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Efeitos dos hormônios tireoidianos sobre a regulação da expressão de proteínas envolvidas com a lipólise no tecido adiposo branco subcutâneo e visceral. / Effects of thyroid hormones on the regulation of the expression of proteins involved on lipolysis in subcutaneous and visceral white adipose tissue.Mariana de França Oliveira da Silva 21 August 2015 (has links)
Os hormônios tireoidianos (HT) executam um papel lipolítico importante no Tecido Adiposo Branco (TAB), sendo este efeito mediado por meio do aumento da expressão de receptores beta adrenérgicos na membrana do adipócito, o que aumenta a sensibilidade deste tecido as catecolaminas. Sabe-se que os principais efetores da ação lipolítica nesse tecido são a lipase hormônio sensível (LHS) e a lipase dos triglicerídeos dos adipócitos (ATGL), as quais hidrolisam os triglicerídeos em ácidos graxos e glicerol. Além disso, outros componentes estão envolvidos na atividade lipolítica, como as perilipinas, proteínas estas que envolvem a gota de gordura, formando uma barreira contra a ação da LHS e ATGL, de modo que precisam ser fosforiladas para que a LHS e ATGL possam exercer seu efeito lipolítico. Considerando: (a) a importância do tecido adiposo na homeostase energética e como fonte de citocinas, as quais estão relacionadas com a sensibilidade tecidual à insulina; (b) que a função e o metabolismo do tecido adiposo variam com a sua distribuição regional, e (c) que as ações lipolíticas dos HT, importantes reguladores da homeostase energética, têm sido muito pouco exploradas, pretendemos investigar, em ratos, (i) se os HT interferem na expressão da LHS, ATGL, perilipina A e dos receptores beta3 adrenérgicos no tecido adiposo branco, e (ii) se essas ações diferem nos distintos depósitos de gordura, o que poderia ampliar o campo de conhecimento sobre os efeitos lipolíticos destes hormônios e a nossa compreensão sobre a contribuição deles nas complicações associadas à obesidade e suas co-morbidades. / Thyroid hormones (TH) play an important lipolytic role in white adipose tissue (WAT). This effect is mediated by increased expression of beta-adrenergic receptors on adipocytes membrane, which increases the sensitivity of that tissue to catecholamines. It is known that the main effectors of the lipolytic action in WAT enzymatic activity, especially: hormone sensitive lipase (HSL) and adipose triglyceride lipase (ATGL), which hydrolyze triglycerides into fatty acids and glycerol. In addition, other components are involved in the lipolytic activity, such as perilipin. These proteins support the fat droplet, forming a protective barrier against HSL and ATGL action. Considering: (a) the importance of adipose tissue in energy homeostasis and as a source of cytokines which are related to insulin tissue sensitivity; (b) function and metabolism of adipose tissue vary with their regional distribution; and (c) lipolytic actions of HT, important regulators of energy homeostasis, have been little explored, we investigated in rats with hypothyroidism and submitted to T3 treatment: (i) TH effects on the expression of hormone sensitive lipase (HSL), adipose triglyceride lipase (ATGL),perilipin A and beta-3 adrenergic receptors in WAT, and (ii) if this action are different on subcutaneous and visceral fat depot. This study has increased our understanding about the contribution of these hormones on WAT metabolism and metabolic disease as obesity.
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Efeito do agonista b2-adrenérgico formoterol na regeneração muscular de ratos idosos. / Effect of the b2-adrenoceptor agonist formoterol on skeletal muscle regeneration of aged rats.Lucila Hernandes da Silva 01 March 2012 (has links)
Músculos esqueléticos de ratos idosos apresentam uma reduzida capacidade de se regenerar após lesão. No presente estudo, nós lançamos a hipótese de que a estimulação farmacológica de adrenoceptores b2 em músculos de ratos idosos lesados poderia melhorar a regeneração destes. Ratos jovens e idosos foram tratados com injeção subcutânea do agonista b2-adrenérgico formoterol (2 mg/kg/dia) durante 10 e 21 dias após lesão do músculo sóleo. Os músculos de ratos idosos lesados e tratados com formoterol por 10 e 21 dias apresentaram menor processo inflamatório e fibras musculares em regeneração com maior calibre quando comparados aos músculos apenas lesados. O tratamento com formoterol preveniu a queda da força tetânica e aumentou a síntese de proteínas e a fosforilação de mTOR em músculos de ratos idosos lesados e avaliados após 10 dias. Nossos resultados sugerem que o formoterol melhora a capacidade regenerativa estrutural e funcional dos músculos esqueléticos de ratos idosos, e que esse efeito é mediado pelo aumento da síntese protéica através da ativação de mTOR. / Skeletal muscles from old rats fail to completely regenerate following injury. In the present work, we hypothesized that pharmacological stimulation of b2-adrenoceptors in aged muscles following injury could improve their regenerative capacity. Young and aged rats were treated with a subcutaneous injection of b2-adrenergic agonist formoterol (2 mg/kg/day) up to 10 and 21 days after soleus muscle injury. Formoterol-treated muscles from old rats evaluated at 10 and 21 days post-injury showed reduced inflammation and regenerating myofibers of greater caliber when compared to their injured controls. Formoterol minimized the decrease in tetanic force and increased protein synthesis and mTOR phosphorylation in old muscles at 10 days post-injury. Our results suggest that formoterol improves structural and functional regenerative capacity of regenerating skeletal muscles from aged rats by increasing protein synthesis via mTOR activation.
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Ações da metilecgonidina sobre a síntese de melatonina na glândula pineal de ratos. / Actions of the metilecgonidine on the syntesis of melatonin in the pineal gland of rats.Livia Silva Medeiros de Mesquita 19 April 2012 (has links)
A glândula pineal sintetiza o hormônio melatonina no período escuro. No rato, a ativação dos receptores a e b-adrenérgicos aumenta os níveis de AMPc, levando à síntese e ativação da enzima arilalquilamina-N-acetiltransferase (AANAT). A glândula recebe também inervação parassimpática, sendo inibitório o efeito da acetilcolina. A metilecgonidina (AEME) é o produto da pirólise da cocaína, quando esta é usada sob a forma de \"crack\". Neste trabalho estudamos os efeitos e os mecanismos de ação da AEME sobre a síntese da melatonina. Foram investigados a atividade da AANAT, o Ca2+, o AMPc e a viabilidade celular e a fragmentação do DNA. A AEME reduziu a síntese da melatonina in vivo e in vitro, sendo este efeito revertido pela atropina. A AEME induziu um aumento do Ca2+, não alterando o AMPc e a atividade da AANAT. A viabilidade celular e fragmentação do DNA não foram modificadas pela AEME. Em conclusão, a AEME reduz a síntese da melatonina, in vitro e in vivo, e a sua ação se dá por interferir com o sistema colinérgico muscarínico. / The pineal gland synthesizes the hormone melatonin in the dark. In rats, the activation of a and b-adrenergic receptors increases cAMP levels and the synthesis and activity of arylalkylamine-N-acetyltransferase enzyme (AANAT). The pineal gland is also innervated by parasympathetic fibers, being inhibitory the effect of acetylcholine. Methylecgonidine (AEME) is the pyrolysis product of cocaine when it is used as \"crack.\" In this work we studied the effects of AEME on the melatonin synthesis, in vitro and in vivo. We investigated AANAT activity, iCa2+, cAMP, cell viability and DNA fragmentation. AEME reduced melatonin synthesis in vivo and in vitro, and this effect was reversed by atropine. There was an increase in Ca2+, but not in cAMP or AANAT activity induced by AEME. Cell viability and DNA fragmentation were not affected by AEME. In conclusion, AEME reduced melatonin synthesis in vitro and in vivo, being this effect mediated by the muscarinic cholinergic system.
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Generalized anxiety disorder in the elderly : role of bio-environmental factors and genetic vulnerability / Anxiété généralisée du sujet âgé : rôle des facteurs bio-environnementaux et de la vulnérabilité génétiqueZhang, Xiaobin 23 September 2016 (has links)
Le trouble anxieux généralisé (TAG) est un problème majeur de santé publique. Il est fréquemment sous ou mal diagnostiqué, notamment chez les personnes âgées. Il est souvent comorbide et source d’incapacité et présente un faible taux de rémission complète. Malgré des conséquences socio-économiques et sanitaires importantes, les recherches sur les déterminants du TAG en population générale âgée restent limitées. L'objectif de cette thèse était d’étudier les caractéristiques cliniques et étiologiques du TAG à partir de l'étude prospective ESPRIT, constituée de 2259 personnes âgées de 65 ans et plus et examinées à 6 reprises pendant 12 ans.La prévalence du TAG des 6 derniers mois était de 4,6 %, 14% des cas présentant une comorbidité avec une dépression majeure et 35% avec une phobie mais les facteurs associés sont différents. Au cours des 12 ans de suivi, 8,4% des participants ont présenté un TAG incident (10 pour 1000 personnes-années), qui était un premier épisode dans 80% des cas. Plusieurs facteurs prédictifs de TAG ont été identifiés à partir de modèles statistiques multivariés : le sexe féminin, la survenue d’événements de vie stressants récents ou anciens (pendant l’enfance), certaines maladies chroniques (troubles respiratoires, cognitifs, arythmie et insuffisance cardiaque, dyslipidémie, adiposité) et troubles psychiatriques (dépression majeure, phobie, antécédents de TAG). Certains variants génétiques des récepteurs adrénergiques augmentent le risque de TAG (mais pas de phobie) et peuvent moduler l'effet des événements stressants. Le TAG apparaît comme un trouble affectif multifactoriel lié au stress résultant de facteurs de risque proximaux et distaux et cliniquement distinct des autres troubles psychiatriques majeurs de la personne âgée.Ce travail apporte de nouvelles connaissances sur les déterminants du TAG avec des implications cliniques en termes de diagnostic et d’étiologie. Il pourrait permettre le développement de stratégies originales de prévention et d'intervention chez le sujet âgé, avec des conséquences majeures en santé publique. / Generalized anxiety disorder (GAD) is a major public health concern. It is frequently under-recognized or misdiagnosed, especially in the elderly. It is associated with high comorbidity and disability, and a low rate of full remission. Despite substantial socioeconomic and public health consequences, there has been little research to identify GAD determinants in general elderly populations. The aim of this thesis was to provide a deeper understanding of the clinical characteristics and risk factors for GAD in late life from the prospective ESPRIT study of 2259 community-dwelling French elderly (aged 65 years and over) examined six times over 12 years.The 6-month current prevalence of GAD was 4.6%, 14% of the cases were comorbid with major depression and 35% with phobia but the factors associated with these disorders differed. During the 12-year follow-up, 8.4% of the participants experienced incident GAD (10 per 1000 person-years) of which 80% were first episodes. Multivariate statistical models showed that the main predictors for late-life GAD were being female, reporting recent and childhood adverse life events, having chronic physical (respiratory disorders, arrhythmia and heart failure, cognitive impairment, dyslipidemia, and adiposity), and mental (major depression, phobia, and past GAD) disorders. Specific genetic variants of adrenergic receptors increase the risk of GAD (but not phobia) and moderate the effect of adverse life events. GAD can be characterized as a multifactorial stress-related affective disorder resulting from both proximal and distal risk factors, and is clinically distinct from other major psychiatric disorders in the elderly.This work provides new knowledge on GAD determinants with clinical implications for diagnosis and etiology. It could also contribute to developing novel preventative and intervention strategies in the elderly, with major potential consequences for overall health and daily functioning.
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Úloha beta 1 adrenergních receptorů v srdci chladově adaptovaného potkana / The role of beta1 adrenergic receptors in heart of cold acclimated ratLiptáková, Andrea January 2020 (has links)
During cold acclimation the heat production is shifted from shivering to non-shivering thermogenesis, which is mediated by adrenergic signaling. It has also been observed, that cold acclimation may increase the organismal resistence to pathological stimuli and may affect functional parameters of cardiovascular system. However, acute exposure to sever cold is often associated with detrimental effects on the body. We have recently shown that chronic exposure to cold increases the heart's resistance to ischemia-reperfusion injury without negative side effects when mild temperatures are used, however the mechanism of protection is not yet known. The aim of this work was to determine whether: i) if the sensitivity of the heart to ischemia changes already after the first day of cold exposure and does not show any negative effects, ii) if β1-adrenergic signaling plays a role in chronic regimen of cold-induced cardioprotection. The results of this work showed that i) one day of exposure to mild cold did not change the sensitivity of the heart to ischemia and ii) metoprolol treatment reduced the infarct size in the control group, but did not affect the heart of cold-adapted rats. Key words : Heart, rat, beta 1 adrenergic receptors, cold acclimation
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Vliv endogenních faktorů na mezenchymální kmenové buňky / Effect of endogenous factors on mesenchymal stem cellsČerná, Kristýna January 2020 (has links)
Maintaining of homeostasis is essential for the survival of the organism. Stress disturbs the homeostasis and prepares the organism for mental or physical stress. During the stress situation, the endogenous stress factors are released. Through these factors stress affects tissue regeneration, the immune system and other metabolic processes. Chronic stress impacts many parts of body and mind and has a negative effect on these processes. Acute stress has the opposite effect. Mesenchymal stem cells (MSCs) participate in regenerative processes and modulate the immune system. Therefore, it can be assumed that stress will affect on MSCs. The aim of this study was to investigate the effect of stress factors, norepinephrine and corticosterone on the properties and function of MSCs in acute and chronic stress model. In our study, stress factors did not affect the morphology, vitality and differentiation of MSCs. However, the metabolic activity of MSCs was reduced regardless of the duration of their action. The action of stress factors also affected the production of some immunologically relevant molecules and proteins. Unfortunately, the results did not show a clear effect of stress factors on the lymphocyte modulation by MSCs. Key words: mesenchymal stem cells, catecholamines, adrenergic receptors,...
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The Role of Osteopontin in Extracellular Matrix Remodeling Following Chronic Sympathetic Stimulation in The Aging HeartDavis, Danisha Marie, Dalal, Suman, James, Connor, Foster, Cerrone R., Singh, Krishna 12 April 2019 (has links)
Cardiovascular disease (CVD) is the leading cause of death in the United States. A common feature in most cardiac pathologies is the dysregulation of beta-adrenergic receptors (β-AR) and changes in the extracellular matrix (ECM). The ECM maintains strength and normal organization of cardiac tissue, while fibrosis (connective tissue scarring) is necessary for repair of damaged cardiac tissue. However, the dysregulation of the ECM leads to a number of cardiac disease pathologies. Osteopontin (OPN) is a protein with diverse biological functions in regulating the ECM such as bone resorption and calcification, wound healing, cell adhesion, cell survival, and apoptosis. OPN is expressed at low levels in the heart but increases with injury by promoting collagen synthesis, cardiac fibroblast growth, and adhesions to ECM proteins. Furthermore, as the heart ages, increases in ECM reorganization leads to cardiac damage and failure. Several studies have examined the role of OPN in the heart, but to date, no studies exist on the role of OPN in response to β-AR signaling and cardiac remodeling or the role that aging plays in this response. The goal of this study was to examine the effects of OPN on cardiac ECM remodeling following chronic beta-adrenergic stimulation. We proposed that OPN expression increases cardiac remodeling and dysfunction following ISO treatment in the aging heart evidenced by increased fibrosis. For this study, young (4 months) and middle age (14 months) mice with (WT) and without (KO) the OPN gene were treated with isoproterenol (ISO) for 28 days. Echocardiography was used to assess cardiac function. Mice were euthanized, and the hearts were analyzed for fibrosis using Masson’s Trichrome Staining. Results showed ISO increased fibrosis in the WT-ISO, but not KO-ISO compared to the respective controls (SHAM, no ISO treatment) for the middle age mice (p≤0.05). Furthermore, the aged WT-ISO group exhibited a 3-fold increase in fibrosis compared to the young WT-ISO group. Results from echocardiography will be analyzed and we expect to see compromised cardiac function in the WT-ISO groups compared to KO-ISO groups. OPN is currently being examined as a potential biomarker in heart failure. The results from this study will provide new insight on changes in the cardiac vasculature in the aging heart following injury and the role OPN plays in this process.
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Β-Adrenergic Receptor-Stimulated Apoptosis in Cardiac Myocytes Is Mediated by Reactive Oxygen Species/C-Jun NH<sub>2</sub>-Terminal Kinase-Dependent Activation of the Mitochondrial PathwayRemondino, Andrea, Kwon, Susan H., Communal, Catherine, Pimentel, David R., Sawyer, Douglas B., Singh, Krishna, Colucci, Wilson S. 07 February 2003 (has links)
Stimulation of β-adrenergic receptors (βARs) causes apoptosis in adult rat ventricular myocytes (ARVMs). The role of reactive oxygen species (ROS) in mediating βAR-stimulated apoptosis is not known. Stimulation of βARs with norepinephrine (10 μmol/L) in the presence of prazosin (100 nmol/L) for 24 hours increased the number of apoptotic myocytes as determined by TUNEL staining by 3.6-fold. The superoxide dismutase/catalase mimetics Mn(III)tetrakis(1-methyl-4-pyridyl)porphyrin pentachloride (MnTMPyP; 10 μmol/L) and Euk-134 decreased βAR-stimulated apoptosis by 89±6% and 76±10%, respectively. Infection with an adenovirus expressing catalase decreased βAR-stimulated apoptosis by 82±15%. The mitochondrial permeability transition pore inhibitor bongkrekic acid (50 μmol/L) decreased βAR-stimulated apoptosis by 76±8%, and the caspase inhibitor zVAD-fmk (25 μmol/L) decreased βAR-stimulated apoptosis by 62±11%. βAR-stimulated cytochrome c release was inhibited by MnTMPyP. βAR stimulation caused c-Jun NH2-terminal kinase (JNK) activation, which was abolished by MnTMPyP. Transfection with an adenovirus expressing dominant-negative JNK inhibited βAR-stimulated apoptosis by 81±12%, and the JNK inhibitor SP600125 inhibited both βAR-stimulated apoptosis and cytochrome c release. Thus, βAR-stimulated apoptosis in ARVMs involves ROS/JNK-dependent activation of the mitochondrial death pathway.
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Angiotensin II Potentiates Adrenergic and Muscarinic Modulation of Guinea Pig Intracardiac NeuronsGirasole, Allison E., Palmer, Christopher P., Corrado, Samantha L., Southerland, Elizabeth Marie, Ardell, Jeffrey L., Hardwick, Jean C. 01 November 2011 (has links)
The intrinsic cardiac plexus represents a major peripheral integration site for neuronal, hormonal, and locally produced neuromodulators controlling efferent neuronal output to the heart. This study examined the interdependence of norepinephrine, muscarinic agonists, and ANG II, to modulate intrinsic cardiac neuronal activity. Intracellular voltage recordings from whole-mount preparations of the guinea pig cardiac plexus were used to determine changes in active and passive electrical properties of individual intrinsic cardiac neurons. Application of either adrenergic or muscarinic agonists induced changes in neuronal resting membrane potentials, decreased afterhyperpolarization duration of single action potentials, and increased neuronal excitability. Adrenergic responses were inhibited by removal of extracellular calcium ions, while muscarinic responses were inhibited by application of TEA. The adrenergic responses were heterogeneous, responding to a variety of receptor-specific agonists (phenylephrine, clonidine, dobutamine, and terbutaline), although α-receptor agonists produced the most frequent responses. Application of ANG II alone produced a significant increase in excitability, while application of ANG II in combination with either adrenergic or muscarinic agonists produced a much larger potentiation of excitability. The ANG IIinduced modulation of firing was blocked by the angiotensin type 2 (AT 2) receptor inhibitor PD 123319 and was mimicked by the AT 2 receptor agonist CGP-42112A. AT 1 receptor blockade with telmasartin did not alter neuronal responses to ANG II. These data demonstrate that ANG II potentiates both muscarinically and adrenergically mediated activation of intrinsic cardiac neurons, doing so primarily via AT 2 receptor-dependent mechanisms. These neurohumoral interactions may be fundamental to regulation of neuronal excitability within the intrinsic cardiac nervous system.
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Alpha-1-Adrenergic receptors as new targets in NeuroblastomaBroso, Francesca 11 October 2021 (has links)
High-risk neuroblastoma (NB) is an aggressive childhood tumor that originates from progenitor neural crest cells. Even if the therapeutic protocol for NB is articulate and aggressive, the outcome remains dismal, with the 5-year disease-free overall survival below rating 50%. A novel drug combination strategy can possibly provide a new solution to this unmet therapeutic need. 13-cis retinoic acid (13-cis-RA, isotretinoin) is an anti-proliferative and pro-differentiative agent currently used in the post-consolidation phase of NB therapy. To identify molecules able to potentiate the anti-proliferative activity of 13-cis-RA, NB cells were treated with a library of 169 naturally occurring polyphenols in combination with the retinoid. This in vitro screen led to the identification of isorhamnetin as a synergistic partner of 13-cis-RA, producing an 80% reduction in cell viability. At the molecular level, this synergistic effect is followed by a marked increase in the expression of a member of the catecholamine receptor superfamily: the adrenergic receptor alpha-1B (ADRA1B) suggesting that this receptor might represent a key mediator of the synergistic effect of 13-cis-RA and isorhamnetin observed in vitro. This finding redirected our attention to the class of adrenergic receptors (ARs) as novel targets in NB. To investigate the role of ADRA1B in the synergism, we generated CHP134 NB cell lines knocked-out (KO) for the receptor and observed that exposure of CHP134 KO cell to 13-cis-RA leads to a reduction of cell viability and neural differentiation. We, therefore, substituted the genetic KO strategy with the alpha-1B adrenergic antagonist, L765,314, obtaining the same results. Subsequently, we extended the analysis on the role of adrenergic receptors (AR) performing a biased screen using two libraries of AR-ligands. The screen results confirm that the molecules working as alpha-1-ARs antagonists are those that greatly increase cell sensitivity to 13-cis-RA with reduction of cell viability and increase in differentiation. We confirmed our observation in NB xenograft mice models in vivo, treating mice with a combination of 13-cis-RA and the FDA approved alpha-1 AR antagonist doxazosin. The proposed pharmacological treatment was effective in slowing tumor growth, leading to tumors of smaller size. From our results, we can conclude that the deletion or inhibition of alpha-1-AR sensitizes NB cells to 13-Cis-RA, both in terms of induction of apoptosis and neural differentiation. Since NB is a catecholamine-rich tumor, we propose that antagonization of alpha-1-AR disrupts the established autocrine pro-survival circuit generated by catecholamines in NB and restores the ability of the cells to follow the pro-differentiative and pro-apoptotic programs endorsed by 13-cis-RA. Considering the druggable nature of the alpha-1-AR receptors, we indicate this class of receptors as a novel pharmacological target for the treatment of neuroblastoma.
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