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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.
351

A multivariate approach to QSAR

Hellberg, Sven January 1986 (has links)
Quantitative structure-activity relationships (OSAR) constitute empirical analogy models connecting chemical structure and biological activity. The analogy approach to QSAR assume that the factors important in the biological system also are contained in chemical model systems. The development of a QSAR can be divided into subproblems: 1. to quantify chemical structure in terms of latent variables expressing analogy, 2. to design test series of compounds, 3. to measure biological activity and 4. to construct a mathematical model connecting chemical structure and biological activity. In this thesis it is proposed that many possibly relevant descriptors should be considered simultaneously in order to efficiently capture the unknown factors inherent in the descriptors. The importance of multivariately and multipositionally varied test series is discussed. Multivariate projection methods such as PCA and PLS are shown to be appropriate far QSAR and to closely correspond to the analogy assumption. The multivariate analogy approach is applied to a beta- adrenergic agents, b haloalkanes, c halogenated ethyl methyl ethers and d four different families of peptides. / <p>Diss. (sammanfattning) Umeå : Umeå universitet, 1986, härtill 8 uppsatser</p> / digitalisering@umu
352

Pathophysiology and treatment of chlorine gas-induced lung injury : an experimental study in pigs /

Wang, Jianpu. January 2004 (has links) (PDF)
Diss. (sammanfattning) Linköping : Linköpings universitet, 2004. / Härtill 5 uppsatser.
353

Mechanism of action of antipsychotic drugs: focus on the nucleus accumbens and the prefrontal cortex : an experimental study /

Marcus, Monica M., January 2005 (has links)
Diss. (sammanfattning) Stockholm : Karolinska institutet, 2005. / Härtill 5 uppsatser.
354

The role of norepinephrine in learning : cerebellar motor learning in rats /

Paredes, Daniel A. January 2007 (has links)
Dissertation (Ph.D.)--University of South Florida, 2007. / Includes vita. Includes bibliographical references (leaves 109-141). Also available online.
355

Διερεύνηση μοριακών μηχανισμών που εμπλέκονται στον καθορισμό του φαινότυπου των λείων μυικών κυττάρων των αγγείων

Νταή, Αικατερίνη 29 July 2011 (has links)
Ο έλεγχος της έκφρασης των πρωτεϊνών που χαρακτηρίζουν τον Λείο Μυικό Φαινότυπο (ΛΜΦ) είναι εξαιρετικής σημασίας για την κατανόηση, σε μοριακό επίπεδο, διεργασιών που σχετίζονται με πολλές φυσιο-παθολογικές καταστάσεις στον άνθρωπο. Μεταξύ των ασθενειών όπου ο ΛΜΦ είναι καθοριστικής σημασίας για την ανάπτυξη και εξέλιξή τους, είναι η αθηροσκλήρωση, η υπέρταση, η επαναστένωση των αρτηριών μετά από αγγειοπλαστική, η ίνωση οργάνων όπως οι πνεύμονες, το ήπαρ και οι νεφροί, και η ανάπτυξη μεταστάσεων από συμπαγείς όγκους. Επομένως, κατανόηση των κυτταρικών και μοριακών μηχανισμών που οδηγούν σε τροποποίηση του ΛΜΦ είναι βασικής σημασίας για την αναγνώριση στρατηγικών περιορισμού της εξέλιξης των νόσων αυτών και της εκδήλωσης των κλινικών συνεπειών τους. Αρχικό στόχο αποτέλεσε η ανάπτυξη και καθιέρωση ενός in vitro προτύπου συστήματος για την διαφοροποίηση μη διαφοροποιημένων κυττάρων προς φαινότυπο που προσομοιάζει με αυτό των Λείων Μυικών Κυττάρων (ΛΜΚ), ώστε να χρησιμεύσει στη μελέτη του μοριακού καθορισμού και ελέγχου του φαινότυπου των κυττάρων αυτών. Πρώτα-πρώτα, χαρακτηρίσαμε βασικά, σημαντικά «μοριακά εργαλεία» για την διαπίστωση και μοριακή διερεύνηση του ΛΜ-φαινοτύπου. Χρησιμοποιώντας τα, αναπτύξαμε και χαρακτηρίσαμε πρωτογενώς ένα πρότυπο σύστημα διαφοροποίησης σε ΛΜΚ, βασιζόμενο σε Μεσεγχυματικά Βλαστικά Κύτταρα (ΜΒΚ) προερχόμενα από γέλη Wharton ομφάλιου λώρου. Στα κύτταρα αυτά, η έκφραση γονιδίων και πρωτεϊνών που χαρακτηρίζουν τον ΛΜΦ εξαρτάται από την επαρκή έκφραση της πρωτεΐνης Serum Response Factor (SRF), από την ύπαρξη αλληλουχιών Serum Response Element (SRE) στον υποκινητή των εξεταζόμενων ΛΜΚ-ειδικών γονιδίων, και επάγεται από εξωγενή έκφραση της Μυοκαρδίνης. Επομένως, όπως έχει περιγραφεί και για άλλα πρότυπα συστήματα, η διαφοροποίηση των κυττάρων αυτών σε κύτταρα που προσομοιάζουν ΛΜΚ στηρίζεται στην συνέργεια δύο μεταγραφικών παραγόντων, του SRF και της Μυοκαρδίνης. Το πρότυπο αυτό θα είναι χρήσιμο για να διερευνήσουμε τους μοριακούς μηχανισμούς δράσης φυσιολογικών και φαρμακολογικών παραγόντων στον έλεγχο του ΛΜΦ. Επί πλέον, το πρότυπο σύστημα αυτό δύναται να αποβεί χρήσιμο για την κατανόηση εν γένει διεργασιών που οδηγούν στην βασική κυτταρική αλλαγή γνωστή ως Επιθηλιακή-Μεσεγχυματική Μετάβαση (ΕΜΤ) και κατ’ επέκταση για την κατανόηση μηχανισμών παθογένειας πλείστων νόσων που χαρακτηρίζονται από ΕΜΤ. Παράλληλα, έγινε προσπάθεια διερεύνησης αν η κυτταρική σειρά A7r5 αγγειακών ΛΜΚ αποτελεί βιώσιμο φαρμακολογικό σύστημα για την διερεύνηση των μηχανισμών μέσω των οποίων η έκφραση του ΛΜΦ ελέγχεται σε μοριακό επίπεδο από τους αδρενεργικούς υποδοχείς, μία οικογένεια υποδοχέων που διαδραματίζουν σημαντικό ρόλο στην ομοιόσταση του αγγειακού τοιχώματος και στην αρτηριακή παθοφυσιολογία. Δείξαμε ότι ο κυτταρικός πληθυσμός A7r5 δεν απαντά σε α1-αδρενεργική διέγερση διότι στερείται α1-αδρενεργικών υποδοχέων. Διέγερση αποκτάται με εισαγωγή μέσω πλασμιδίου α1-αδρενεργικών υποδοχέων, άρα το ενδογενές σηματοδοτικό σύστημα είναι παρόν και λειτουργικό. Επιπρόσθετα, ανακαλύψαμε ότι τα κύτταρα A7r5 εκφράζουν ενδογενώς λειτουργικούς β-αδρενεργικούς υποδοχείς. Θέτουμε έτσι τα θεμέλια για μία σε βάθος διερεύνηση του τυχόν ρόλου των β-αδρενεργικών υποδοχέων στον έλεγχο του φαινοτύπου των αγγειακών ΛΜΚ, ο οποίος είναι καθοριστικός για την γένεση και πορεία των καρδιαγγειακών νοσημάτων εν γένει. Συμπερασματικά λοιπόν α) τα μεσεγχυματικά βλαστικά κύτταρα προερχόμενα από τη γέλη Wharton ανθρώπινου ομφάλιου λώρου αποτελούν κατάλληλο πρότυπο σύστημα διερεύνησης της ρύθμισης των μοριακών μηχανισμών που εμπλέκονται στη διαφοροποίηση προς ΛΜΚ από μόρια φαρμακολογικής σημασίας, και β) τα κύτταρα A7r5 αποτελούν καλό πρότυπο σύστημα για την διερεύνηση του τυχόν ρόλου των β-αδρενεργικών υποδοχέων στον έλεγχο του φαινοτύπου των ΛΜΚ των αγγείων. / The control of the genes that specify the Smooth Muscle Cell Phenotype is of great importance for our understanding, at a molecular level, of the processes central in a number of human pathologies. Among the diseases whose onset and progress is influenced by alterations in Smooth Muscle-Like (SM-L) phenotype are atherosclerosis, organ fibrosis (lung, liver and kidney), and metastasis associated with solid tumors. For these reasons, the understanding of the cell and molecular mechanisms that lead to changes in the SM phenotype expression are of central importance in our efforts to identify new approaches in limiting the progress of these diseases and the manifestation of the associated clinical symptoms. The first Aim of this work was the development and initial characterization of an in vitro model of differentiation towards a Smooth-Muscle-Like phenotype, to serve for the study of its molecular control. Initially, we characterized basic important molecular tools useful in determining the SM-L phenotype. With their aid, we developed and characterized a model system based on Wharton’s Jelly-derived Mesenchymal stem Cells (MSCs). In these cells, the expression of genes and proteins characteristic of the SM Phenotype depends on the protein levels of Serum Response Factor (SRF) and on the existence of SRF-binding elements on the promoters of the SM-specific genes; it is also potently induced by the exogenous expression of the transcription factor Myocardin. Therefore, this population of MSCs behaves as other characterized model systems, in that their differentiation to a SM-L phenotype is supported by the synergistic action of SRF and Myocardin. This novel model system based on Wharton’s Jelly MSCs will be useful to study the role of specific physiological and pharmacological agents in the control of the SM phenotype. In addition, such a system can offer insights in the basic cellular process of Epithelial-to-Mesenchymal Transition (EMT) and by extent, in the pathological mechanisms of diseases characterized by EMT. In parallel, we investigated whether the differentiated SMC line A7r5 is a viable pharmacological model system to investigate the control of the SMC phenotype by adrenergic receptors, a family of receptors that plays a crucial role in the homeostasis of the vessel wall. We showed that A7r5 cells do not express functional α1-adrenergic receptors; however, the intracellular signaling system linked to α-adrenergic receptors is present and functional. In contrast, A7r5 cells endogenously express functional β-adrenergic receptors, and A7r5 cells are therefore an attractive model to study the role of these receptors in the control of the SMC-phenotype. In conclusion, a) Mesenchymal Stem Cells from Wharton’s Jelly surrounding the human umbilical cord are a suitable in vitro model for the study of the molecular mechanisms that modulating Smooth Muscle Cell differentiation, and b) A7r5 cells are a good in vitro model system to investigate the role of the β-adrenergic receptor in controlling the phenotype of Vascular Smooth Muscle cells.
356

Efeito da superalimentação neonatal sobre a função adrenal e o desenvolvimento da microesteatose hepática em ratos adultos / Early overfeeding effect on adrenal function and development of mictoleatasis in adults rats

Ellen Paula Santos da Conceição 27 February 2012 (has links)
Fundação de Amparo à Pesquisa do Estado do Rio de Janeiro / O estado nutricional e hormonal em fases iniciais de desenvolvimento (gestação e lactação) está relacionado a alterações epigenéticas, que podem levar ao desenvolvimento de doenças. A obesidade infantil está relacionada com a ocorrência da obesidade na idade adulta, resistência à insulina e maior risco cardiometabólico. Em estudos experimentais, a superalimentação neonatal causa obesidade e aumenta o risco de doenças cardiovasculares. Estes animais apresentam obesidade visceral, hiperfagia, hiperleptinemia e hipertensão na idade adulta. Previamente, demonstramos que a hiperleptinemia neonatal causa hiperfunção da medula adrenal e microesteatose na idade adulta. No presente estudo avaliamos a função adrenal de ratos adultos obesos no modelo de superalimentação neonatal por redução do tamanho da ninhada e a sensibilidade as catecolaminas no tecido adiposo visceral (TAV) e no fígado. Ao nascimento todas as ninhadas tiveram seu número de filhotes ajustados para 10. Para induzir a superalimentação neonatal, o tamanho da ninhada foi reduzido de dez para três filhotes machos no terceiro dia de lactação até o desmame (SA), enquanto que o grupo controle permaneceu com 10 filhotes durante toda a lactação. Após o desmame, os ratos tiveram livre acesso à dieta padrão e água até 180 dias (1 animal de cada ninhada, n = 7). O TAV e as glândulas adrenais foram pesadas. As contrações hormonais séricas, o conteúdo hepático de glicogênio e triglicerídeos foram avaliados por kits comerciais. O conteúdo e a secreção de catecolaminas adrenais foram avaliados utilizando o método do trihidroxindol. O conteúdo dos hormônios eixo hipotálamo-hipófise-córtex adrenal, das enzimas da via de síntese das catecolaminas na glândula adrenal, ADRB2 no fígado e ADRB3 no TAV foram determinados por Western blotting ou imunohistoquímica. As diferenças foram consideradas significativas quando p <0,05. Aos 180 dias de vida, o grupo SA apresentou maior massa corporal (+15%), maior consumo alimentar (+15%) e maior adiposidade visceral (+79%). Os hormônios do eixo hipotálamo-hipófise-córtex-adrenal não foram alterados. O grupo SA apresentou maior expressão de tirosina hidroxilase e de DOPA descarboxilase (+31% e 90%, respectivamente); conteúdo de catecolaminas adrenais (absoluta: 35% e relativa: 40%), e secreção de catecolaminas, tanto basal quanto estimulada por cafeína (+35% e 43%, respectivamente). O conteúdo ADRB3 no TAV não foi alterado nos grupo SA, entretanto o ADRB2 no fígado apresentou-se menor (-45%). O grupo SA apresentou maior conteúdo de glicogênio e triglicerídeos no fígado (+79% e +49%, respectivamente), além de microesteatose. A superalimentação neonatal resulta em hiperativação adrenomedular e aparentemente está associada a preservação da sensibilidade às catecolaminas no VAT. Adicionalmente sugerimos que o maior conteúdo de glicogênio e triglicerídeos hepático seja devido a menor sensibilidade as catecolaminas. Tal perfil pode contribuir para a disfunção metabólica hepática e hipertensão arterial que são características deste modelo de obesidade programada. / Nutritional and hormonal status at early phases of development are related to epigenetic changes, promoting disease development. Childhood overweight is related with late obesity, insulin resistance and higher cardiometabolic risk. Rats overfed during lactation show higher visceral adiposity, hyperphagia, leptin resistance and hypertension in adulthood. Previously, we demonstrated that neonatal hyperleptinemia is associated with adrenal medullary hyperfunction and liver steatosis at adulthood. Here, we evaluated the adrenal function and liver tissue of adult obese rats that were overfed during lactation. To induce early overfeeding, the litter size was reduced from ten to three male pups at the third day of lactation until weaning (SL). Control group had ten rats per litter (NL). After weaning, rats had free access to standard diet and water until 180 days old (1 animal from each litter, n=7). Significant differences had p<0.05. The SL group presented higher adrenal catecholamine content (absolute: +35% and relative: +40%), tyrosine hydroxylase (+31%), DOPA decarboxylase (+90%) protein contents, basal and caffeine-induced catecholamine in vitro secretion (+35% and +43%, respectively). However, hormones of the hypothalamic-pituitary-adrenal cortex axis were unchanged. The &#946;3-adrenergic receptor content in visceral adipose tissue was unchanged in SL rats, but the &#946;2-adrenergic receptor in the liver was lower (-45%). SL group showed higher glycogen and triglycerides contents in liver (+79% and +49%, respectively), which showed microesteatosis. Although the neonatal overfeeding leads to higher adrenomedullary function, adult obese SL rats have a dysfunction in hepatic &#946;2-adrenergic receptor, which can contribute for the hepatic dysfunction characteristic of liver obesity complications.
357

Influência do treinamento físico sobre a função cardíaca e o sistema β-adrenérgico miocárdico em ratos com disfunção ventricular

Souza, Sérgio Luiz Borges January 2017 (has links)
Orientador: Antonio Carlos Cicogna / Resumo: Introdução: A remodelação cardíaca compreende mudanças no fenótipo cardíaco, determinadas por alterações na expressão gênica em resposta a estresse biomecânico de etiologia fisiológica ou patológica. A RC, eventualmente, pode evoluir para um quadro de disfunção e posteriormente insuficiência cardíaca grave (ICG); alterações no sistema β-adrenérgico podem estar envolvidas nesse processo. Medidas não farmacológicas, como o treinamento físico (TF) são empregadas no manejo das cardiopatias, e entre os efeitos benéficos dessa terapia está a modulação do sistema β-adrenérgico. Apesar das evidencias de que o TF impacta positivamente a sinalização β-adrenérgica e a função cardíaca, não encontramos na literatura trabalhos que avaliaram a associação entre treinamento físico aeróbio de baixa intensidade, sistema β-adrenérgico e função cardíaca em ratos com sobrecarga pressórica e disfunção ventricular. Objetivo: Testar a hipótese de que o TF atenua as alterações β-adrenérgicas miocárdicas e a deterioração do desempenho cardíaco em ratos com sobrecarga pressórica e disfunção ventricular previamente instalada. Métodos: Ratos Wistar machos (70-90 g), submetidos à cirurgia de estenose aórtica supravalvar (EAo), foram inicialmente divididos em dois grupos: Controle operado (Sham) e estenose aórtica (EAo). Após 18 semanas do procedimento cirúrgico, foi realizada análise da função cardíaca para redistribuição dos grupos: não expostos ao treinamento físico (Sham, n= 18 e EAo, ... (Resumo completo, clicar acesso eletrônico abaixo) / Abstract: Introduction: Cardiac remodeling comprises changes in the cardiac phenotype, determined by changes in genic expression in response to biomechanical stress of physiological or pathological etiology. CR can eventually evolve into a condition of dysfunction and subsequently severe heart failure (GCI); Alterations in the β- adrenergic system may be involved in this process. Non-pharmacological measures such as physical training (PT) are used in the management of heart diseases, and among the beneficial effects of this therapy is the β-adrenergic system modulation. Despite the evidence that TF has a positive effect on β-adrenergic signaling and cardiac function, we did not find in the literature studies that evaluate the association between low-intensity aerobic physical exercise, β-adrenergic system and cardiac function in rats with pressure overload and ventricular dysfunction. Objective: To test the hypothesis that PT attenuates myocardial β-adrenergic alterations and deterioration of cardiac performance in rats with pressure overload and previously installed ventricular dysfunction. METHODS: Male Wistar rats (70-90 g) submitted to supravalvular aortic stenosis surgery (AS), were initially divided into two groups: Operated control (Sham) and aortic stenosis (AS). After 18 weeks of the surgical procedure, cardiac function analysis was performed for redistribution of the groups: non-exposed to physical training (Sham, n = 18 and AS, n = 18) and trained (TFSham, ... (Complete abstract click electronic access below) / Mestre
358

Regulation of β-Adrenergic-Induced Protein Phosphorylation in the Myocardium: A Dissertation

George, Edward E. 01 October 1990 (has links)
The purpose of this investigation was to examine selected biochemical mechanisms known to influence contractility and energy metabolism in the myocardium, with particular emphasis placed on the regulatory role of protein phosphorylation in the ventricular myocardium. The investigation was conducted in three phases; initially the cardiac contraction cycle was examined to determine whether reported fluctuations in myocardial cAMP levels were associated with other biochemical events known to be cAMP-dependent. The second phase involved the determination of specific kinase activities and endogenous substrates in a highly purified cardiac sarcolemmal preparation. In the final phase, ventricular myocytes were utilized to examine the ability of adenosinergic and muscarinic agonists to influence the isoproterenol-induced increases in protein phosphorylation. Studies in the first phase examined cyclic AMP levels and selected kinase activities in hearts frozen at various stages of the cardiac cycle. An automated clamping device, capable of freezing a perfused rat heart in less than 50 msec, was utilized to separate the cardiac cycle into various phases. Three different timing schemes were employed to divide the cycle into 2 to 4 segments. These different timing schemes revealed no significant differences in cAMP during the cardiac cycle. Myocardial cAMP values ranged from 2.5 to 4.1 pmol/min/mg protein in all phases. However, in one scheme there was a tendency for cAMP to be elevated in early systole, with minimal values occurring diastole. There were also no significant differences seen for either glycogen phosphorylase or cAMP-dependent protein kinase (PKA) activity between various phases of the cardiac cycle. Since no significant fluctuations were observed in the levels of cAMP or the activities of PKA or glycogen phosphorylase during a single cardiac contraction cycle, it would appear that these agents do not exert their effects on cardiac function on a beat to beat basis. The second phase of study examined the nature and function of individual protein kinases in the myocardium. Using a highly purified cardiac sarcolemmal preparation, kinase specific, synthetic substrates were employed to quantify the activities of cAMP-dependent (PKA), calcium/calmodulin-dependent (PKCM), calcium/phospholipid-dependent (PKC) and cGMP-dependent (PKG) protein kinases. Additionally, endogenous protein substrates were examined in this preparation to provide possible insight as to the function of these kinases in the heart. The activities of PKA, PKG, PKCM, and PKC in nmol 32P/min/μg protein were as follows: PKA, 1606; PKG, 35.7; PKCM, 353; and PKC, 13.2. Three endogenous protein substrates of apparent molecular weights of 15kD, 28kD and 92kD were phosphorylated. While no endogenous protein phosphorylation was detectable as a result of cG-PK activity, all of the substrates were phosphorylated, to varying degrees, by both PKA and CACM-PK. PKC phosphorylated only the 15kD substrate. Even though several endogenous kinases are evident in the sarcolemmal preparation, cAMP-dependent protein kinase demonstrates the greatest degree of activity. This kinase also appeared to be the most abundant; however, there is some concern as to the source of these kinases in the membrane preparation since endothelial membranes as well as cardiac membranes appeared to be present. Evidence for endothelial contamination was provided by the finding that the membrane preparation contained appreciable amounts of angiotensin converting enzyme (ACE) activity, an enzyme felt to reside in the vascular endothelium. Since studies with this preparation could not exclude contribution of nonmuscle cell membranes a model consisting solely of dispersed ventricular myocytes was developed. The third phase of these studies examined protein phosphorylation in primary cultures of ventricular myocytes. Specifically, these studies examined protein phosphorylation induced by exposure to isoproterenol (ISO), a catecholamine known to effect changes in the phosphorylation state of proteins in the heart by means of a β-adrenergic-mediated/cAMP-dependent mechanism was examined. Additionally, the effects of phenylisopropy-ladenosine (PIA) and carbamyl choline chloride (CARB) were examined with regard to their anti-adrenergic role(s) in this process. Adherent, collagenase-dispersed, radiolabelled (32p) ventricular myocytes exposed to ISO demonstrated a dose and time dependent increase in 32p incorporation into several endogenous protein substrates. When the myocytes were exposed (60 sec) to either PIA or CARB prior to the exposure to ISO, ISO-induced 32p incorporation into protein substrates of apparent molecular weight of 6kD, 31kD and 155kD was reduced up to 67% when compared to the effects of ISO alone. Additionally, both PIA and CARB attenuated the ISO-induced increase in PKA activity in the myocyte, yet only CARB was seen to produce an inhibitory effect on the ISO-induced increase in cAMP levels in the myocytes. The effects of CARB were dose-dependent and inhibited the effects of ISO on 32p incorporation at all doses tested. PIA elicited biphasic effects: lower PIA concentrations were inhibitory in nature, while higher concentrations of PIA appeared to potentiate the increase in 32p incorporation induced by ISO. Based on electrophoretic mobilities (SDS/PAGE) of the 6kD and the 155kD substrates, these substrates have been tentatively identified as the monomeric form of the sarcoplasmic reticulum-associated protein, phospholamban, and the contractile filament-associated protein, C protein, respectively. The 31kD substrate has been identified, by means of immunoblot, as the contractile filament-associated protein, troponin I. The role of protein phosphorylation in the myocardium involves complex, inter-related mechanisms that encompass extracellular, transmembranal and cytoplasmic elements in the heart. It is well understood that certain mechanisms of the contraction cycle known to vary on a beat to beat basis, such as myosin ATPase, involve changes in protein phosphorylation. However, the nature of the various kinases and substrates examined in this study appear to influence longer-term events of myocardial contractility. Mechanisms coupled with hormone action, modulation of second messenger-dependent components, and factors associated with changes in contractility seen with aging and disease are more likely to exhibit changes similar to those described herein. A better understanding of the underlying biochemistry may provide greater insight into the importance of these metabolic changes.
359

Efeitos do treinamento físico sobre as propriedades morfológicas e mecânicas em cardiomiócitos de camundongos knockout para os receptores β1- e β2-adrenérgicos / Effects of exercise training on the morphological and mechanical properties in cardiomyocytes from β1-and β2-adrenergic receptors knockout mice

Rodrigues, Aurora Corrêa 11 March 2014 (has links)
Made available in DSpace on 2015-03-26T13:22:04Z (GMT). No. of bitstreams: 1 text completo.pdf: 757671 bytes, checksum: 435de7db4aaa7b1bdaf1bc5260f57dd9 (MD5) Previous issue date: 2014-03-11 / O objetivo do presente estudo foi investigar os efeitos do treinamento físico sobre as propriedades morfológicas e mecânicas de cardiomiócitos de camundongos knockout (KO) para receptores os β1- e β2 adrenérgicos. Camundongos C57BL/6J, KO para os receptores β1-adrenérgicos, FVB/N e KO para os receptores β2-adrenérgicos com 4 meses de idade, foram inicialmente separados aleatoriamente em 8 grupos: C57c, C57t, KO β1c, KO β1t, FVBc, FVBt, KO β2c e KO β2t. Os animais dos grupos treinados (C57t, KO β1t, FVBt, KO β2t) foram submetidos a um protocolo de treinamento aeróbico de 8 semanas, 5 dias por semana, 1hora por dia, com intensidade de 60% da velocidade máxima de corrida. 3 a 4 animais de cada grupo foram separados para a análise de contração celular com perfusão do agonista β-adrenérgico isoproterenol (ISO) [100nM]. Após a eutanásia, os cardiomiócitos do ventrículo esquerdo foram isolados por dispersão enzimática. O comprimento e a largura dos cardiomiócitos foram medidos utilizando um sistema de captação de imagens e o volume celular foi calculado. As contrações celulares foram medidas através da técnica de alteração do comprimento dos cardiomiócitos, após estimulação elétrica a 1 Hz, em temperatura controlada à 37oC, usando-se um sistema de detecção de bordas. Os resultados mostraram que os camundongos KO β1 apresentaram menor comprimento celular comparados aos C57. O grupo KO β2t apresentou maior comprimento celular comparado ao grupo KO β2c. O protocolo de treinamento aumentou a amplitude de contração, a velocidade máxima de contração e a velocidade máxima de relaxamento dos cardiomiócitos dos animais KO β1t e KO β2t. O ISO não alterou a amplitude de contração, a velocidade máxima de contração e de relaxamento nos cardiomiócitos dos camundongos KO β1+ISO, já os animais KO β2+ISO apresentaram aumento nas mesmas propriedades mecânicas. Conclui-se que o protocolo de treinamento aeróbico: a) aumentou as propriedades mecânicas dos cardiomiócitos dos animais KO β1 e KO β2; b) aumentou o comprimento dos cardiomiócitos dos camundongos KO β2; c) associado ao ISO não alterou as propriedades mecânicas nos cardiomiócitos dos camundongos KO β1 e reduziu nos cardiomiócitos dos camundongos KO β2. / The aim of this study was to investigate the effects of endurance training on cardiovascular parameters and morphological and mechanical properties of isolated cardiomyocytes from the left ventricle of β1-and β2 adrenergic receptors knockout mice. 4 months old C57BL/6J, β1- adrenergic receptor knockout (KO 1), FVB/N and β2-adrenergic receptor knockout (KO 2) mice were randomly allocated into one of the 8 groups: C57c, C57t, KO β1c, KO β1t, FVBc, FVBt, KO β2c e KO β2t. The animals of the trained groups (C57t, KO β1t, FVBt, KO β2t) underwent a protocol of aerobic training 8 weeks, 5 days/week, 1 hour/day, intensity of 60% of maximal speed. 3 to 4 animals in each group were divided for the analysis of cellular contraction with infusion of -adrenergic agonist isoproterenol (ISO) [100nM]. At sacrifice, the heart was removed and left ventricular myocytes were enzymatically dispersed. Cell length and width were measured using an image capture system and cell volume was calculated. Myocytes were stimulated at 1 Hz at controlled temperature (37oC) and cell contractility was measured by using an edge detection system. The results showed that KO 1 mice showed lower cell length compared to C57. The KO β2t group showed higher cell length compared to the KO β2c group. The training protocol increased the contraction amplitude, maximum contraction velocity and maximum relaxation velocity of cardiomyocytes of KO β1t and KO β2t animals. The ISO did not alter the amplitude of contraction, maximum contraction velocity and maximum relaxation velocity of cardiomyocytes from KO β1+ISO animals, while the KO β2+ISO animals showed an increase in the same mechanical properties. It is concluded that the aerobic training protocol: a) increased the mechanical properties of cardiomyocytes from KO β1t and KO β2t animals; b) increased the length of cardiomyocytes from β2 KO mice; c) associated with the ISO did not alter the mechanical properties of cardiomyocytes from β2 KO 1mice and reduced of cardiomyocytes from KO β2 mice.
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Efeito da superalimentação neonatal sobre a função adrenal e o desenvolvimento da microesteatose hepática em ratos adultos / Early overfeeding effect on adrenal function and development of mictoleatasis in adults rats

Ellen Paula Santos da Conceição 27 February 2012 (has links)
Fundação de Amparo à Pesquisa do Estado do Rio de Janeiro / O estado nutricional e hormonal em fases iniciais de desenvolvimento (gestação e lactação) está relacionado a alterações epigenéticas, que podem levar ao desenvolvimento de doenças. A obesidade infantil está relacionada com a ocorrência da obesidade na idade adulta, resistência à insulina e maior risco cardiometabólico. Em estudos experimentais, a superalimentação neonatal causa obesidade e aumenta o risco de doenças cardiovasculares. Estes animais apresentam obesidade visceral, hiperfagia, hiperleptinemia e hipertensão na idade adulta. Previamente, demonstramos que a hiperleptinemia neonatal causa hiperfunção da medula adrenal e microesteatose na idade adulta. No presente estudo avaliamos a função adrenal de ratos adultos obesos no modelo de superalimentação neonatal por redução do tamanho da ninhada e a sensibilidade as catecolaminas no tecido adiposo visceral (TAV) e no fígado. Ao nascimento todas as ninhadas tiveram seu número de filhotes ajustados para 10. Para induzir a superalimentação neonatal, o tamanho da ninhada foi reduzido de dez para três filhotes machos no terceiro dia de lactação até o desmame (SA), enquanto que o grupo controle permaneceu com 10 filhotes durante toda a lactação. Após o desmame, os ratos tiveram livre acesso à dieta padrão e água até 180 dias (1 animal de cada ninhada, n = 7). O TAV e as glândulas adrenais foram pesadas. As contrações hormonais séricas, o conteúdo hepático de glicogênio e triglicerídeos foram avaliados por kits comerciais. O conteúdo e a secreção de catecolaminas adrenais foram avaliados utilizando o método do trihidroxindol. O conteúdo dos hormônios eixo hipotálamo-hipófise-córtex adrenal, das enzimas da via de síntese das catecolaminas na glândula adrenal, ADRB2 no fígado e ADRB3 no TAV foram determinados por Western blotting ou imunohistoquímica. As diferenças foram consideradas significativas quando p <0,05. Aos 180 dias de vida, o grupo SA apresentou maior massa corporal (+15%), maior consumo alimentar (+15%) e maior adiposidade visceral (+79%). Os hormônios do eixo hipotálamo-hipófise-córtex-adrenal não foram alterados. O grupo SA apresentou maior expressão de tirosina hidroxilase e de DOPA descarboxilase (+31% e 90%, respectivamente); conteúdo de catecolaminas adrenais (absoluta: 35% e relativa: 40%), e secreção de catecolaminas, tanto basal quanto estimulada por cafeína (+35% e 43%, respectivamente). O conteúdo ADRB3 no TAV não foi alterado nos grupo SA, entretanto o ADRB2 no fígado apresentou-se menor (-45%). O grupo SA apresentou maior conteúdo de glicogênio e triglicerídeos no fígado (+79% e +49%, respectivamente), além de microesteatose. A superalimentação neonatal resulta em hiperativação adrenomedular e aparentemente está associada a preservação da sensibilidade às catecolaminas no VAT. Adicionalmente sugerimos que o maior conteúdo de glicogênio e triglicerídeos hepático seja devido a menor sensibilidade as catecolaminas. Tal perfil pode contribuir para a disfunção metabólica hepática e hipertensão arterial que são características deste modelo de obesidade programada. / Nutritional and hormonal status at early phases of development are related to epigenetic changes, promoting disease development. Childhood overweight is related with late obesity, insulin resistance and higher cardiometabolic risk. Rats overfed during lactation show higher visceral adiposity, hyperphagia, leptin resistance and hypertension in adulthood. Previously, we demonstrated that neonatal hyperleptinemia is associated with adrenal medullary hyperfunction and liver steatosis at adulthood. Here, we evaluated the adrenal function and liver tissue of adult obese rats that were overfed during lactation. To induce early overfeeding, the litter size was reduced from ten to three male pups at the third day of lactation until weaning (SL). Control group had ten rats per litter (NL). After weaning, rats had free access to standard diet and water until 180 days old (1 animal from each litter, n=7). Significant differences had p<0.05. The SL group presented higher adrenal catecholamine content (absolute: +35% and relative: +40%), tyrosine hydroxylase (+31%), DOPA decarboxylase (+90%) protein contents, basal and caffeine-induced catecholamine in vitro secretion (+35% and +43%, respectively). However, hormones of the hypothalamic-pituitary-adrenal cortex axis were unchanged. The &#946;3-adrenergic receptor content in visceral adipose tissue was unchanged in SL rats, but the &#946;2-adrenergic receptor in the liver was lower (-45%). SL group showed higher glycogen and triglycerides contents in liver (+79% and +49%, respectively), which showed microesteatosis. Although the neonatal overfeeding leads to higher adrenomedullary function, adult obese SL rats have a dysfunction in hepatic &#946;2-adrenergic receptor, which can contribute for the hepatic dysfunction characteristic of liver obesity complications.

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