Sucinato melhora a memória da tarefa de medo condicionado em ratos / Succinate improves the memory of fear conditioning in rats

Pasquetti, Liana

03 July 2007

Succinate is a dicarboxylic acid that accumulates due to succinate dehydrogenase inhibition. This dicarboxylic acid has a biphasic effect on neural activity in vitro that seems to be mediated by N-methyl-D-aspartate (NMDA) receptors. The NMDA receptor is distributed throughout the central nervous system and mediates synaptic plasticity-related events, such as learning and memory. Although it has been described that succinate modulates NMDA conductance, it is not known if this organic acid modulates learning and me mory. Therefore, in the present study we investigated whether the immediate post-training systemic or intrahippocampal administration of succinate affects the memory of fear conditioning in rats. In addition, we investigated whether the NMDA and β-adrenergic receptors are involved in the facilitatory effect of succinate on memory. Systemic (0,00005, 0,0005, 0,005, 0,05 and 0,5 mg/kg i.p) or bilateral intra-hippocampal (0.21 pmol i.h.) immediate post-training administration of succinate biphasically facilitated contextual fear conditioning and had no effect on conditioning to tone. Systemic or intra-hippocampal administrations of MK-801 (0,001 mg/kg i.p. or 0,21 pmol i.h. respectively), a noncompetitive NMDA receptor antagonist, at a dose that had no effect per se, reversed the facilitatory effect of succinate on contextual fear conditioning. The systemic administration of propranolol (10 mg/kg i.p.), a β-adrenergic antagonist, at a dose that had no effect per se, also reversed the facilitatory effect of succinate on contextual fear conditioning. The administration of succinate (0,005 mg/kg i.p.) immediately after training and 15 minutes before the test did not affect the performance of the animals on fear conditioning. These results suggest that the facilitatory effect of succinate on the memory of fear conditioning involves NMDA and β-adrenergic receptors. The results also indicate that the facilitatory effect of succinate on memory is not related to state-dependence / O sucinato é um intermediário do ciclo de Kreks e também da cadeia respiratória, mas que também parece ter funções não relacionadas ao metabolismo energético. De fato, este ácido dicarboxílico tem efeito bifásico sobre a atividade neural in vitro, que parece ser mediado pelo receptor glutamatérgico N-metil-D-aspartato (NMDA). O receptor NMDA está presente em todo o sistema nervo central (SNC) e os processos mediados por este receptor incluem plasticidade sináptica e formação de circuitos neurais. Embora tenha sido descrito que o sucinato modula a atividade neural in vitro, não se sabe se este ácido orgânico modula processos fisiológicos ligados ao receptor NMDA, como o aprendizado e memória. Consequentemente, neste estudo foi investigado o efeito da administração sistêmica e intrahipocampal de sucinato, MK-801 e propranolol sobre a consolidação da memória em ratos, utilizando a tarefa de medo condicionado clássico. Posteriormente se investigou se os efeitos do sucinato sobre a memória envolvem dependência de estado. O teste do medo condicionado consistiu na apresentação de estímulos pareados, condicionado (tom 2000 Hz 90 dB/10 s) e incondicionado (choque 0.6 mA/1 s). O estado de imobilidade do animal foi utilizado como um indicativo de memória nas sessões de avaliação de memória ao contexto e ao tom. A administração sistêmica de sucinato nas doses de 0,00005, 0,0005, 0,005, 0,05 e 0,5 mg/kg i.p. imediatamente após o treino melhorou a memória. Contudo, a dose de 5 mg/kg de sucinato não alterou a memória dos animais, caracterizando um efeito bifásico sobre a memória. Essa melhora da memória induzida por sucinato (0,005 mg/kg i.p.) foi revertido pela administração pós-treino de um antagonista do receptor NMDA, MK-801 (0,001 mg/kg i.p.) e pela administração imediatamente após o treino de um bloqueador adrenérgico, propranolol (10 mg/kg i.p.). A administração de sucinato (0,005 mg/kg i.p.) imediatamente após o treino e 15 minutos antes do teste não afetou a performance dos animais, não caracterizando dependência de estado. Nos experimentos que visaram identificar se a administração central de sucinato alterava a memória, os animais foram canulados bilateralmente no hipocampo e após a recuperação cirúrgica, recebiam injeções bilaterais imediatamente após o treino, de sucinato (0,21 pmol i.h.) que melhorou a memória. A administração imediatamente após o treino de MK- 801 (0,22 nmol i.h.) foi capaz de reverter esse efeito facilitador do sucinato sobre a memória. Estes resultados sugerem que o efeito facilitador da memória induzida pela administração de sucinato é mediado pelo receptor NMDA e envolve de alguma maneira o sistema adrenérgico

Sucinato

Memória

Medo condicionado

Receptor NMDA

MK-801

Propranolol

Succinate

Memory

Fear conditioning

NMDA receptor

β-adrenergic receptor

Rats

CNPQ::CIENCIAS BIOLOGICAS::BIOQUIMICA

Aspects of the interrelation between hypertension and insulin resistance

Osuafor, Godswill Nwabuisi

January 2009

Magister Scientiae (Medical Bioscience) - MSc(MBS) / Conclusion of this study: These data suggest that 6 weeks of high-fat feeding induces hypertension but does not produce obesity, dyslipidemia and insulin resistance. However, this model may be useful in studying vascular reactivity in hypertension in the absence of insulin resistance. / South Africa

Glucose tolerance test

High-fat diet

Hypertension

Insulin resistance

Lipid profile

QUICKI

Sprague Dawley rat

Vascular reactivity

Visceral fat

Î- adrenergic response

Aspects of the interrelation between hypertension and insulin resistance: a preliminary study

Nwabuisi, Osuafor Godswill

January 2009

Magister Scientiae (Medical Bioscience) - MSc(MBS) / Background: It is well known that some genetic factors and dietary factors, such as excessive salt intake and excessive caloric intake (resulting in obesity) are risk factors for hypertension. Fifty percent of all hypertensive patients are also insulin resistant. Both hypertension and insulin resistance are again risk factors for other cardiovascular diseases such as atherosclerosis and heart failure. The nature of the association between hypertension and insulin resistance has not been clearly elucidated. Spontaneously hypertensive rats are the ideal models to study the aspects of the relationships between hypertension and insulin resistance. Models of high-fat feeding induce obesity,hypertension and insulin resistance and are thus used extensively to study hypertension because these models closely mimic some of the renal and cardiovascular changes found in human hypertensive patients. The present study was initiated to evaluate if insulin resistance will develop within 6 weeks in a model of high-fat diet induced hypertension and if so, to determine whether captopril will affect the presence of insulin resistance.This model should in future be used to study vascular reactivity to phenylephrine (PHE),acetylcholine (ACH) and sodium nitroprusside (SNP) in hypertensive animals in theabsence or presence of insulin resistance and in normotensive insulin resistant animals. Methods: In a series of experiments, rats were divided into four groups that received different treatments: (i) laboratory pellets, (ii) high-fat diet, (iii) high-fat diet plus captopril and (iv) high-fat diet plus vehicle. Body weight was measured weekly for 6 weeks. Systolic blood pressure (SBP) and diastolic blood pressure (DBP) were measured every week during the 6-weeks feeding period by the tail cuff method using a two channel computerized non-invasive system from Kent Scientific Corporation, USA.m Intraperitonealy glucose tolerance tests (IPGTTs) were performed at week 3 and week 6.After 6 weeks, and after an overnight fast, the plasma lipid profile was determined using a portable CardiochekTM blood test system. Fasting plasma insulin was determined using an immunoenzymatic assay for the in vitro quantitative measurement of rat insulin (INS) in serum and plasma. Insulin sensitivity was estimated by the quantitative insulin sensitivity check index (QUICKI) using the fasting plasma insulin and fasting glucose levels. After week 6 on the high-fat diet, thoracic aortae from the control and high-fat fed(HFD) animals were excised and vascular response to PHE, ACH and SNP were assessed in intact and denuded endothelium.Result: High-fat feeding did not cause a significant increase in body weight. High-fat feeding significantly increased systolic blood pressure from 125±2.1 mmHg in control animals to 155±5.9 mmHg in the HFD group (P < 0.05) and 158±5.6 mmHg in the HFDV group (P < 0.05). Diastolic blood pressure was increased from 86±2.8 mmHg in the control group to 117±2.5 mmHg in the HFD group (P < 0.05) and 113±3.4 mmHg in the HFDV group (P < 0.05). Visceral fat was increased from 0.8±0.1g in the control group to 3.1±0.6 g in the HFD group and 3.8±0.6 g in the HFDV group. IPGTTs performed at weeks 3 and 6 respectively did not differ significantly from the control group as evidenced from the AUC’s at weeks 3 and 6 respectively. High-fat feeding had no significant effects on blood cholesterol, triglyceride, high-density lipoprotein cholesterol (HDL-C), low-density lipoprotein cholesterol (LDL-C) values or and fasting plasma insulin levels. The KCl induced contraction in both aortic rings with intact and denuded endothelium did not differ significantly between the control and HFD groups (P= 0.4 and 0.8) respectively. The contraction mediated by KCl in aortic rings with intact and denuded endothelium from the control or HFD groups also did not differ significantly(control: intact vs denuded, P = 0.2; HFD: intact vs denuded, P = 1). Dose responsecurves(1-10 μM) to PHE indicated slightly stronger contractions in the high-fat fed animals at submaximal doses tested. The maximum contraction achieved was however the same (94±19% and 99±2.6% relative to KCl induced contraction, in the control and HFD group respectively, P<0.05). Relaxation responses to ACH and SNP represent preliminary data.Conclusion: These data suggest that 6 weeks of high-fat feeding induces hypertension but does not produce obesity, dyslipidemia and insulin resistance. However, this model may be useful in studying vascular reactivity in hypertension in the absence of insulin resistance.

Glucose tolerance test

High-fat diet

Hypertension

Insulin resistance

Lipid profile

QUICKI

Sprague dawley rat

Vascular reactivity

Visceral fat

α- adrenergic response

Ractopamina e arginina na alimentação de suínos / Arginine and ractopamine in swine diets

Calixto, Jussara Maria Reis

23 November 2012

Made available in DSpace on 2016-05-02T13:55:34Z (GMT). No. of bitstreams: 1 JussaraMaria ReisCalixto-dissertacao.pdf: 678492 bytes, checksum: 69d16272c951188cf230141c93f2978b (MD5) Previous issue date: 2012-11-23 / The objective of this study was to evaluate the effect of arginine and ractopamine on performance, carcass characteristics, lipid profile and liver histological features in growing and finishing pigs. The experimental design was randomized blocks with three treatments, eight repetitions, two animals per experimental unit, for a total of 24 animals (12 barrows and 12 gilts) with 65 days of age and live weight of 32 ± 0,75 quilogramas .The treatments were divided into: T1: control (C) (isocaloric meal and isocaloric), T2: C + 4 ppm of ractopamine and T3: C + 0.8% arginine.The additives ractopamine and arginine were added to the mash feed and these ad libitum for 89 days and 46 days of growth phase and 43 days from the termination phase. On reaching 150 days of age, the animals were slaughtered. We evaluated animal performance (average daily feed intake, average daily gain in weight and feed conversion) weighing the animals at the beginning and end of each phase and the rations offered. At slaughter blood samples were collected for biochemical analysis of lipid profile and liver slices for histological examination. The carcasses were hot and heavy after 24 hours refrigerated, carcass length, backfat thickness and loin eye area, were measured in hot carcass. Ractopamine supplementation improved the average feed intake during the growing phase (P <0.05), and average daily weight gain in crescimemto and finishing phases (P <0.05), without however changing other variables, carcass characteristics (P> 0.05) and lipid profile (P> 0.05). The addition of arginine did not affect performance (P> 0.05), carcass traits (P> 0.05) and lipid profile (P> 0.05).Therefore, it was characterized the beneficial effect of ractopamine on reducing the average consumption ration in the growth phase and increased average daily weight gain and decreased average daily consumption of feed during the finishing phase . / O objetivo deste trabalho foi avaliar o efeito da ractopamina e arginina sobre o desempenho, características de carcaça, perfil lipídico e característica histológica de fígado em suínos em crescimento e terminação. O delineamento experimental foi em blocos casualisados, com três tratamentos, oito repetições, dois animais por unidade experimental, perfazendo um total de 24 animais(12 suínos machos castrados e 12 fêmeas), com 65 dias de idade e peso vivo médio 32 ± 0,75 quilogramas.Os tratamentos foram: T1: controle (C): dieta isoenergética e isocalórica; T2: C + 4 ppm de ractopamina e T3: C + 0,8% de arginina. Os aditivos ractopamina e arginina foram adicionados às rações fareladas e estas fornecidas ad libitum por 89 dias sendo 46 dias da fase crescimento e 43 dias da fase terminação. Ao atingirem 150 dias de idade, os animais foram abatidos. Avaliou-se o desempenho animal (consumo médio diário de ração, ganho médio diário em peso e conversão alimentar) pesando-se os animais no início e final de cada fase e as rações oferecidas. No momento do abate foram colhidas amostras de sangue para análises bioquímicas de perfil lipídico e cortes de fígado para exame histológico. As carcaças foram pesadas quentes e após 24 horas de resfriadas, foram medidos o comprimento de carcaça, espessura de toucinho e a área de olho-de-lombo. A suplementação de ractopamina diminuiu o consumo médio de ração na fase de crescimento e terminação (P<0,05) e o ganho médio diário de peso nas fases de terminação(P<0,05) sem, contudo alterar as outras variáveis como as características de carcaça (P>0,05) e perfil lipídico (P>0,05). A inclusão de arginina não alterou o desempenho (P>0,05), característica da carcaça (P>0,05) e perfil lipídico(P>0,05). Portanto, ficou caracterizado o efeito benéfico da ractopamina sobre a diminuição do consumo médio de ração na fase de crescimento e terminação e o aumento do ganho médio de peso diário na fase de terminação

aditivo alimentar

agonista &#946

-adrenérgico

carcaça suína

desempenho animal

perfil lipídico

food additive

beta-adrenergic agonist

carcass

performance

lipid profile

CNPQ::CIENCIAS BIOLOGICAS::BIOQUIMICA

Contrôle de la voie de l’AMPc vasculaire par les phosphodiestérases en situation physiopathologique. / Contribution of the phosphodiesterases in the regulation of vascular cAMP in pathophysiological situation

Belacel Ouari, Milia

08 December 2016

L’AMPc est un second messager exerçant un rôle vasculoprotecteur majeur, par ses effets relaxants et inhibiteurs de la prolifération et de la migration cellulaires. Les concentrations intracellulaires d’AMPc sont finement régulées par leur synthèse via les adénylates cyclases et leur dégradation par les phosphodiestérases (PDEs). Nous avons évalué l’impact de l’environnement cellulaire sur la voie de signalisation couplée au récepteur β-adrénergique (β-AR/AMPc/PDE) dans les cellules musculaires lisses vasculaires (CMLVs), ainsi que les altérations potentielles de celle-ci en situation pathologique d’insuffisance cardiaque (IC).Notre première étude montre que dans les CMLs d’aorte de rat en culture, adoptant un phénotype synthétique, la voie de signalisation β-AR/AMPc/PDE est hautement modulée par la densité cellulaire Ainsi, une faible densité cellulaire est associée à une régulation négative de l’expression fonctionnelle du récepteur β1-AR, à une activité hydrolytique des PDEs-AMPc plus faible et à des concentrations d’AMPc intracellulaire plus élevées que celles observées dans des cellules confluentes.Notre deuxième étude montre que dans l’aorte de rat, l’IC est associée à une dysfonction endothéliale (DE), une hyperréactivité aux agents contractants et une altération de la fonction et de l’expression des PDEs-AMPc. Nos résultats suggèrent que l’altération de la voie du NO/GMPc suite à la DE conduit à une hyper-activation de la PDE3, qui masque la fonction de la PDE4 et altère la relaxation β-AR.L’ensemble de ce travail met en évidence le rôle critique de l'environnement cellulaire dans le contrôle de la voie β-AR/AMPc/PDE des CMLVsMots clés : Muscle lisse vasculaire, récepteur β-adrénergique, AMPc, phosphodiestérases, densité cellulaire, insuffisance cardiaque / CAMP is second messenger which plays a prominent vasculoprotective role by its relaxing effects and inhibition of cell proliferation and migration. Intracellular cAMP level is regulated by its synthesis by adenylate cyclase and its degradation by phosphodiesterases (PDEs). We evaluated the influence of cellular environment on signaling pathway coupled to β-adrenoceptors (β-AR/cAMP/PDE) on vascular smooth muscle cells (VSMCs), as well as potential alterations in heart failure (HF).The first study showed that in cultured rat aortic SMCs exhibiting synthetic phenotype, the β-AR/cAMP/PDE signaling pathway is highly modulated by the cellular density.Thus, the low density state being associated to a downregulation of the β1-AR, a lower cAMP-PDE activity and a higher basal [cAMP]i compared to confluent cells.Our second study showed that in rat aorta, HF is associated with endothelial dysfunction, hyper-reactivity to contractile agents and an alteration of function and expression of cAMP-PDEs. Our results suggest that NO/cGMP pathway alteration following the ED in HF leads to hyper-activation of PDE3 which masks PDE4 function and alters β-adrenoceptor relaxationThus, our works highlights the critical role of the cellular environment in controlling the vascular β-AR signaling.Keywords: Vascular smooth muscle, β-adrenoceptor, cAMP, phosphodiesterases, cellular density, heart failure.

Cellule musculaire lisse vasculaire

Signalisation

AMPc

Récepteurs béta-Adrénergiques

Phosphodiestérases

Vascular physiology and pathophysiology

Vascular smooth muscle cell

Signaling

Camp

Beta-Adrenergic receptors

Phosphodiesterases

Metabolic Mechanisms in Physiologic and Pathologic Oxygen Sensing

Stephens, Olivia R.

28 August 2019

No description available.

Biology

Biomedical Research

Molecular Biology

Physiology

beta-adrenergic receptor

hypoxia-inducible factor

mitochondria

pulmonary hypertension

metabolism

hypoxia

beta-blocker

microparticles

pulmonary arterial hypertension

Charakterisierung kardialer β-Adrenozeptoren in B.U.T. Big 6 Puten in Abhängigkeit von Alter und Geschlecht: Bedeutung für die Entstehung kardiovaskulärer Erkrankungen

Hoffmann, Sandra

24 January 2017

Einleitung: / Introduction:

info:eu-repo/classification/ddc/636.089

ddc:636.089

Vliv akutního chladu a stálého světla na levou komoru srdce potkana / The effect of acute cold and permanent light to left ventricular of the rat heart

Vítková, Ivana

January 2018

Acute cold exposure increases the risk of sudden cardiac events, similarly exposure to constant light negatively affects the cardiovascular system. However, the individual effects of these factors and the effect of their combination on cardiomyocytes are not yet known. The thesis deals with the influence of a 3 day cold exposure and constant light on the expression of β-adrenergic receptors and associated G-proteins in association with apoptotic signals in the left ventricle of the Wistar rat heart. In this work apoptotic proteins BAX, BCL2, caspase 8 and important components of β-adrenergic signalization - β1, β2, G-proteins, Gas, Gi1/2 and Gi3 were determined. The relative expression of the proteins was analyzed by Western blotting. The results confirm the detrimental effect of cold and light exposure. However, the synergistic effect of these two stressors shows surprising results.

Vliv chronického působení morfínu na funkci signálních systémů řízených trimérními G-proteiny v srdci potkana / Effect of chronic morphine treatment of rats on myocardial signaling systems regulated by trimeric G-proteins

Škrabalová, Jitka

January 2011

It has recently been discovered that the effect of morphine can significantly reduce the tissue damage that occurs during myocardial ischemia. The molecular mechanisms by which morphine acts on the heart are still little understood. The aim of this thesis was to monitor the effect of chronic 27-day and 10-day administration of low (1 mg/kg/day) and high (10 mg/kg/ day) doses of morphine on the expression of selected G-protein-coupled receptors (GPCR) and on the expression and activity of adenylyl cyclase (AC). Chronic (27 days) morphine treatment reduced the expression of к-opioids receptors, but 10-day morphine exposure did not influence the expression of these receptors. Assessment of β1- and β2-AR by immunoblot technique did not show any significant change in the expression, but the more accurate determination of β-AR expression using the saturation binding studies revealed that 27-day treatment with high doses of morphine appreciable increased the total number of these receptors. Administration of high doses of morphine led to marked up-regulation of adenylyl cyclase (AC) isoforms V/VI, and the amount of AC decreased proportionally with the time of discontinuation of morphine administration. Low doses of morphine up- regulated AC only during 27-day administration. Chronic morphine exposure did...

Thrombolytic therapy and beta-adrenergic blockade in acute myocardial infarction : a prospective evaluation at Groote Schuur Hospital 1988-1990

Green, Belinda K W

January 1991

The advent of intravenous thrombolytic agents has revolutiontzed the management of patients with acute myocardial infarction and has dramatically altered the morbidity and mortality associated with this condition. The aims of this study in patients presenting with acute myocardial infarction and treated with thrombolytic agents are: 1. To evaluate the efficacy of thrombolytic agents used at Groote Schuur Hospital in terms of (a) patency of the infarct related artery; ( b) short and long-term mortality. 2. To assess the feasibility and safety of combining intravenous beta-adrenergic blockade with intravenous thrombolytic therapy in patients presenting with acute nyocardial infarction. 3. To assess the need for coronary angiography in all patients treated with thrombolytic agents for acute myocardial infarction. 4. To assess the effect on mortality of offering coronary angioplasty or coronary artery bypass grafting only to those patients manifesting spontaneous or inducible ischaemia post infarction.