Activation of the β-adrenergic receptor exacerbates lipopolysaccharide-induced wasting of skeletal muscle cells by increasing interleukin-6 production / 骨格筋細胞βアドレナリン受容体の活性化はIL-6の産生増加を介してリポ多糖による骨格筋萎縮を増悪させる

Matsukawa, Shino

24 September 2021

京都大学 / 新制・課程博士 / 博士(医学) / 甲第23468号 / 医博第4775号 / 新制||医||1053(附属図書館) / 京都大学大学院医学研究科医学専攻 / (主査)教授 竹内 理, 教授 山下 潤, 教授 戸口田 淳也 / 学位規則第4条第1項該当 / Doctor of Medical Science / Kyoto University / DFAM

β-adrenergic receptor

wasting of skeletal muscle

interleukin-6

lipopolysaccharide

490

Expression of B-adrenergic receptors in chicken fetuses

Hedlund, Sebastian

January 2006

<p>Chicken fetuses exposed to chronic hypoxia suffer from growth retardation and</p><p>induces an overall sympathetic activity, including elevation of the concentration</p><p>of circulating catecholamines. Simultaneously, hypoxic fetuses display a</p><p>lowered β-adrenoreceptor (βAR) density in myocardial tissue. In vertebrates,</p><p>β1AR and β2AR are the most important signalling pathways for acute elevation</p><p>of cardiac performance. The aim of this study was to see how chronic hypoxia</p><p>affects the level of messenger RNA (mRNA) for the β1AR in the fetal chicken</p><p>heart at different developmental ages. The broiler chicken is a suitable model</p><p>organism for studying the progression of heart failure because the fast growth</p><p>rate requires a large increase in blood perfusion at the end of fetal development.</p><p>The β1AR sequence of the broiler chicken is 1587 bp and located on</p><p>chromosome 6. When running a PCR for quantification of the sequence,</p><p>primers for almost the whole sequence failed (1404 bp) and so did primers of</p><p>1193 bp; instead primers of 692 bp of the sequence were used and made</p><p>quantification possible. Similar results were obtained from both the heart and</p><p>liver of day 15 fetal chickens. The PCR product was cloned into a TOPO vector</p><p>and sent for sequencing, to enable the making of a probe for a northern blot</p><p>analysis of the mRNA in the fetal chicken hearts.</p>

Chicken fetus

β-adrenergic receptor

Hypoxia

mRNA

Heart

Molecular biology

Molekylärbiologi

Expression of B-adrenergic receptors in chicken fetuses

Hedlund, Sebastian

January 2006

Chicken fetuses exposed to chronic hypoxia suffer from growth retardation and induces an overall sympathetic activity, including elevation of the concentration of circulating catecholamines. Simultaneously, hypoxic fetuses display a lowered β-adrenoreceptor (βAR) density in myocardial tissue. In vertebrates, β1AR and β2AR are the most important signalling pathways for acute elevation of cardiac performance. The aim of this study was to see how chronic hypoxia affects the level of messenger RNA (mRNA) for the β1AR in the fetal chicken heart at different developmental ages. The broiler chicken is a suitable model organism for studying the progression of heart failure because the fast growth rate requires a large increase in blood perfusion at the end of fetal development. The β1AR sequence of the broiler chicken is 1587 bp and located on chromosome 6. When running a PCR for quantification of the sequence, primers for almost the whole sequence failed (1404 bp) and so did primers of 1193 bp; instead primers of 692 bp of the sequence were used and made quantification possible. Similar results were obtained from both the heart and liver of day 15 fetal chickens. The PCR product was cloned into a TOPO vector and sent for sequencing, to enable the making of a probe for a northern blot analysis of the mRNA in the fetal chicken hearts.

Chicken fetus

β-adrenergic receptor

Hypoxia

mRNA

Heart

Molecular biology

Molekylärbiologi

Study on the regulatory mechanism for Uncoupling protein 1 (Ucp1) expression in beige adipocytes / ベージュ脂肪細胞の脱共役タンパク質１発現調節機構に関する研究

Ana, Yuliana

24 September 2019

京都大学 / 0048 / 新制・課程博士 / 博士(農学) / 甲第22073号 / 農博第2365号 / 新制||農||1072(附属図書館) / 学位論文||R1||N5227(農学部図書室) / 京都大学大学院農学研究科食品生物科学専攻 / (主査)教授 井上 和生, 教授 保川 清, 教授 谷 史人 / 学位規則第4条第1項該当 / Doctor of Agricultural Science / Kyoto University / DFAM

beige adipocytes

uncoupling protein 1

β-adrenergic receptor

histone modification

ednoplasmic reticulum stress

610

Β1 Integrins Modulate β-Adrenergic Receptor-Stimulated Cardiac Myocyte Apoptosis and Myocardial Remodeling

Krishnamurthy, Prasanna, Subramanian, Venkateswaran, Singh, Mahipal, Singh, Krishna

01 April 2007

Sympathetic nerve activity increases in the heart during cardiac failure. Here, we hypothesized that β1 integrins play a protective role in chronic β-adrenergic receptor-stimulated cardiac myocyte apoptosis and heart failure. l-isoproterenol (iso; 400 μg/kg per hour) was infused in a group of wild-type (WT) and β1 integrin heterozygous knockout (hKO) mice. Left ventricular structural and functional remodeling was studied at 7 and 28 days of iso-infusion. Western blot analysis demonstrated reduced β1 integrin levels in the myocardium of hKO-sham. Iso-infusion increased heart weight:body weight ratios in both groups. However, the increase was significantly higher in WT-iso. M-mode echocardiography indicated increased left ventricular end-diastolic diameter, percentage of fractional shortening, and ejection fraction in the WT-iso group. The percentage of fractional shortening and ejection fraction were significantly lower in hKO-iso versus hKO-sham and WT-iso. Peak left ventricular developed pressure and left ventricular end-diastolic pressure measured using Langendorff-perfusion analyses were significantly higher in the WT-iso group (P<0.05 versus WT-sham and hKO-Iso). The number of TUNEL-positive myocytes was significantly higher in hKO-iso hearts 7 and 28 days after iso-infusion. The increase in myocyte cross-sectional area and fibrosis was higher in the WT-iso group. Matrix metalloproteinase-9 protein levels were significantly higher in WT-iso, whereas matrix metalloproteinase-2 levels were increased in hKO-iso hearts. Iso-infusion increased phosphorylation of c-Jun N-terminal kinase and extracellular signal-regulated kinase 1/2 in both groups. The increase in c-Jun N-terminal kinase phosphorylation was significantly higher in hKO-iso (P<0.001 versus WT-iso). Thus, β1 integrins play a crucial role in β-adrenergic receptor-stimulated myocardial remodeling with effects on cardiac myocyte hypertrophy, apoptosis, and left ventricular function.

β-adrenergic receptor

β1 integrins

apoptosis

heart failure

JNK

MMPs

Biomedical Sciences

Ataxia-Telangiectasia Mutated Kinase: Role in Myocardial Remodeling

Thrasher, Patsy, Singh, Mahipal, Singh, Krishna

01 January 2017

Ataxia-telangiectasia mutated kinase (ATM) is a serine/threonine kinase. Mutations in the ATM gene cause a rare autosomal multisystemic disease known as Ataxia-telangiectasia (AT). Individuals with mutations in both copies of the ATM gene suffer from increased susceptibility to ionizing radiation, predisposition to cancer, insulin resistance, immune deficiency, and premature aging. Patients with one mutated allele make-up ~1.4 to 2% of the general population. These individuals are spared from most of the symptoms of the disease. However, they are predisposed to developing cancer or ischemic heart disease, and die 7-8 years earlier than the non-carriers. DNA double-strand breaks activate ATM, and active ATM is known to phosphorylate an extensive array of proteins involved in cell cycle arrest, DNA repair, and apoptosis. The importance of ATM in the regulation of DNA damage response signaling is fairly well-established. This review summarizes the role of ATM in the heart, specifically in cardiac remodeling following β-adrenergic receptor stimulation and myocardial infarction.

apoptosis

ataxia-telangiectasia mutated kinase

fibrosis

hypertrophy

myocardial infarction

myocardial remodeling

β-adrenergic receptor

Biomedical Sciences

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

Rôles et mécanismes d’action de la protéine Epac dans l’hypertrophie cardiaque / Functions and signaling of Epac protein in cardiac hypertrophy

Laurent, Anne-Coline

17 July 2013

Les catécholamines induisent la synthèse d’AMPc par une stimulation des récepteurs β-adrénergiques et contrôlent ainsi la fonction cardiaque en activant une pléiade de voies de signalisation intracellulaires. Les protéines Epac sont des facteurs d’échange pour les petites protéines G et sont directement activés par l’AMPc. Devant l’importance de la voie β-adrénergique dans la physiopathologie cardiaque et dans le but de mieux comprendre la régulation des processus cellulaires dépendants de l’AMPc dans le cœur, il apparaît essentiel de caractériser le rôle des facteurs d’échange Epac dans le myocarde. Dans une première partie, cette étude démontre que les effets de Epac sur l’hypertrophie des cardiomyocytes ventriculaires de rats nouveaux nés requièrent les GTPases H-Ras et Rap2B. Epac active la voie PLC/IP3/Ca2+ qui est nécessaire pour l’activation de H-Ras. Au niveau transcriptionnel, Epac induit l’export nucléaire de HDAC4 permettant l’activation d’un programme génique d’hypertrophie. Dans une deuxième partie, cette étude révèle l’implication de Epac1 dans l’hypertrophie des cardiomyocytes in vivo, chez la souris. La délétion de Epac1 protège du remodelage cardiaque induit par l’activation prolongée des récepteurs β-adrénergiques et améliore la fonction cardiaque. La surexpression de Epac1 spécifiquement dans le myocarde entraîne une hypertrophie des cardiomyocytes. Par ailleurs, la voie β-AR/Epac1 induit l’accumulation de protéines ubiquitinylées et provoque l’activation du processus d’autophagie in vitro et in vivo. L’autophagie protège des effets délétères de la voie β-adrénergique/Epac en participant à l’élimination des agrégats protéiques et en contrant les effets hypertrophiques de Epac1. Ces résultats ouvrent de nouvelles perspectives pour le traitement de l’hypertrophie et de l’insuffisance cardiaque. / Catecholamines regulate cardiac function by stimulating β-adrenergic receptors (β-AR), leading to cAMP production and activation of a multiplicity of signaling pathways. Epac proteins are exchange factors for small G proteins which are directly activated by cAMP. Given the importance of the β-adrenergic pathway in cardiac physiopathology, it becomes essential to characterize functions of Epac protein in myocardium. In a first part, this study shows that H-Ras and Rap2B GTPases are involved in Epac-induced neonatal rat cardiac myocytes hypertrophy. Epac induces activation of the PLC/IP3/Ca2+ pathway which is necessary for H-Ras activation. At the transcriptional level, Epac causes HDAC4 nuclear export leading to activation of a hypertrophic gene program. In a second part, this study reveals implication of Epac1 in cardiac hypertrophy in vivo. Deletion of Epac1 in mice protects from cardiac remodeling induced by chronic isoproterenol infusion and enhances cardiac function. Cardiac specific overexpression of Epac1 in mice induces cardiac myocytes hypertrophy. Interestingly, β-AR/Epac1 pathway triggers ubiquitinated proteins accumulation and activation of autophagy both in vitro and in vivo. By eliminating aggregates and by counteracting hypertrophic effects of Epac, autophagy protects from deleterious effects of the β-AR/Epac pathway. These results open news insights into the treatment of cardiac hypertrophy and heart failure.

Hypertrophie et insuffisance cardiaque

Autophagie

Récepteur β-adrénergique

AMP cyclique

Epac

Petites protéines G

HDAC

Protéines ubiquitinylées

Bécline 1

P62

LC3

Cardiac hypertrophy and failure

Autophagy

Β-adrenergic receptor

Cyclic AMP

Epac

Small GTPases

HDAC

Ubiquitinated proteins

Beclin 1

P62

LC3

Sireline variation in neonatal lamb cold tolerance

Gudex, B. W.

January 2001

The cost of lamb mortality caused by cold exposure has been estimated at approximately 40 million dollars per year. This value is probably conservative as it does not include the cost due to the reduction in productivity in hypothermic lambs that manage to survive or the cost of reduced selection potential incurred by fewer lambs surviving until selection. The objectives of this research was to investigate whether sire-line variation exists in neonatal lamb cold tolerance and whether polymorphism in the β₃ adrenergic receptor gene can be used as a genetic marker for lamb cold tolerance and lean muscle growth. The influence of the climate, birthweight, age of dam at lambing, gender and birth rank on neonatal lamb cold tolerance was also analysed. Neonatal lamb mortality due to cold exposure was analysed in four field trials that used neonatal lamb morality from cold exposure as a predictor of neonatal lamb cold tolerance. Sire-line variation in neonatal lamb morality was observed in all trials, though it appeared that this effect was largely mediated through sire-line variation in lamb birth weight. Variation in lamb birth weight between birth rank classed was also found to be responsible for the influence of birth rank on neonatal lamb mortality due to cold exposure. The age of dam at lambing and the lamb gender was not observed to influence neonatal lamb mortality due to cold exposure. The sires from the cold tolerance study and the progeny of the lean muscle growth study were genotyped for the β₃ adrenergic receptor locus. Other studies have found evidence that a major gene exists in the catecholamine stimulation of brown adipose thermogenesis and evidence that the β₃-AR gene is a likely candidate. However, this hypothesis and the hypothesis that polymorphism in the β₃-AR gene is also linked to lean muscle growth in lambs was not confirmed in this study. So while it appears that the results were confounded by experimental design, there is evidence that influence of polymorphism in the ovine β₃ AR gene on neonatal lamb mortality and/or lean muscle growth is not sufficient to be considered a major gene effect. The implications of this experiment on the sheep industry and sheep farmers in general are huge. While completely eliminating lamb deaths due to inadequate cold tolerance is impossible, this study shows that large gains in lamb survival could be possible through selective breeding.

sheep

Ovis aries

cold tolerance

lean muscle growth

birthweight

β₃-adrenergic receptor

Beta3 adrenergic receptor

Sireline variation in neonatal lamb cold tolerance

Gudex, B. W.

January 2001

The cost of lamb mortality caused by cold exposure has been estimated at approximately 40 million dollars per year. This value is probably conservative as it does not include the cost due to the reduction in productivity in hypothermic lambs that manage to survive or the cost of reduced selection potential incurred by fewer lambs surviving until selection. The objectives of this research was to investigate whether sire-line variation exists in neonatal lamb cold tolerance and whether polymorphism in the β₃ adrenergic receptor gene can be used as a genetic marker for lamb cold tolerance and lean muscle growth. The influence of the climate, birthweight, age of dam at lambing, gender and birth rank on neonatal lamb cold tolerance was also analysed. Neonatal lamb mortality due to cold exposure was analysed in four field trials that used neonatal lamb morality from cold exposure as a predictor of neonatal lamb cold tolerance. Sire-line variation in neonatal lamb morality was observed in all trials, though it appeared that this effect was largely mediated through sire-line variation in lamb birth weight. Variation in lamb birth weight between birth rank classed was also found to be responsible for the influence of birth rank on neonatal lamb mortality due to cold exposure. The age of dam at lambing and the lamb gender was not observed to influence neonatal lamb mortality due to cold exposure. The sires from the cold tolerance study and the progeny of the lean muscle growth study were genotyped for the β₃ adrenergic receptor locus. Other studies have found evidence that a major gene exists in the catecholamine stimulation of brown adipose thermogenesis and evidence that the β₃-AR gene is a likely candidate. However, this hypothesis and the hypothesis that polymorphism in the β₃-AR gene is also linked to lean muscle growth in lambs was not confirmed in this study. So while it appears that the results were confounded by experimental design, there is evidence that influence of polymorphism in the ovine β₃ AR gene on neonatal lamb mortality and/or lean muscle growth is not sufficient to be considered a major gene effect. The implications of this experiment on the sheep industry and sheep farmers in general are huge. While completely eliminating lamb deaths due to inadequate cold tolerance is impossible, this study shows that large gains in lamb survival could be possible through selective breeding.

sheep

Ovis aries

cold tolerance

lean muscle growth

birthweight

β₃-adrenergic receptor

Beta3 adrenergic receptor