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  • About
  • The Global ETD Search service is a free service for researchers to find electronic theses and dissertations. This service is provided by the Networked Digital Library of Theses and Dissertations.
    Our metadata is collected from universities around the world. If you manage a university/consortium/country archive and want to be added, details can be found on the NDLTD website.
31

Investigação funcional e molecular dos adrenoceptores alfa-1 em modelo experimental de epididimite em ratos

Mueller, Andre January 2019 (has links)
Orientador: André Sampaio Pupo / Resumo: Primordialmente, o epidídimo funciona para proteger e realizar a maturação de espermatozoides. A cauda do epidídimo (CE), região que armazena espermatozoides maduros até a ejaculação, recebe densa inervação de fibras pós-ganglionares simpáticas que liberam noradrenalina para contrair o músculo liso do epidídimo via ativação de adrenoceptores alfa-1A (alfa-1A-ARs). As contrações da musculatura lisa têm papel importante no transporte dos espermatozoides ao longo do ducto epididimário, bem como na contração da CE distal durante a fase de emissão seminal da ejaculação. Recentemente, foi demonstrado que a epididimite, a condição inflamatória do epidídimo, induz aceleração do tempo de trânsito espermático em ratos. Nesta tese, testamos a hipótese de que essa aceleração do trânsito espermático induzida pela epididimite é resultado de alterações na contratilidade do ducto epididimário. Dessa forma, o objetivo deste estudo foi investigar a contração da CE distal mediada por alfa-1-ARs em um modelo experimental de epididimite aguda induzida pelo lipopolissacarídeo (LPS) de E. coli em ratos. Após 6 e 24 h da injeção intraductal de LPS (25 µg) para indução da epididimite (in vivo), estudos de contração indicaram que a potência da noradrenalina aumentou ~6 vezes na CE distal inflamada. As contrações induzidas pela noradrenalina foram competitivamente antagonizadas pelo prazosin, um antagonista não-seletivo de alfa-1-ARs, com afinidades semelhantes nos grupos tratados com LPS e salina (pA2... (Resumo completo, clicar acesso eletrônico abaixo) / Abstract: The epididymis works primarly to protect and mature the spermatozoon. The cauda epididymis (CE), which stores mature spermatozoa until ejaculation, is densely innervated by sympathetic postganglionic fibers that release noradrenaline to contract epididymal smooth muscle via activation of alpha-1A adrenoceptors (1A-ARs). The smooth muscle contractions have an important role for the adequate transport of spermatozoa within the epididymal duct, as well as for distal CE contraction during the seminal emission phase of ejaculation. It was recently shown that epididymitis, the inflammatory condition of the epididymis, induces acceleration of the sperm transit time in the rat epididymis. We hypothesize that this epididymitis-induced sperm transit time acceleration is due to changes in the contractility of the epididymal duct. Thus, the aim of this study was to investigate the 1-ARs-mediated contraction of the distal CE in an experimental model of acute epididymitis in rats induced by lipopolysaccharide (LPS) from E. coli. Contraction studies indicated that the potency of noradrenaline increased ~6-fold in the inflamed distal CE at 6 h post-intravasal LPS injection. Noradrenaline-induced contractions were competitively antagonized by prazosin, a non-selective 1-ARs antagonist, with similar affinities in both LPS- and saline-treated groups (pA28.9). However, the potency of BMY 7378, a selective 1D-ARs antagonist, was ~50-fold higher in the distal CE treated with LPS (pA2 LPS = 8.... (Complete abstract click electronic access below) / Doutor
32

Basis for a sympatholytic approach in the treatment of human heart failure

Aggarwal, Anuradha, 1964- January 2002 (has links)
Abstract not available
33

Blood Flow Regulation and Inflammatory Response in Experimental Models of Diabetes

Pettersson, Ulrika January 2012 (has links)
Type 2 diabetes is caused by defect pancreatic islet β-cells together with peripheral insulin resistance. The disease is often accompanied by obesity with associated low-grade visceral adipose tissue inflammation, which contributes to insulin resistance. As a consequence of, and a possible compensation for the increased insulin demand, blood flow to the pancreatic islets is increased in animal models of diabetes. This increased blood perfusion might with time affect the vascular network as well as β-cells within the islets. This thesis investigates the role of changes of blood perfusion in pancreatic islets and adipose tissues, as well as the recruitment to and composition of leukocyte subpopulations in insulin-sensitive tissues in experimental models of diabetes. Blood flow measurements in islets and adipose tissues of rats and mice were performed using the microsphere technique, while leukocyte recruitment was studied in the mouse cremaster muscle using intravital microscopy. Increased islet blood flow was observed in the GK rat model of type 2 diabetes, which was decreased by acute as well as continuous 2-week inhibition of β3-adrenoceptors without affecting plasma insulin concentrations. Increased inflammatory leukocyte recruitment was observed in both alloxan-induced and high-fat diet-induced diabetes. However, an impaired bacterial clearance was observed in diabetic mice, which was due to impaired phagocytosis. A gender difference was detected in mice fed a high-fat diet, since obese female mice did not show increased levels of pro-inflammatory circulatory markers or inflammatory leukocytes in the adipose tissue. The main effector cell in the adipose tissue inflammation in high-fat-fed male mice seemed to be the pro-inflammatory macrophage. The Treg population in adipose tissue was increased in female mice, but remained unchanged in male mice on high-fat diet. In conclusion, increased islet blood flow in type 2 diabetes could be reversed by β3-adrenoceptor inhibition, which may maintain islet function. The diabetes-associated hyperglycemia activated leukocytes but impaired their phagocytic ability. High-fat-fed female mice showed less peripheral inflammation due to a smaller number of recruited inflammatory macrophages and a high-fat diet-induced Treg population in intra-abdominal adipose tissues.
34

Enhanced adrenergic sensitivity of mesenteric veins comparied to arteries and its relation to calcium utilization and handling

Hiavacova, Alexandra. January 2008 (has links)
Thesis (Ph.D.)--Michigan State University. Dept. of Pharmacology and Toxicology, 2008. / Title from PDF t.p. (viewed on July 10, 2009) Includes bibliographical references (p. 226-256). Also issued in print.
35

Effect of ovariectomy and estrogen replacement on the [beta]-Adrenergic receptor signaling pathway and intracellular Ca2+ homeostasis in the rat heart

Kam, Wan-lung, Kenneth. January 2005 (has links)
Thesis (Ph. D.)--University of Hong Kong, 200 . / Title proper from title frame. Also available in printed format.
36

Adrenoceptores- alfa-1 envolvidos na contração da aorta abdominal em modelo experimental de pré-eclâmpsia em ratas

Silva, Katiussia Pinho da January 2016 (has links)
Orientador: André Sampaio Pupo / Resumo: A Pré-eclâmpsia (PE) é uma desordem hipertensiva gestacional, cuja fisiopatologia tem sido atribuída a forte resposta inflamatória, disfunção endotelial, agregação plaquetária e aumento da resistência vascular. Estudos com PE relatam inadequado aumento na ação de vários vasoconstritores, incluindo endotelina, adenosina, angiotensina II, e noradrenalina ocasionando aumento da pressão arterial. De fato, o sistema nervoso autonômo simpático através do neurotransmissor noradrenalina regula a pressão arterial mediante a ativação dos adrenoceptores-alfa-1 (ARs-alfa-1). No presente estudo, foi investigado através do uso de agonistas e antagonistas seletivos os subtipos de ARs-alfa1 envolvidos na contração da aorta abdominal de ratas prenhes submetidas à um modelo experimental de PE por redução da pressão de perfusão uterina (RUPP), e esses receptores foram comparados com aqueles envolvidos na contração da artéria de ratas virgens. Os resultados indicam que as contrações da artéria aorta abdominal de ratas virgens em resposta à noradrenalina resultam da ativação de AR-alfa-1A e AR-alfa-1D, mas que na artéria da fêmea há uma maior contribuição de AR-alfa-1A do que na respectiva artéria de machos. Além disso, a prenhez induziu plasticidade nos subtipos de ARs-alfa-1 envolvidos na contração da artéria aorta abdominal, uma vez que houve menor participação de AR-alfa-1A nas contrações de ratas prenhes do que aquela observada na artéria de ratas virgens. Por outro lado, na artéria aorta ab... (Resumo completo, clicar acesso eletrônico abaixo) / Abstract: Preeclampsia (PE) is a gestational hypertensive disorder, for which the physiopathology has been attributed to an intense inflammatory response, endothelial disfunction, platelet aggregation and increased vascular resistance. Previous studies reported that in PE there is an inadequate increase in the action of several vasoconstrictors, including endothelin, adenosine, angiotensin II and noradrenaline. In fact, the sympathetic nervous system by releasing the neurotransmitter noradrenaline regulates the arterial pressure through activation of 1-adrenoceptors (1-ARs). The present study investigated the 1–ARs subtypes involved in the contractions of the abdominal aortae from pregnant rats submitted to an experimental model of PE, the reduced in uterine perfusion pressure (RUPP), compared these receptors with those involved in the contractions of abdominal aortae from non-pregnant (virgin) and pregnant female rats. The results indicate that there are both 1A–ARs and 1D– ARs in abdominal aortae from non pregnant females, but that the 1A–ARs is more important in the contraction of the female than in the contraction of the respective artery from male rats. Pregnancy induces plasticity in the 1 – ARs of the abdominal aortae, since there was a less significant participation of 1A-AR in the contraction of abdominal aortae from pregnant rats than in the artery of virgin females. In the other hand, selective agonists and antagonists presented complex behaviours in the abdominal ao... (Complete abstract click electronic access below) / Mestre
37

Regulace receptorů spřažených s G proteiny Studie muskarinových a β-adrenergních receptorů u M2KO myší / Regulace receptorů spřažených s G proteiny Studie muskarinových a β-adrenergních receptorů u M2KO myší

Beneš, Jan January 2014 (has links)
(in English): The aim of the work was to perform in-depth analysis of M2KO mice both at baseline and upon a challenge with a cold stress and to explore the role of opposing receptors (i.e. adrenoceptors) in adaptation to lacking M2-receptors in the heart. We have performed receptor binding studies, study of receptor gene expression, echocardiography, telemetric monitoring of heart rate, body temperature and activity, heart rate variability and biorhythm analysis, analysis of heart rate response to the application of drugs (carbachol, atropine, isoprenaline, propranolol), assessment of adenylyl cyclase and NO synthase activity, measurement of catecholamine blood concentration and gene expression of catecholamine-synthesizing enzymes. We have found that the disruption of M2-receptor gene caused a compensatory decrease of cardiostimulatory β1-adrenoceptors and β2-adrenoceptors with corresponding down-regulation of the gene expression, M3-receptors were down-regulated as well. Missing M2-receptors were functionally replaced by the main cardioinhibitory β3-adrenoceptors that were up-regulated, not by cardioinhibitory M4-receptors. β3-adrenoceptors were found to signal through adenylyl cyclase instead of NO synthase. All these changes were found in the left ventricle only, so heterologous regulation is...
38

Efeito do tratamento com doadores de oxido nitrico ou nitroxila sobre parametros cardiovasculares e a população de adrenoceptores 'beta' no coração de camundongos LDLr-/- / Effect of treatment with oxide or nitroxil donors on cardiovascular parametres and 'beta' adrenoceptor population in the hearth of LDLr-/- mice

Caceres, Viviane de Menezes 25 February 2008 (has links)
Orientadores: Marta Helena Krieger, Regina Celia Spadari / Dissertação (mestrado) - Universidade Estadual de Campinas, Instituto de Biologia / Made available in DSpace on 2018-08-11T11:44:59Z (GMT). No. of bitstreams: 1 Caceres_VivianedeMenezes_M.pdf: 892273 bytes, checksum: 832dcecc572cc26759a9832b12d09b9e (MD5) Previous issue date: 2008 / Resumo: Os objetivos do presente estudo são investigar e comparar o efeito do nitrosotiol doador de NO (SNAC) e do doador de NO-/HNO (Sal de Angelis) na estrutura e função do miocárdio sob processo aterogênico precoce induzido pela dieta em camundongos com deleção gênica do receptor de LDL (LDLr-/-). Os dados obtidos possibilitam avaliar a eficácia destas espécies químicas, bem como os mecanismos de ação envolvidos nos efeitos preventivos promovidos pelo sistema NO/NOS e pela via HNO, na hipertrofia ventricular esquerda, neste modelo animal. O papel dos adrenoceptores beta no controle da função cardíaca destes camundongos LDLr-/- também foi avaliado. A deleção gênica do receptor de LDL resultou em déficit contrátil cardíaco, sem alteração na homogeneidade da população miocárdica de adrenoceptores ß1, mas quando associada à dieta hiperlipídica induziu participação de adrenoceptores ß2, com conseqüente alteração da sensibilidade aos efeitos inotrópico e cronotrópico da isoprenalina. O tratamento com SNAC e Sal de Angelis (SA) preveniu o aumento da sensibilidade à isoprenalina, provavelmente ao induzir o acoplamento dos adrenoceptores ß 2 com a proteína Gi. Além disso, o SA foi capaz de corrigir o déficit contrátil do miocárdio. Camundongos LDLr-/- também apresentaram hipertensão, a qual foi prevenida pelo tratamento com SNAC. Quando a deleção gênica estava associada à dieta hiperlipídica, os camundongos apresentaram hipertensão e hipertrofia ventricular esquerda. O SNAC e o SA previniram a hipertrofia, mas não a hipertensão. Concluímos que camundongos com deleção gênica do receptor de LDL, alimentados com dieta hiperlipídica são um modelo interessante de alterações cardíacas e hemodinâmicas, especialmente quando enfocamos alterações das respostas dos adrenoceptores beta adrenérgicos, e que compostos doadores de NO e seus congêneres podem se tornar uma alternativa para prevenir tais alterações / Abstract: The aim of this study is to analyze and to compare the effects of a nitrosothiol NO donnor (SNAC) and of a NO-/HNO donor (Angelis Salt, AS) on the structure and functioning of myocardium under atherogenic process induced by a hyperlipic diet in LDL receptor knockout mice (LDLr-/-). The role played by the ß adrenoceptor subtypes in the control of the cardiac function of LDLr-/- mice has also been analysed. LDLr-/- mice exhibited a contractile deficit in the myocardium, with no alteration in the response to isoprenaline, which is mediated by a homogeneous population of ß1 adrenoceptors. However, when it was associated with a hyperlipidic diet, ß2 adrenoceptors participate in the inotropic and chronotropic responses to isoprenaline, causing an alteration on tissue sensitivity to the agonist. LDLr-/- knockout mice treatment with SNAC or AS avoided the atria supersensitivity to isoprenaline by inducing ß2 adrenoceptors coupling to Gi protein. Moreover, AS but not SNAC was able to recover the atria contractile performance. LDLr-/- mice also presented hypertension that it was prevented by the SNAC treatment. Hypertension was accompanied by ventricular hypertrophy when the gene deletion was associated with a hyperlipidic diet. SNAC or AS treatment prevented the hypertrophy, but not the hypertension. We concluded that LDLr-/- mice fed with a hyperlipidic diet are useful models for the study of haemodynamic and cardiac diseases related to a hypercholesterolemic profile, mostly when the focus is to investigate the participation of the adrenoceptors in the involved processes, and that NO donnors or similar compounds may be an alternative tool to prevent such alterations / Mestrado / Fisiologia / Mestre em Biologia Funcional e Molecular
39

Papel dos receptores beta 2-adrenérgicos nas alterações musculoesqueléticas desencadeadas pela insuficiência cardíaca. / Role of beta2-adrenergic receptors on skeletal muscle alterations induced by heart failure

Vanessa Azevedo Voltarelli 15 February 2012 (has links)
A insuficiência cardíaca (IC) é uma síndrome complexa que envolve múltiplos sistemas e mecanismos compensatórios neuro-hormonais, acompanhada de altos índices de morbidade e mortalidade, e caracterizada por sintomas clínicos como fadiga, dispneia, e intolerância aos esforços físicos. Embora a IC seja uma síndrome de origem cardíaca, observam-se alterações em outros tecidos, como na musculatura esquelética. As modificações do fenótipo muscular e a perda de massa muscular esquelética observadas na IC contribuem para o mau prognóstico e para o aumento da mortalidade dos pacientes. Considerando que os receptores 2-adrenérgicos medeiam a atividade do sistema nervoso simpático na musculatura esquelética, e que a hiperatividade simpática é um dos principais componentes envolvidos no desenvolvimento da miopatia esquelética observada IC, sugere-se que estes receptores estejam associados às alterações morfofuncionais da musculatura esquelética na síndrome. Na presente Dissertação, avaliamos a contribuição dos receptores 2-adrenérgicos nas alterações metabólicas e morfofuncionais da musculatura esquelética e na intolerância aos esforços físicos decorrentes da IC. Para isso, utilizamos camundongos da linhagem FVB controles e com inativação gênica dos receptores 2-adrenérgicos (2KO) que foram submetidos à cirurgia de infarto ou à cirurgia fictícia (sham). O infarto induziu disfunção e remodelamento cardíacos nos animais controles, acompanhados de aumento nos níveis de noradrenalina e adrenalina circulantes, intolerância ao esforço físico, mudança na tipagem de fibras musculares e rarefação capilar nos músculos sóleo e plantar. Essas mesmas respostas foram observadas nos animais com inativação gênica dos receptores 2-adrenérgicos após o infarto do miocárdio, no entanto, os animais 2KO infartados apresentaram uma maior redução da tolerância ao esforço físico e um quadro mais grave de miopatia esquelética. Acompanhando essa atrofia muscular esquelética presente nos animais 2KO infartados, foi observado aumento da expressão de proteínas relacionadas ao sistema proteolítico ubiquitina-proteassoma, aumento da atividade do 26S-proteassoma e tendência a diminuição na expressão proteica de p-Akt (ser473), p-4E-BP1 (thr37/46) e p-FoxO3 (ser253). Os resultados sugerem que a ausência dos receptores 2-adrenérgicos agrava e/ou antecipa as alterações musculoesqueléticas observadas na insuficiência cardíaca, principalmente a atrofia muscular, e que a ativação do sistema proteolítico ubiquitina proteassoma e a inibição da síntese proteica por meio da via Akt/4E-BP1 parecem colaborar para estas respostas / Heart failure (HF) is a complex syndrome involving multiple systems and neurohumoral compensatory mechanisms accompanied by high morbidity and mortality, and it is characterized by clinical signs like fatigue, dyspnea, and increased exercise intolerance. Although HF is a syndrome of cardiac origin, it promotes changes in other tissues, such as skeletal muscle, where modifications of muscle phenotype and the loss of skeletal muscle mass observed in HF contribute to poor prognosis and increased mortality of patients. Taking into consideration that 2-adrenoceptors mediate the activity of sympathetic nervous system in skeletal muscle and that sympathetic hyperactivity is one of the main components involved in developing skeletal muscle abnormalities in HF, it has been suggested that 2-adrenoceptors would be associated with morphofunctional alterations due to chronic sympathetic hyperactivity in skeletal muscles in HF. In the present study, we evaluated the contribution of 2-adrenoceptors on metabolic and morphofunctional alterations in skeletal muscle and also on exercise intolerance-induced by HF. For this, we used FVB mice and mice lacking 2-adrenoceptors (2KO) that were submitted to myocardial infarction or sham surgery. Myocardial infarction induced cardiac dysfunction and remodeling in FVB mice, which was accompanied by significantly increased plasma levels of norepinephrine and epinephrine, exercise intolerance, changes in muscle fiber type and vascular rarefaction in both soleus and plantaris muscles. These same responses were observed in mice lacking 2-adrenoceptors submitted to myocardial infarction. However, infarcted 2KO mice presented a higher decrease of exercise tolerance and more severe skeletal myopathy. Accompanying the skeletal muscle atrophy of infarcted 2KO mice, it was observed a significantly increased protein expression of proteins related with the ubiquitin-proteasome system, an increased 26S-proteassome activity and a trend toward decreased protein expression of p-Akt (ser473), p-4E-BP1 (thr37/46) and p- FoxO3a (ser253). These results suggest that the lack of 2-adrenoceptors worsens and/or anticipates the skeletal muscle alterations observed in HF, mainly muscular atrophy, and the activation of ubiquitin-proteassome system and inhibition of protein synthesis by Akt/4E-BP1 pathway seem to play an important role in skeletal muscle myopathy
40

Alterações vasculares induzidas pelo tratamento crônico com Isoproterenol: Investigação dos subtipos de receptores b-adrenérgicos envolvidos e da possível geração de um processo inflamatório local. / Vascular alterations induced by chronic isoproterenol-treatment: b-adrenoceptor subtypes involved and possible local proinflammatory process generation.

Ana Paula Couto Davel 11 December 2008 (has links)
Neste estudo investigou-se: 1) os subtipos de receptores b-adrenérgicos (b-AR) envolvidos nas alterações de reatividade vascular induzida pela hiperativação dos receptores b-AR com do uso de camundongos nocaute para os receptores b1- ou b2-AR e selvagens tratados por 7 dias com isoproterenol; 2) a expressão gênica e protéica de mediadores pró-inflamatórios na aorta de ratos tratados por 7 dias com isoproterenol. Os dados demonstram que: em aorta de camundongos selvagens o receptor b1-AR é mais importante em mediar vasodilatação, enquanto o b2AR modula negativamente a contração vascular de maneira dependente do endotélio. A hiperativação dos receptores b-AR aumenta a vasoconstrição à fenilefrina via desequilíbrio NO/ ânion superóxido em aorta de camundongos e o b2-AR parece estar envolvido no desencadeamento destes efeitos. Sugere-se que a ativação crônica dos receptores b-AR aumenta a síntese de fatores pró-inflamatórios e induz maior ativação do NF-kB no tecido vascular, efeitos que parecem estar associados ao aumento da reatividade vascular à fenilefrina. / In this study, it was investigated: 1) the b-adrenoceptor (AR) subtypes involved in the altered vascular reactivity induced by overactivation of b-AR using b1- or b2-adrenoceptor knock-out mice and respective wild-types treated for 7 days with isoproterenol or with vehicle; 2) gene and protein expression of vascular inflammatory mediators in aorta from 7-day isoproterenol-treated rats. In conclusion, the data suggest that b1-AR is more important in the modulation of vasodilator mechanisms while b2 down regulates mice vascular contraction in an endothelium-dependent manner. Overactivation of b-AR increased vasoconstrictor response to phenylephrine, by NO/ superoxide anion unbalance in mice aortic rings, and b2-AR seems to be involved in the triggering of these chronic isoproterenol effects. The results also suggest that chronic activation of b-AR enhances the synthesis of proinflammatory factors and induces higher NF-kB activation on vascular tissue, and these effects seem to be related to hiperreactivity to phenylephrine induced by chronic isoproterenol.

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