanto a espermidina (3 e 10 mg/kg) melhorou, a arcaína (1 e 10 mg/kg) piorou a reconsolidação da memória. Estas drogas não tiveram efeito sobre a memória quando foram administradas na ausência da reativação ou 6 horas após. A arcaína (0,1 mg/kg) preveniu a melhora da reconsolidação da memória induzida pela espermidina (3 mg/kg) e por sua vez, a espermidina (1 mg/kg) preveniu o prejuízo da reconsolidação da memória induzido pela arcaína (10 mg/kg). O efeito amnésico da arcaína não foi revertido pela administração da mesma dose de arcaína antes do teste, descartando a hipótese de dependência de estado para o efeito da arcaína na reconsolidação. Estes resultados sugerem que a administração sistêmica dos ligantes do sítio de ligação das poliaminas do receptor NMDA modulam a reconsolidação da memória, todavia são necessários mais estudos a fim de elucidar o mecanismo pelo qual as poliaminas modulam a reconsolidação da memória.

Memória

Reconsolidação

Receptor NMDA

Espermidina

Arcaína

Medo condicionado contextual

Memory

Reconsolidation

NMDA receptor

Spermidine

Arcaine

Contextual fear conditioning

CNPQ::CIENCIAS BIOLOGICAS::BIOQUIMICA

Delayed Versus Immediate Corrective Feedback on Orally Produced Passive Errors in English

Quinn, Paul

21 August 2014

Research demonstrating the beneficial effects of corrective feedback (CF) for second language (L2) learning (e,g., Li, 2010) has almost invariably resulted from studies in which CF was provided immediately. Yet teachers are often encouraged to delay CF to avoid interrupting learners (Harmer, 2001). This study investigates how differences in the timing of CF on oral production affect L2 learning and learners’ reactions to CF. Theoretically, Immediate CF may facilitate L2 development by allowing learners to immediately compare their errors to accurate models (i.e., recasting, e.g., Doughty, 2001). The effectiveness of Immediate CF has also been linked to skill acquisition theory because some CF (i.e., prompting) is hypothesized to help learners proceduralize their L2 knowledge (Ranta & Lyster, 2007). This thesis introduces additional theoretical explanations to explain the effectiveness of both Immediate and Delayed CF. For example, reactivation and reconsolidation theory (Nader & Einarsson, 2010) holds that long-term mental representations are susceptible to change when they are recalled. Thus, both Immediate and Delayed CF may help learners alter their incorrect mental representations of language features if that CF reminds learners of those incorrect representations and provides them with accurate models. In a laboratory-based study, 90 intermediate-level adult ESL learners were randomly assigned to Immediate, Delayed, and No CF conditions. Learners took three pre-tests to measure their knowledge of the English passive construction: an aural grammaticality judgment test (AGJT), an oral production test (OPT), and a written error correction test (ECT). Next, they received some brief instruction on the passive. Learners then completed three communicative tasks in which the CF conditions were provided. These tasks were followed by immediate and delayed post-tests. Learners’ reactions to CF were elicited with a questionnaire. Mixed-design one-way ANOVAs revealed statistically significant improvement for all conditions over time on all measures, but no statistically significant differences between conditions. The questionnaires revealed that learners prefer Immediate CF, but that Immediate CF may constrain CF noticeability and learners’ independence, while Delayed CF may cause anxiety or embarrassment. In summary, altering the timing of CF did not differentially affect L2 development, but it did elicit different reactions from learners.

timing of corrective feedback

corrective feedback

error correction

second language acquisition

timing of instruction

form-focused instruction

second language learning

second language pedagogy

cognitive aspects of language learning

ESL

English as a second language

second language teaching

English passive voice

L2 learning

L2 teaching

types of corrective feedback

correction

reactivation and reconsolidation

cognitive comparison

skill acquisition

proceduralization

delayed corrective feedback

immediate corrective feedback

second language education

SLA

0290