DIFFERENTIAL SKELETAL MUSCLE ENERGY EXPENDITURE IN LEAN VS. OBESITY-PRONE RATS

Gavini, Chaitanya Kumar

07 October 2015

No description available.

Biology

Biomedical Research

Cellular Biology

Molecular Biology

Neurosciences

Physiology

Ventromedial Hypothalamus

Skeletal Muscle

Non-exercise activity thermogenesis

Melanocortins

DYNAMIC CILIARY LOCALIZATION IN THE MOUSE BRAIN

Katlyn M Brewer (18308818)

03 June 2024

<p dir="ltr">Primary cilia are hair-like structures found on nearly all mammalian cell types, including cells in the developing and adult brain. Cilia establish a unique signaling compartment for cells. For example, a diverse set of receptors and signaling proteins localize within cilia to regulate many physiological and developmental pathways including the Hh pathway. Defects in cilia structure, protein localization, or cilia function lead to genetic disorders called ciliopathies, which present with various clinical features including several neurodevelopmental phenotypes and hyperphagia associated obesity. Despite their dysfunction being implicated in several disease states, understanding their roles in CNS development and signaling has proven challenging. I hypothesize that dynamic changes to ciliary protein composition contributes to this challenge and may reflect unrecognized diversity of CNS cilia. The proteins ARL13B and ADCY3 are established ciliary proteins in the brain and assessing their localization is often used in the field to visualize cilia. ARL13B is a regulatory GTPase important for regulating cilia structure, protein trafficking, and Hh signaling, while ADCY3 is a ciliary adenylyl cyclase thought to be involved in ciliary GPCR singaling. Here, I examine the ciliary localization of ARL13B and ADCY3 in the perinatal and adult mouse brain by defining changes in the proportion of cilia enriched for ARL13B and ADCY3 depending on brain region and age. Furthermore, I identify distinct lengths of cilia within specific brain regions of male and female mice. As mice age, ARL13B cilia become relatively rare in many brain regions, including the hypothalamic feeding centers, while ADCY3 becomes a prominent cilia marker. It is important to understand the endogenous localization patterns of these proteins throughout development and under different physiological conditions as these common cilia markers may be more dynamic than initially expected. Understanding regional and development associated cilia signatures and physiological condition cilia dynamic changes in the CNS may reveal molecular mechanisms associated with ciliopathy clinical features such as obesity.</p>

Cell metabolism

Neurogenetics

Vertebrate biology

ARL13B

Primary cilia

ADCY3

Hypothalamus

Energy Homeostasis

Nucleus Accumbens

Primary Cilia

Ciliary Protein Localization

Postnatal Development

CNS

Molekulare Charakterisierung an der hypothalamischen Appetitregulation beteiligter Rezeptoren

Tarnow, Patrick

06 January 2009

Das Körpergewicht und die Nahrungsaufnahme werden unter anderem vom Hypothalamus reguliert. Dort werden Hormonelle Signale der Peripherie und neuronale Signale integriert. Die G-Protein gekoppelten Melanocortinrezeptoren 3 und 4 (MC3R und MC4R) werden von ihren Agonisten, den Melanocortinen aktiviert und durch den inversen Agonisten/Antagonisten Agouti-Related Peptide (AgRP) inaktiviert. Als weiterer Downstream-Mediatoren der MC4R-Aktivierung wurden kürzlich Brain Derived Neurotrophic Factor (BDNF) und dessen Rezeptor TrkB (Tropomyosin-Related –Kinase) identifiziert. Mutationen im MC4R gelten als häufigste monogenetische Ursache für Adipositas. Da viele dieser Mutationen aber in vitro funktionell nicht relevant sind, wurde ein Amosäurevergleich von orthologen MC4R aus 70 verschiedenen Spezies erstellt. Funktionsverlustmutationen waren häufiger an koservierten Positionen, während Mutationen ohne Effekt überwiegend an schwach konservierten Positionen zu finden waren. Funktionelle Charakterisierung der von in Mausmodellen identifizierten Punktmutationen I194F und Y302C ergaben eine gute in-vivo/in-vitro Korrelation. Desweiteren wurden in der Normalbevölkerung in normalgewichtigen Personen identifizierte MC4R-Punktmutationen funktionell charakterisiert. Die Mutationen R7C, A70T, T112K, Q156R, M200V, V166I und R236H hatten keinen Effekt auf die Rezeptorfunktion, die H158R. Mutation zeigte eine hohe Basalaktivität, die aber durch AgRP erniedrigt werden konnte. Die in adipösen Patienten gefundenen Mutationen S136F und S139R wiesen einen kompletten Funktionsverlust auf, erstere verursachte zudem sogar einen dominant-negativen Effekt bei Koexpression mit dem Wildtyprezeptor. Für den MC3R wurde das zum Translationsstart bevorzugte Startcodon identifiziert. Für die Rezeptortyrosinkinase TrkB konnte in Hefe-2-Hybridscreens der neue Interaktionspartner Sept3 identifiziert werden. Dieses Protein bindet phosphorylierungsunabhängig an die intrazelluläre Juxtamembrandomäne. / Bodyweight and food intake are regulated by the hypothalamus which integrates peripheral hormonal and neural signals. The G-protein-coupled melanocortin-receptors 3 and 4 (MC3R and MC4R) are activated by melanocortins or inhibited by agouti-related pepetide (AgRP) and signal via the cAMP pathway. Brain-derived neurotrophic Factor (BDNF) was recently shown to signal downstream the MC4R via its receptor TrkB (tropomyosin-related kinase). Mutations in the MC4R are the most common cause of monogenetic obesity. However, many of these mutations are not functionally relevant in vitro. Here, an amino acid alignment of orthologous MC4R from over 70 species was used to evaluate reported mutations. Loss-of-function mutations were predominantly located at highly conserved positions whereas mutations without effect were located at non-conserved positions. Functional characterization of MC4R point mutations I194F (partial loss of function) and Y302C (complete loss of function) identified in mouse models showed good in vitro/in vivo correlation. Furthermore mutations found in normal weight persons were characterized: R7C, A70T, T112K, Q156K, M200V, V166I and R236H had no effect on receptor function in vitro, whereas the H158R Mutation showed high constitutive activity, which however could be diminished by AgRP. The mutations S136F and S139F identified in obese patients were characterized as complete loss-of-function mutations, the former additionally caused a dominant-negative effect on wildtype MC4R in vitro. For the MC3R the preferred start-codon for initiation of translation was identified. For TrkB Sept3 could be identified as a new interaction partner in a yeast-2-hybrid screen. This Protein belonging to the septin family binds to the intracellular juxtamembrane domain of TrkB independent of phosphorylation of the Shc-binding site.

Adipositas

G-Protein gekoppelter Rezeptor

Signaltransduktion

Hypothalamus

Neurotrophin

Melanocortin

evolutionärer Vergleich

Punktmutation

Septin

Protein-Protein-Interaktion

Translationsinitiaition

obesity

g-protein coupled receptor

hypothalamus

signaltransduction

neurotrophin

melanocortin

evolutionary approach

pointmutation

septin

protein-protein-interaction

initiation of translation

570 Biowissenschaften, Biologie

32 Biologie

YC 8100

ddc:570

Endokrine Wirkungen (anti)androgener Substanzen bei der Ploetze (Rutilus rutilus)

Ballegooy, Christoph van

28 March 2008

Substanzen, die durch ihr hormonell wirksames Potenzial mit dem Hormonsystem interagieren und adverse Effekte auf die Reproduktion von Invertebraten und Vertebraten ausueben koennen, erlangten in den letzten Jahrzehnten große Aufmerksamkeit. Viele dieser Substanzen reduzieren die Fertilitaet oder die Fekunditaet, fuehren zu Abnormalitaeten in der Ontogenese oder im Verhalten der Tiere und haben Einfluss auf die Geschlechterverhaeltnisse. In der vorliegenden Arbeit wurden verschiedene Aspekte dieses Themengebietes bearbeitet. Das in Europa endemisch vorkommende Rotauge (Rutilus rutilus), ein Sueßwasserfisch, wurde als Modelltier fuer den Nachweis von (anti)androgenen Effekten auf aquatisch lebende Organismen etabliert. Zum Nachweis der (anti)androgenen Wirkmechanismen wurden die Tiere mit Modellsubstanzen aus drei verschiedenen Gruppen exponiert. Aus der Gruppe der Substanzen mit potenziell androgener Wirkung wurden Triphenylzinn (TPT) und Methyltestosteron (MT) verwendet, aus der Gruppe der Antiandrogene Vinclozolin (VIN) und Cyproteronazetat (CYP) und aus der Gruppe der Aromatasehemmer, und somit potenziell androgener Wirkung, Letrozol (LET) und Fenarimol (FEN). Feedbackmechanismen auf die Hypothalamus-Hypophysen-Gonaden-Achse (mRNA-Expression des Luteinisierenden Hormons, des Follikel stimulierenden Hormons und der Aromatase), mRNA-Expression potentieller Biomarker in der Leber (Androgen-Rezeptor-mRNA, Oestrogen-Rezeptor-mRNA), Sexsteroidspiegel im Blutplasma (17beta-Oestradiol und 11-keto-Testosteron), Enzymaktivitaeten im Gehirn (Aromatase), Histologie der Gonaden, Totallaenge, Gewicht und Geschlechterverteilung wurden als Endpunkte analysiert, um adverse Effekte auf die Reproduktionsbiologie von R. rutilus zu zeigen. Die untersuchten Endpunkte eigneten sich sehr gut zum Nachweis verschiedener Wirkmechanismen. / Substances that are able to interact with the endocrine system and cause adverse effects on the reproduction of invertebrates and vertebrates have gained much attention over the last few decades. Many of these substances reduce fertility or fecundity, lead to developmental abnormalities or abnormalities in the behaviour of animals and have an impact on sex ratios. The present study examines various aspects of these topics. The roach (Rutilus rutilus), a freshwater fish endemic in Europe, was established as a model animal for the detection of (anti)androgenic effects on aquatic organisms. For examination of the (anti)androgenic action, the animals were exposed to model compounds from three different groups: triphenyltin (TPT) and methyltestosterone (MT) from the group of substances with potentially androgenic effect, vinclozolin (VIN) and cyproteronacetate (CYP) from the group of antiandrogens, and letrozol (LET) and fenarimol (FEN) from the group of aromatase inhibitors, which thus have a potentially androgenic effect. Feedback mechanisms on the hypothalamus-pituitary-gonad-axis (mRNA expression of luteinising hormone, follicle stimulating hormone and aromatase), mRNA expression of potential biomarkers in the liver (androgen receptor mRNA, oestrogen receptor mRNA), steroid levels in the blood plasma (17beta-oestradiol and 11-ketotestosterone), enzyme activity in the brain (aromatase), histology of the gonads, total length, weight and sex ratios were analysed as endpoints to show adverse effects on the reproductive biology of R. rutilus. The studied endpoints are suitable for the detection of different modes of action. The histological examination of the gonads proved to be especially sensitive with the exposure to AACs to resulting in fundamental adverse damages to the gonads. It was ascertained that - in the early stages of ontogeny - androgens play as crucial of a role in the development of the gonads as previously attributed primarily to oestrogens.

Reproduktion

Hormonsystem

Plötze (Rutilus rutilus)

(anti)androgenen Wirkmechanismen

Triphenylzinn (TPT)

Methyltestosteron (MT)

Vinclozolin (VIN)

Cyproteronazetat (CYP)

Letrozol (LET)

Fenarimol (FEN)

Hypothalamus-Hypophysen-Gonaden-Achse

Endocrine system

Reproduction

Roach (Rutilus Rutilus)

(Anti)androgenic action

Triphenyltin (TPT)

Methyltestosterone (MT)

Vinclozolin (VIN)

Cyproteronazetate (CYP)

Letrozol (LET)

Fenarimol (FEN)

Hypothalamus-pituitary-gonad-axis

570 Biowissenschaften, Biologie

32 Biologie

WD 5823

WR 4700

ddc:570

Impact des acides gras alimentaires sur le système dopaminergique mésolimbique : effets différentiels des acides gras saturés et mono-insaturés

Hryhorczuk, Cecile

06 1900

Les comportements motivés dont l‟addiction aux drogues d‟abus, mettent en jeu le système dopaminergique mésolimbique. Aussi connu sous le nom de système de la récompense, celui-ci comprend les neurones à dopamine de l‟aire tegmentale ventrale qui projettent, entre autres, vers le noyau accumbens. Tout comme les neurones de l‟hypothalamus, les neurones à dopamine de l‟aire tegmentale ventrale répondent aux hormones telles que la leptine, l‟insuline et la ghréline pour modifier la prise alimentaire, la motivation ou encore le tonus dopaminergique. Ceci indique que le système dopaminergique mésolimbique est sensible aux signaux hormonaux circulants et suggère que les neurones de l‟aire tegmentale ventrale pourraient percevoir les signaux métaboliques comme le glucose ou les acides gras. De plus, plusieurs études chez les humains et les rongeurs démontrent que l‟obésité et les diètes riches en gras affectent négativement la fonction dopaminergique mésolimbique. Étant donné les lacunes qui demeurent quant aux mécanismes impliqués dans la dysfonction du système dopaminergique mésolimbique induite par la nourriture riche en gras, nous avons cherché à évaluer les effets de l‟acide oléique et de l‟acide palmitique, deux des acides gras les plus abondants dans l‟organisme et l‟alimentation contemporaine, sur le système de la récompense. Ces deux acides gras, l‟un saturé (acide palmitique) et l‟autre mono-insaturé (acide oléique), se distinguent par leurs effets différentiels sur la prise alimentaire, la signalisation hormonale ou encore leur métabolisme intracellulaire mais aussi sur la santé cardiovasculaire et mentale. Nous avons dans un premier temps évalué la capacité du système dopaminergique mésolimbique à détecter les acides gras. Nous avons comparé les effets de l‟injection d‟acide oléique ou d‟acide palmitique dans l‟aire tegmentale ventrale sur la prise alimentaire, la motivation et l‟activité électrique des neurones à dopamine de l‟aire tegmentale ventrale. Nos résultats montrent que l‟acide oléique, mais pas l‟acide palmitique, diminue la prise alimentaire et le comportement motivé. L‟acide oléique inhibe également l‟activité électrique des neurones à dopamine, ces effets semblent dépendre de son entrée dans la cellule. De plus, nous montrons que les neurones à dopamine de l‟aire tegmentale ventrale expriment plusieurs 3 gènes de protéines importantes pour le transport et le métabolisme des acides gras et qu‟ils sont capables de d‟incorporer les acides gras. Nous avons dans un second temps évalué les effets de l‟acide oléique et de l‟acide palmitique dérivés de l‟alimentation. Nous avons soumis des rats à l‟une de ces trois diètes : une riche en gras enrichie en acide oléique, une riche en gras enrichie en acide palmitique ou une contrôle faible en gras. Après huit semaines, et en l‟absence d‟obésité ou d‟altérations métaboliques majeures, la diète enrichie en acide palmitique, mais pas la diète isocalorique enrichie en acide oléique, induit une hyposensibilité aux effets récompensants et locomoteurs de l‟amphétamine, associée, entre autres, à la diminution de la signalisation du récepteur à la dopamine D1R et de l‟expression du transporteur de la dopamine. Nous avons finalement exploré l‟impact de ces diètes sur l‟activité de l‟axe hypothalamo-hypophysaire-surrénalien. Les résultats montrent que la diète enrichie en acide palmitique altère aussi la fonction de l‟axe et l‟expression de plusieurs gènes cibles des corticostéroïdes, sans toutefois modifier le comportement anxieux. Ce travail de doctorat vient compléter les connaissances sur les dysfonctions du système dopaminergique mésolimbique induites par la nourriture riche en gras. Il met en lumière les effets différentiels des classes d‟acides gras et les mécanismes par lesquels ils modulent les comportements motivés et alimentaires. De façon chronique, avant l‟apparition d‟obésité et d‟altérations métaboliques, les acides gras saturés, et non les acides gras mono-insaturés, issus de l‟alimentation perturbent le fonctionnement de l‟axe hypothalamo-hypophysaire-surrénalien et réduisent la fonction dopaminergique. Ceci pourrait contribuer à perpétuer la recherche et la prise de ce type d‟acides gras afin de compenser ce déficit. / The mesolimbic dopamine system, also known as the reward system, is well recognized for its role in motivated reward-related behaviours such as drug addiction. It consists of dopamine neurons originating in the ventral tegmental area that project, among others, to the nucleus accumbens. Similar to neurons in the hypothalamus, dopamine neurons in the ventral tegmental area can detect circulating hormones such as leptin, insulin and ghrelin to adjust food intake, motivation and dopamine tone. This suggests that they could also perceive nutritional signals like glucose and fatty acids. Moreover, several lines of evidence exist showing that palatable food enriched in fat and obesity reduce mesolimbic dopamine function. Given the many unknowns regarding the mechanisms of obesity-induced dopamine dysfunction, and given that fatty acids differentially influence cardiovascular and mental health according to their class, we sought to determine the effects of the monounsaturated fatty acid oleic acid and the saturated fatty acid palmitic acid, two of the most abundant fatty acids in the body and foods, on mesolimbic dopamine function. Notably palmitic acid and oleic acid differ in their intracellular metabolic fate as well as in their effects on food intake and leptin and insulin signaling at the level of the hypothalamus. We first evaluated the fatty acid sensing properties of the mesolimbic dopamine system. We looked at the effects of the injection of oleic acid or palmitic acid in the ventral tegmental area on food intake, motivation and dopamine neurons activity. Our results demonstrate that oleic acid, but not palmitic acid, reduces basal and motivated feeding behavior and neuronal activity. Those effects seem to be dependent on its entry into the cell. Moreover, using a neurons culture system we show that dopamine neurons can uptake fatty acids. We then examined the effect of food-derived oleic and palmitic acid on mesolimbic dopamine function. We assigned rats to a low-fat control diet or to one or the other of a high-fat diet: one enriched in oleic acid or one enriched in palmitic acid. The two high-fat diets are isocaloric and differed only in the fat source. Following eight weeks of feeding, the palmitic 5 acid-enriched high-fat diet, but not the oleic acid-enriched diet, decreased the sensitivity to the rewarding and locomotor-sensitizing effects of amphetamine. This was associated with a reduction of dopamine receptor D1R signaling and dopamine transporter expression. Importantly this occured independently of weight gain and hormonal changes. Lastly, we explored the impact of those diets on the activity of the hypothalamus-pituitary-adrenal axis. Results show that the saturated fat diet alters the function of the axis as well as the expression of several keys genes targeted by glucocorticoids in the hypothalamus but without affecting anxiety-related behavior. This work provides further insight into how the mesolimbic dopamine system is altered by high-fat food consumption. It brings light to the differential effects of two classes of fatty acids and the mechanisms by which they modulate food intake and motivation. The prolonged intake of saturated fat, but not mono-unsaturated fat, disrupts the hypothalamus-pituitary-adrenal axis and decreases mesolimbic dopamine function prior to the onset of obesity and major metabolic alterations. Dysfunction of dopaminergic systems induced by saturated fat consumption could promote further intake of such palatable food as a means to compensate for reward hyposensitivity.

Aire tegmentale ventrale

Noyau accumbens

Dopamine

Acides gras

Motivation

Homéostasie énergétique

Corticostérone

Ventral tegmental area

Nucleus accumbens

Fatty acids

Reward

Energy homeostasis

Hypothalamus-pituitary-adrenal axis

Corticosterone

Vztah metabolismu kortikosteroidů a ontogeneze ke stresové odpovědi / Relationship between corticosteroid metabolism, ontogenesis and stress response

Makal, Jakub

January 2013

Stress is a widespread phenomenon in the western society of these days. It is a risky factor for health and well-being of the majority of people. Based on these facts, it is the main subject for the field of "stress physiology" research, which aims to study processes occurring during stress response and tries to elucidate mechanisms leading to stress-induced health impairment. The first aim of this thesis was to describe effects of psycho-social stress on organism. The second aim was to find out if can stress applied in juvenile age affect the stress response in adulthood. If so, how is the role of glucocorticoid-metabolism enzyme 11β-HSD1 in this influence? To answer these questions, two different animal models inducing stress response in the laboratory rat were used. The first one is the model of mild social stress based on the resident-intruder paradigm. Our results show efficancy of this model. Fisher 344 male rats treated under this model for seven consecutive days show highly elevated plasma corticosterone concentrations and elevated expression of the glucocorticoid receptor gene in the pituitary. Behavioral analysis demonstrates a decreased social behavioral profile of the intruders, suggesting submisive social position of these animals in the resident-intruder paradigm. The second model used is...

The innate defensive behaviour and unconditioned fear-induced antinociception evoked by NMDA receptor activation in the medial hypothalamus are modulated by the intradiencephalic treatment with cannabidiol: the role of CB1 cannabinoid receptor / O comportamento de defesa inato e a antinocicepção induzida pelo medo incondicionado induzidos pela ativação de receptores NMDA no hipotálamo medial são modulados pelo tratamento intradiencefálico com cannabidiol: papel do receptor canabinoide CB1

Khan, Asmat Ullah

15 October 2018

The impacts of exogenous cannabinoids, such as the chemical constituents of Cannabis sativa like cannabidiol (CBD), on brain regions having a modest number of cannabinoid receptors, for example, the ventromedial hypothalamus, are not yet surely knew. A few researches have shown evidence that ventromedial hypothalamus (VMH) neurons play a role in modulating innate fear-induced behavioural reactions in rodents submitted to experimental models of panic attack, for example those based on prey versus wild snake confrontation paradigm. The panic attack-like state was also potentially induced in laboratory animals by N-Methyl-D-aspartate (NMDA), an excitatory amino acid, which stimulates neurons that organize defensive behavioural reactions in the central nervous system. Despite the fact that CB1 receptor-mediated endocannabinoid signaling mechanism underlies the antiaversive effect of exogenous anandamide in medial hypothalamus, there is still a lack of morphological evidence to support the distribution of CB1 receptors in the VMH. Henceforth, this study was designed to explore the specific pattern of distribution of the CB1 receptors in the VMH and, subsequently, the implication of these receptors in the endocannabinoidmodulated defensive behavioural responses followed by fear-induced antinociception evoked by NMDA microinjected in the VMH. A stainless steel guide-cannula was embedded in the rodent\'s brain coordinated towards VMH by means of stareotaxic surgery. Three different doses of cannabidiol (CBD) were microinjected in the VMH. The most effective dose was used after the pretreatment with the CB1 receptor-antagonist AM251, followed by NMDA microinjection in the VMH. The outcomes demonstrated that the defensive behavioural responses evoked in response to intra-VMH administration of NMDA (6 nmol) were decreased by intra-hypothalamic microinjections of CBD at the highest dose (100 nmol).These effects, however, were blocked by the administration of the CB1 receptor-antagonist AM251 (100 pmol) in the VMH. In addition, the fear-induced antinociception elicited by VMH chemical stimulation diminished after the VMH treatment with CBD, an effect reversed by the intra-diencephalic pretreatment with AM251. These findings suggested that CBD causes panicolytic-like effects when administered in the VMH, and that antiaversive effect recruits the CB1 receptor-endocannabinoid signaling mechanism in VMH. / O papel dos canabinoides exógenos nas regiões do cérebro com um número modesto de receptores cannabinoides, por exemplo, o hipotálamo ventromedial, ainda não está plenamente esclarecido. Algumas pesquisas de nosso grupo, não obstante, mostraram o hipotálamo ventromedial (HVM) exerce modulação de reações comportamentais provocadas pelo medo inato em animais submetidos a um modelo de ataques de pânico. Crises de pânico foram induzidas em animais de laboratório por N-metil-D-aspartato (NMDA), um aminoácido excitatório que, ao ser microinjetado em estruturas do sistema encefálico de aversão, estimula reações comportamentais defensivas no sistema nervoso central que mimetizam as respostas defensivas eliciadas por roedores confrontados com serpentes. Apesar do mecanismo de sinalização endocanabinoide mediado pelos receptores CB1 desempenhar um papel na modulação da neurotransmissão excitadora e inibitória no SNC, ainda há escassez de evidências morfológicas que embasem a distribuição dos receptores CB1 no HVM. Por conseguinte, este estudo foi idealizado para explorar a forma específica de distribuição dos receptores CB1 no HVM e, posteriormente, estudar a implicação desses receptores na modulação de respostas comportamentais defensivas, seguidas por antinocicepção induzida pelo medo, moduladas por endocanabinoides e evocadas por microinjetação de NMDA no HVM. Uma cânula-guia feita de aço inoxidável foi implantada no cérebro do roedor, e direcionada para o HVM por meio de cirurgia estareotóxica. Três diferentes doses de cannabidiol (CBD) foram microinjetadas no HVM. A dosagem mais eficaz foi utilizada após o pré-tratamento do hipotálamo medial com um antagonista do receptor CB1, o AM251, seguido da microinjeção NMDA no HVM. Os resultados demonstraram que as respostascomportamentais defensivas evocadas em resposta à administração intra-HVM de NMDA (6 nmol) foram diminuídas por microinjeções intra-hipotalâmicas de CBD na dose mais alta (100 nmol). Estes efeitos, no entanto, foram atenuados pela administração do antagonista do receptor CB1, AM251, na dose de 100 pmol no HVM. Além disso, a antinocicepção induzida pelo medo foi atenuada pela administração intra-diencefálica de CBA, o que foi revertido pelo pré-tratamenot do HVM com AM251. Esses dados sugerem que o CBD causa efeitos panicolíticos, quando administrado no HVM, envolvendo o mecanismo de sinalização do receptor CB1-endocannabinoide.

Antinocicepção induzida pelo medo

Ataques de pânico

Cannabidiol

Cannabinoid receptor type-1

Comportamento de defesa

Defensive behavior

Hipotálamo ventromedial

Innate fear-induced antinociception

NMDA

NMDA

Panic attack-like responses

Receptores canabinoides de tipo 1

Ventromedial hypothalamus

Le contrôle hypothalamique de l’homéostasie énergétique : impact de l’environnement maternel et implication du CNTF / H ypothalamic control of the energetic homeostasis : Impact of the maternal environment and the implication of the CNTF

Couvreur, Odile

21 December 2011

Le maintien de l’homéostasie énergétique est placé sous le contrôle de cytokines qui agissent dans le système nerveux central, notamment au niveau de l’hypothalamus. En particulier, la leptine, cytokine produite par le tissu adipeux, diminue la prise alimentaire et stimule la perte de poids. L’obésité est une épidémie mondiale qui progresse de façon alarmante, notamment chez les enfants et souvent associée à des pathologies sévères et des désordres endocriniens comme la résistance à la leptine ou à l’insuline. Le CNTF (Ciliary Neurotrophic Factor) est une neurocytokine de la même famille que la leptine dont l’un des principaux avantages est qu’il stimule la perte de poids dans les cas de leptino-résistance en activant les mêmes voies de signalisation que la leptine (Benomar et al., 2009). Face à l’épidémie mondiale d’obésité,chez la population adulte comme enfantine, il apparaît nécessaire de décrypter les mécanismes impliqués dans la genèse de la maladie ainsi que les potentiels agents thérapeutiques.L’objectif premier de ce travail de thèse a été de caractériser l’impact d’une alimentation maternelle hyperlipidique (HF) sur les capacités de contrôle de l’homéostasie énergétique chez la descendance. En effet, le concept de « programmation métabolique » propose que des pertubations de l’environnement périnatal puissent influencer durablement la descendance, la rendant plus susceptible de développer une obésité dans un contexte nutrionnellement riche.Des études menées au sein du laboratoire ont montré qu’un régime maternel HF pouvait programmer l’acquisition de la leptino-résistance chez la descendance à l’âge adulte (Ferezou-Viala et al., 2007b). Nous avons donc testé la prédispostion de ces animaux à prendre du poids lorsqu’ils étaient nourris avec un régime hypercalorique (P). Nos données ont montréqu’étonnamment, le régime maternel HF protégeait la descendance contre le gain de poids induite par le régime P, induisait des modifications d’expression des marqueurs de l’homéostasie énergétique dans le foie et l’hypothalamus, ainsi que de profondes réorganisations cytoarchitectoniques dans le noyau arqué. Plus précisément, le régime maternel HF était associé à une réorganisation de la couverture astrocytaire périvasculaire dans le noyau arqué de la descendance qui persistait à l’âge adulte.Dans une seconde partie de la thèse, nous avons étudié les mécanismes d’action du CNTF. En effet, notre équipe a récemment mis en évidence que le CNTF endogène pourrait jouer un rôle dans la régulation de l’homéostasie énergétique. Les niveaux hypothalamiques de cette cytokine, présente dans les astrocytes et les neurones du noyau arqué, augmentent chez les animaux résistant à une alimentation hypercalorique. Cela pourrait suggérer un rôle protecteur du CNTF contre la prise de poids chez certains individus (Vacher et al., 2008). A ce jour, les mécanismes d’action du CNTF restent cependant mal compris car ce dernier ne possède pas de peptide signal et n’est donc pas sécrété selon des mécanismes d’exocytose classiques. Partant du constat que le CNTF et ses sous-unités réceptrices étaient distribuées de façon similaire dans les cellules du noyau arqué, nous avons émis l’hypothèse que le CNTF pourrait exercer une action intracellulaire sur les cellules de cette structure. Dans cette étude nous démontrons que le CNTF peut interagir directement avec ses récepteurs dans le noyau des neurones anorexigènes du noyau arqué, pour réguler leur activité transcriptionnelle. Ces données proposent ainsi un nouveau mécanisme à l’action anorexigène du CNTF / Obesity is a major health disease which involves numerous metabolic disorders. Increasing evidence suggests that the risk of developing the pathology in adulthood may be influenced through inappropriate perinatal nutrition. In our study, we first investigated the impact of a maternal high-fat (HF) diet, which is known to induce hypothalamic leptin resistance in adult offspring (Férézou-Viala et al., 2007), to develop obesity in a rich diet environment (P diet). Our results showed that surprisingly, HF maternal diet protected offspring against body weight gain induced by P diet. In a second part of the thesis, we studied mechanisms of action of CNTF, a neurocytokine which could protect some people against body weight gain induced by a P diet (Vacher et al., 2008). Results of this study showed that CNTF ant its subunits receptors could translocate to the hypothalamic cell nucleus to induced POMC transcription.

Homéostasie énergétique

Leptino-résistance

Noyau arqué

Régime maternel HF

CNTF

Noyau

Astrocytes

Microcopie confocale

Immunohistochimie

Run on

Energetic homeostasis

Leptin resistance

Hypothalamus

Maternal High-Fat diet

CNTF

Nucleus

Palatable diet

Envolvimento de mecanismos glutamatérgicos da substância cinzenta periaquedutal dorsal e do hipotálamo medial no medo condicionado à luz / Involvement of glutamatergic mechanisms of the dorsal periaqueductal gray matter and medial hypothalamus in conditioned fear to the light

Adriano Edgar Reimer

27 September 2012

A substância cinzenta periaquedutal dorsal (dPAG) e o hipotálamo medial (MH) são duas estruturas encefálicas que estão envolvidas na elaboração de estados aversivos e expressão de respostas defensivas. A estimulação elétrica da dPAG ou do MH produz uma série de respostas comportamentais que se assemelham às respostas defensivas induzidas pela presença de um predador. Esses mesmos comportamentos podem ser eliciados com a microinjeção local de agonistas glutamatérgicos nessas estruturas, indicando o envolvimento de aminoácidos excitatórios na expressão das respostas defensivas incondicionadas. Apesar disso, a participação destas estruturas no medo condicionado ainda é pouco conhecida. Assim, o objetivo deste estudo foi avaliar o envolvimento da mediação glutamatérgica da dPAG e de núcleos do MH núcleo anterior (AH) e núcleo pré-mamilar dorsal (PMd) na expressão do medo condicionado à luz. Para isso, foram avaliados os efeitos de agonistas e antagonistas glutamatérgicos (AMPA/Cainato e NMDA) administrados nessas estruturas no teste do sobressalto potencializado pelo medo (SPM) e na medida de congelamento condicionado. Ratos Wistar machos com cânulas-guias implantadas na dPAG, AH ou PMd foram submetidos ao condicionamento aversivo (pareamentos luz+choque). Vinte e quatro horas depois, esses animais receberam injeções intra-dPAG, AH ou PMd de NMDA ou ácido caínico (agonistas NMDA e AMPA/Cainato, respectivamente) ou AP7 ou NBQX (antagonistas NMDA e AMPA/Cainato, respectivamente) e foram submetidos ao teste do SPM. A resposta de congelamento condicionado foi avaliada na mesma sessão. Eventuais alterações motoras foram avaliadas no teste do campo aberto. A administração dos agonistas glutamatérgicos na dPAG promoveu efeitos pró-aversivos no SPM e congelamento condicionado. NBQX sozinho não produziu nenhum efeito significativo, ao passo que o AP7 diminuiu somente o congelamento condicionado. Entretanto, ambos os antagonistas bloquearam os efeitos dos respectivos agonistas. Já a administração dos agonistas e antagonistas glutamatérgicos no AH e PMd, em doses que não afetaram a atividade motora, não produziu efeitos significativos na resposta de congelamento condicionado e SPM. Os presentes resultados sugerem a participação de aminoácidos excitatórios da dPAG, mas não do MH, na expressão do medo condicionado à luz. / The dorsal periaqueductal gray matter (dPAG) and the medial hypothalamus (MH) are two brain structures that are involved in the elaboration of aversive states and expression of defensive responses. Electrical stimulation of the dPAG or MH produces a series of behavioral responses that resemble those defensive responses triggered in the presence of a predator. These same behaviors can be elicited with the local microinjection of glutamate agonists into these structures, indicating the involvement of excitatory amino acids in the expression of unconditioned fear responses. Nevertheless, the involvement of these structures in fear conditioning is still unknown. The objective of this study was to evaluate the involvement of glutamatergic mediation of the dPAG and MH nuclei anterior nucleus (AH) and dorsal pre-mammillary nucleus (PMd) in the expression of conditioned fear to the light. Thus, we evaluated the effects of glutamatergic agonists and antagonists (AMPA/Kainate and NMDA) administered into these structures in fear potentiated startle (FPS) and conditioned freezing responses to the light. Male Wistar rats with guide-cannulae implanted in the dPAG, AH or PMd were subjected to aversive conditioning (light+shock pairings). Twenty-four hours later, the animals were injected intra-dPAG, AH or PMd with NMDA or kainic acid (NMDA and AMPA/Kainate agonists, respectively) or AP7 or NBQX (NMDA and AMPA/Kainate antagonists, respectively) and were subjected to the FPS test. The conditioned freezing response was measured in the same session. Potential motor effects were evaluated with the open-field test. The administration of glutamate agonists into the dPAG promoted pro-aversive effects in the FPS and conditioned freezing. NBQX produced no significant effect per se, whereas AP7 only decreased conditioned freezing. Both antagonists blocked the effects of the respective agonist. On the other hand, the administration of glutamatergic agonists and antagonists into AH and PMd, in doses that did not affect motor activity, produced no significant effects on conditioned fear responses. The present results suggest the involvement of mechanisms mediated by excitatory amino acids of the dPAG, but not of the MH, in the expression of conditioned fear responses to light.

congelamento condicionado

hipotálamo medial

Mediação glutamatérgica

Medo condicionado

sobressalto potencializado pelo medo

Conditioned freezing

Dorsal periaqueductal gray matter

Fear conditioning

Fear potentiated startle

Glutamate

Medial hypothalamus

Envolvimento de mecanismos glutamatérgicos da substância cinzenta periaquedutal dorsal e do hipotálamo medial no medo condicionado à luz / Involvement of glutamatergic mechanisms of the dorsal periaqueductal gray matter and medial hypothalamus in conditioned fear to the light

Reimer, Adriano Edgar

27 September 2012

A substância cinzenta periaquedutal dorsal (dPAG) e o hipotálamo medial (MH) são duas estruturas encefálicas que estão envolvidas na elaboração de estados aversivos e expressão de respostas defensivas. A estimulação elétrica da dPAG ou do MH produz uma série de respostas comportamentais que se assemelham às respostas defensivas induzidas pela presença de um predador. Esses mesmos comportamentos podem ser eliciados com a microinjeção local de agonistas glutamatérgicos nessas estruturas, indicando o envolvimento de aminoácidos excitatórios na expressão das respostas defensivas incondicionadas. Apesar disso, a participação destas estruturas no medo condicionado ainda é pouco conhecida. Assim, o objetivo deste estudo foi avaliar o envolvimento da mediação glutamatérgica da dPAG e de núcleos do MH núcleo anterior (AH) e núcleo pré-mamilar dorsal (PMd) na expressão do medo condicionado à luz. Para isso, foram avaliados os efeitos de agonistas e antagonistas glutamatérgicos (AMPA/Cainato e NMDA) administrados nessas estruturas no teste do sobressalto potencializado pelo medo (SPM) e na medida de congelamento condicionado. Ratos Wistar machos com cânulas-guias implantadas na dPAG, AH ou PMd foram submetidos ao condicionamento aversivo (pareamentos luz+choque). Vinte e quatro horas depois, esses animais receberam injeções intra-dPAG, AH ou PMd de NMDA ou ácido caínico (agonistas NMDA e AMPA/Cainato, respectivamente) ou AP7 ou NBQX (antagonistas NMDA e AMPA/Cainato, respectivamente) e foram submetidos ao teste do SPM. A resposta de congelamento condicionado foi avaliada na mesma sessão. Eventuais alterações motoras foram avaliadas no teste do campo aberto. A administração dos agonistas glutamatérgicos na dPAG promoveu efeitos pró-aversivos no SPM e congelamento condicionado. NBQX sozinho não produziu nenhum efeito significativo, ao passo que o AP7 diminuiu somente o congelamento condicionado. Entretanto, ambos os antagonistas bloquearam os efeitos dos respectivos agonistas. Já a administração dos agonistas e antagonistas glutamatérgicos no AH e PMd, em doses que não afetaram a atividade motora, não produziu efeitos significativos na resposta de congelamento condicionado e SPM. Os presentes resultados sugerem a participação de aminoácidos excitatórios da dPAG, mas não do MH, na expressão do medo condicionado à luz. / The dorsal periaqueductal gray matter (dPAG) and the medial hypothalamus (MH) are two brain structures that are involved in the elaboration of aversive states and expression of defensive responses. Electrical stimulation of the dPAG or MH produces a series of behavioral responses that resemble those defensive responses triggered in the presence of a predator. These same behaviors can be elicited with the local microinjection of glutamate agonists into these structures, indicating the involvement of excitatory amino acids in the expression of unconditioned fear responses. Nevertheless, the involvement of these structures in fear conditioning is still unknown. The objective of this study was to evaluate the involvement of glutamatergic mediation of the dPAG and MH nuclei anterior nucleus (AH) and dorsal pre-mammillary nucleus (PMd) in the expression of conditioned fear to the light. Thus, we evaluated the effects of glutamatergic agonists and antagonists (AMPA/Kainate and NMDA) administered into these structures in fear potentiated startle (FPS) and conditioned freezing responses to the light. Male Wistar rats with guide-cannulae implanted in the dPAG, AH or PMd were subjected to aversive conditioning (light+shock pairings). Twenty-four hours later, the animals were injected intra-dPAG, AH or PMd with NMDA or kainic acid (NMDA and AMPA/Kainate agonists, respectively) or AP7 or NBQX (NMDA and AMPA/Kainate antagonists, respectively) and were subjected to the FPS test. The conditioned freezing response was measured in the same session. Potential motor effects were evaluated with the open-field test. The administration of glutamate agonists into the dPAG promoted pro-aversive effects in the FPS and conditioned freezing. NBQX produced no significant effect per se, whereas AP7 only decreased conditioned freezing. Both antagonists blocked the effects of the respective agonist. On the other hand, the administration of glutamatergic agonists and antagonists into AH and PMd, in doses that did not affect motor activity, produced no significant effects on conditioned fear responses. The present results suggest the involvement of mechanisms mediated by excitatory amino acids of the dPAG, but not of the MH, in the expression of conditioned fear responses to light.

Conditioned freezing

congelamento condicionado

Dorsal periaqueductal gray matter

Fear conditioning

Fear potentiated startle

Glutamate

hipotálamo medial

Mediação glutamatérgica

Medial hypothalamus

Medo condicionado

sobressalto potencializado pelo medo