Papel dos receptores adrenérgicos b1 e b2 na termogênese facultativa. / Role of adrenergic receptor b1 e b2 in facultative thermogenesis.

Ueta, Cintia Bagne

17 March 2009

O peso corporal dos animais tende a ser relativamente estável durante longos períodos de tempo. Situações de restrição calórica ou aumento na ingestão de calorias levam a alterações fisiológicas compensatórias que resistem aos efeitos destas perturbações. De fato, o gasto energético aumenta em animais submetidos à dieta hipercalórica, a chamada termogênese facultativa, de modo a manter os estoques energéticos constantes. É possível que defeitos na termogênese facultativa estejam envolvidos no desenvolvimento da obesidade. O BAT, o principal sítio de termogênese facultativa, é ativado pela liberação de NE pelo Sistema Nervoso Simpático, que se liga aos receptores adrenérgicos b1, b2 e b3 expressos nos adipócitos marrons. Diversos estudos demonstram que os receptores b são importantes na proteção contra a obesidade, mas ainda não é claro qual o papel de cada isoforma neste processo. Assim sendo, o objetivo do nosso trabalho foi avaliar o papel das isoformas b1 e b2 na mediação da termogênese facultativa induzida pela dieta. Para tanto, nós tratamos camundongos com nocaute para o receptor adrenérgico b1 (KOb1) e camundongos com nocaute para o receptor b2 (KOb2) com dieta hipercalórica por 22 semanas. O peso corporal foi medido diariamente e o consumo de oxigênio foi determinado usando-se um sistema de respirometria aberto ao final do experimento. A composição corporal foi determinada pela análise da carcaça. Animais foram expostos ao frio de 4ºC por 4h e sua temperatura corporal foi medida em vários tempos e a resposta térmica do iBAT foi determinada pela infusão de NE ou agonista b adrenérgico. Além disso, foram determinados os níveis de RNAm das isoformas de receptores adrenérgicos b nos animais nocaute. Os resultados obtidos em nosso estudo mostram que os animais KOb1 e KOb2 tratados com dieta hipercalórica não desenvolvem obesidade mais severa do que os animais selvagens mas não são capazes de aumentar o consumo de oxigênio induzido pela dieta, sugerindo que estes receptores não são relevantes na termogênese induzida pela dieta. Por outro lado, nossos dados indicam que a presença do receptor b1 é exigida para termogênese induzida pelo frio, uma vez que os camundongos KOb1 são sensíveis ao frio e a capacidade termogênica do BAT destes animais em reposta à NE é bastante reduzida quando comparados com animais selvagens. A ausência do receptor b2 não piora a resposta dos animais ao frio sugerindo que esta isoforma não esteja envolvida na termogênese induzida pela dieta ou pelo frio. Os nossos achados indicam que a isoforma do receptor adrenérgico b1 é fundamental na termogênese induzida pelo frio, mas não pela dieta. Além disso, é provável que a termogênese induzida pela dieta seja regulada por mecanismos distintos da termogênese induzida pelo frio. / The body weight of animals tends to be relatively stable over long periods of time. Situations of caloric restriction or increase in intake of calories lead to compensatory physiological changes that resist the effects of these disorders. In fact, the energy expenditure increases in animals treated with diet hypercaloric called facultative thermogenesis, in order to keep to energy stock constant. Defects in this facultative thermogenesis may be related to the development of obesity. Brown adipose tissue is the main site of facultative thermogenesis and is activated by signaling of b1, b2 e b3 adrenergic receptors by Norepinephrine released by Sympathetic Nervous System. Several studies showed that the isoforms b of adrenergic receptors are important in mechanisms involved in obesity and also in promoting cold tolerance. Nonetheless, it is unclear the role of each isoform in these process. Therefore, the purpose of our study was to evaluate the role of isoforms b1 and b2 in mediate the facultative thermogenesis. For that, we fed nocaute mice for the adrenergic receptor b1 (KOb1) and nocaute mice for the adrenergic receptor b2 (KOb2) with high fat diet for 22 weeks. During treatment body weight was determined daily. By the end of the experiment oxygen consumption was measured using a system of open respirometry and body composition was determined by analysis of the carcass. We also exposed KOb1 and KOb2 animals to cold (4C). The thermogenic response of iBAT was evaluated through i.v NE infusion. The results obtained in our study showed that the animals KOb1 and KOb2 treated with high fat diet did not gain more fat when compared to wild type animals, but are unable to increase the oxygen consumption, suggesting that these receptors are not relevant in development of obesity. Furthermore, our data indicate that the presence of the b1 receptor is required for cold-induced thermogenesis, since the KOb1 mice are sensitive to cold and BAT thermogenic response is significantly impaired when compared with animals wild type. The absence of b2 receptor does not worsen the response of animals to cold suggesting that this isoform is not involved in the diet- or cold- induced thermogenesis. In conclusion, our findings indicate that the b1 isoform of the adrenergic receptor is critical in the cold-induced thermogenesis, but not in diet induced thermogenesis. Moreover, it is likely that the diet-induced thermogenesis and cold-induced thermogenesis are regulated by different mechanisms.

Adrenergic receptor

Brown adipose tissue

Facultative thermogenesis

Knockout

Nocaute

Tecido adiposo marrom

Termogênese facultativa

Migração e invasão do câncer de boca via ativação de receptor beta 2 adrenérgico por mediador do estresse / Cell migration and invasion of oral cancer via activation of beta 2 adrenergic receptor by stress mediator

Diego Mauricio Bravo Calderón

01 October 2015

A ativação do receptor beta 2 adrenérgico (β2-AR), pelos mediadores químicos do estresse, pode induzir efeitos estimuladores ou inibidores na migração e invasão celular, dependendo do tipo de tumor maligno. A importância deste receptor na evolução do câncer de boca não está totalmente esclarecida. O objetivo deste estudo foi verificar a expressão do β2-AR em linhagens de carcinomas espinocelular de boca (SCC-9 e SCC-25), e investigar o papel da ativação deste receptor pela norepinefrina e de seu bloqueio por um antagonista na migração e invasão destas células neoplásicas. As células SCC-9 e SCC-25 foram investigadas quanto à expressão gênica e proteica do β2-AR, respectivamente, pelo RT-qPCR e pelo Western blot. A migração e a invasão celular foram analisadas pelo ensaio de cicatrização de feridas e pelo sistema de câmeras de invasão Transwell, respectivamente. Diferentes concentrações (0,1; 1 e 10μM) de norepinefrina foram utilizadas para estimular e 1μM de propranolol foi empregado para bloquear os receptores beta adrenérgicos nas células neoplásicas. As diferenças das médias obtidas nos experimentos de invasão e migração de SCC-9 e SCC-25 e da expressão proteica do β2-AR, foram comparadas pelo teste t de Student com nível de significância de 5%. Os resultados mostraram que a expressão gênica e proteica do β2-AR foi verificada em ambas as linhagens de câncer de boca. A concentração de 10μM de norepinefrina inibiu, significativamente (p≤0,05), a migração e invasão celular de SCC-9 e SCC-25, sendo este efeito mais acentuado nas células SCC-25. Além disso, houve uma redução significativa (p≤0,05) do efeito da norepinefrina na migração celular quando os β2-AR foram inibidos pelo propranolol. Adicionalmente, o bloqueio dos β-ARs pelo propranolol reverteu parcialmente o efeito da norepinefrina na capacidade invasiva de SCC-9 e SCC-25. Estes resultados comprovam que a norepinefrina, via ativação do β2-AR, reduziu a migração e a invasão das células do carcinoma espinocelular de boca e, portanto, o uso de agonistas dos receptores beta-adrenérgicos poderia se tornar um alvo terapêutico adjuvante no tratamento desta neoplasia maligna. / The activation of beta 2 adrenergic receptor (β2-AR), by chemical mediators of stress, can induce stimulatory or inhibitory effects on cell migration and invasion, depending on the type of malignancy. The importance of this receptor in the oral cancer outcome is not fully understood. The aim of this study was to verify β2- AR expression in oral squamous cell carcinoma cell lines (SCC-9 and SCC-25), and to investigate the role of activation of this receptor by norepinephrine and its blockade by an antagonist in migration and invasion of these neoplastic cells. SCC-9 and SCC-25 cells were investigated for gene and protein expression of β2-AR, respectively, by RT-qPCR and Western blot. The cell migration and invasion were analyzed by wound healing assay and Transwell invasion camera system, respectively. Different concentrations (0.1, 1 and 10μM) of norepinephrine were used to stimulate and 1μM propranolol was used to block the beta adrenergic receptors on cancer cells. Differences in mean values of the invasion and migration assays of SCC-9 and SCC-25 and β2-AR protein expression were compared by the Student t test with 5% significance level. The results showed that β2-AR gene and protein expression was verified in both oral cancer cell lines. The concentration of 10μM of norepinephrine inhibited significantly (p≤0.05), cell migration and invasion of SCC-9 and SCC-25, being the most pronounced effect in SCC-25 cells. Furthermore, there was a significant reduction (p≤0.05) of norepinephrine effect on cell migration when the β2-AR was inhibited by propranolol. In addition, blockade of β-ARs by propranolol partially reversed the effect of norepinephrine on the invasiveness of SCC-9 and SCC-25. These results show that norepinephrine via β2-AR activation, reduced the migration and invasion of oral squamous cell carcinoma cells and, therefore, the use of beta-adrenergic receptors agonists could become an adjuvant therapeutic target in the treatment of this malignancy.

Câncer de boca

Estresse

Receptor beta 2 adrenérgico

Beta 2 adrenergic receptor

Oral cancer

Stress

Expressão de receptor beta-2 adrenérgico em carcinoma espinocelular de boca e sua associação com a evolução clínica tumoral / Expression of beta-2 adrenergic receptor in oral squamous cell carcinoma and its association with tumor clinical outcome

Diego Mauricio Bravo Calderón

10 March 2011

Os hormônios produzidos durante o estresse e seus receptores específicos têm sido amplamente envolvidos com a progressão do câncer. O objetivo deste estudo foi avaliar a expressão dos receptores β2 adrenérgicos pelas células malignas de carcinomas espinocelulares de boca (CEC) e sua correlação com as a características clínicas, evolução e o prognóstico dos pacientes. Um total de 106 pacientes portadores de CEC de boca em estádios clínicos II, III e IV, tratados no Departamento de Cirurgia de Cabeça e Pescoço e Otorrinolaringologia do Hospital de Câncer A.C. Camargo, São Paulo, Brasil, no período de 1970 a 2000, foram analisados quanto aos dados demográficos, história clínica, localização e extensão do tumor, classificação pelo sistema TNM-UICC, tratamento e evolução tumoral. Analisaram-se também as características histopatológicas, índice de malignidade tumoral e a expressão imuno-histoquímica do receptor β2 adrenérgico pelas células malignas no front de invasão tumoral. A associação da expressão do receptor β2 adrenérgico e as variáveis clínicas ou microscópicas foi calculada pelo teste do qui quadrado ou teste exato de Fisher. As probabilidades de sobrevida global e específica por câncer em 5 e 10 anos foram calculadas pelo estimador produto-limite de Kaplan-Meier, comparadas pelo test de long-rank e pelo modelo de regressão múltiplo de Cox. A expressão do receptor β2 adrenérgico foi detectada na membrana e no citoplasma das células malignas da maioria dos CECs de boca (72,6%) e, significativamente associada ao etilismo (p=0,021), tabagismo e etilismo simultâneo (p=0,014) e estadiamento T (p=0,07). Os pacientes cujos tumores demonstraram expressão positiva do receptor β2 adrenérgico apresentaram maiores taxas de sobrevida global (p=0,001) e específica por câncer (p=0,004), quando comparadas aquelas dos pacientes com tumores com ausência da expressão desta proteína. Esses resultados sugerem que a expressão do receptor β2 adrenérgico nas células malignas da região do front de invasão tumoral constitui um fator prognóstico favorável em pacientes com carcinoma espinocelular de boca e pode ser utilizada como alvo de novas estratégias farmacológicas antineoplásicas. / The stress related hormones and their specific receptors have been widely involved with cancer progression. The aim of this study was to evaluate the expression of β2 adrenergic receptor by malignant cells in oral squamous cell carcinoma (OSCC) and its correlation with clinical characteristics, outcome and patients prognosis. A total of 106 patients with OSCC in clinical stages II, III and IV submitted to surgical treatment at the Head and Neck Surgery and Otorhinolaryngology Department, of the Cancer Hospital A.C. Camargo, São Paulo, Brazil, from 1970 to 2000, were analyzed for demographics data, clinical history, location, tumor extension, stage by the TNM-UICC, treatment and tumor outcome. In addition, we investigated the morphologic features, the histopathological malignant index and the immunohistochemical expression of β2 adrenergic receptor by malignant cells of the invasive front of tumor. Chi-square test or Fishers exact test was used to analyze the association among β2 adrenergic receptor expression and the clinical or morphologic variables. The probability of overall and cancer specific survival in 5 and 10 years were calculated by Kaplan-Meier method and the prognostic value of the clinical and morphologic variables was obtained by Cox regression model. Most of OSCCs (72,6%) showed the β2 adrenergic receptor expression in cytoplasm and cell membrane of malignant cells. In OSCC, positive β2 adrenergic receptor expression was significantly associated with alcoholism (p=0.021), simultaneous consumption of alcohol and tobacco (p=0.014) and T stage (p=0.07). OSCC patients with positive expression of β2 adrenergic receptor showed higher rates of overall survival (p=0.001) and cancer specific (p=0.004) than those patients with tumors without expression of this protein. These results suggest that the β2 adrenergic receptor expression by malignant cells in the invasive front of tumor is a favorable prognostic factor in patients with OSCC and can be used as a target for new anti-neoplastic pharmacological strategies.

Câncer de boca

Estresse

Receptor β2 adrenérgico

β2 adrenergic receptor

Oral cancer

Stress

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

De- and Resensitisation of Cardiac β-Adrenergic Receptor Signaling : A Modelling Approach

Lundengård, Karin

January 2011

Desensitisation is defined as a failure of a signaling pathway to respond to chronic or repeated stimulation. The β-adrenergic receptor signaling pathway of the healthy adult heart is known to desensitise, and then regain the sensitivity to stimulation if given enough time to rest between stimulations (resensitisation). The fetal heart does not desensitise, and in animal models of heart failure, a permanent desensitisation have been observed. No isolated element of the signaling pathway have yet been proven to be the sole modulator of the desensitisation behavior. Therefore a mathematical model of the signaling pathway has been constructed, minimized against theoretical desensitisation data and tested for resensitisation. The minimal models and the original model were capable of describing the theoretical de- and resensitisation of the pathway, and only one receptor type with three states was required in the minimal models, but one feedback from the kinases either to phosphorylation of the receptor or to breakdown of cAMP. The original model was also capable of describing experimental data of contraction force from chicken cardiac tissue. The cardiac tissue displays the peak behavior of the desensitisation when stimulated with ISO for ten minutes, and resensitises in less than 5 minutes.

Systems biology

beta adrenergic receptor

desensitisation

heart

chicken

Cell and molecular biology

Cell- och 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

Metoprolol Impairs Mesenteric and Posterior Cerebral Artery Function in Mice

El Beheiry, Mostafa Hossam

31 December 2010

Background/Rationale: In addition to their established cardioprotective role, β-adrenergic antagonists also increase the risk of stroke and mortality. We propose that a vascular mechanism could contribute to cerebral tissue ischemia in β-blocked patients. Methods: Cardiac output (CO), mean arterial pressure (MAP) and microvascular brain oxygen tension (PBrmvO2) were measured in anesthesized mice treated with metoprolol (3mg•kg-1, i.v.). Dose-response curves (DRCs) for adrenergic-agonists were generated in mesenteric resistance arteries (MRAs; isoproterenol, clenbuterol) and posterior cerebral arteries (PCAs; phenylephrine, isoproterenol) before and after metoprolol treatment. Results: Metoprolol reduced CO, maintained MAP and increased systemic vascular resistance (SVR) resulting in a decreased PBrmvO2 in mice. Metoprolol attenuated β-adrenergic mediated vasodilation in both MRAs and PCAs. Conclusions: Metoprolol reduced brain perfusion in mice. A decrease in CO contributed however, metoprolol also inhibited β-adrenergic vasodilation of mesenteric and cerebral arteries. This provides evidence in support of a vascular mechanism for cerebral ischemia in β-blocked patients.

mesenteric resistance artery

beta-blockers

metoprolol

beta-adrenergic receptor

posterior cerebral artery

isoproterenol

0719

Metoprolol Impairs Mesenteric and Posterior Cerebral Artery Function in Mice

El Beheiry, Mostafa Hossam

31 December 2010

Background/Rationale: In addition to their established cardioprotective role, β-adrenergic antagonists also increase the risk of stroke and mortality. We propose that a vascular mechanism could contribute to cerebral tissue ischemia in β-blocked patients. Methods: Cardiac output (CO), mean arterial pressure (MAP) and microvascular brain oxygen tension (PBrmvO2) were measured in anesthesized mice treated with metoprolol (3mg•kg-1, i.v.). Dose-response curves (DRCs) for adrenergic-agonists were generated in mesenteric resistance arteries (MRAs; isoproterenol, clenbuterol) and posterior cerebral arteries (PCAs; phenylephrine, isoproterenol) before and after metoprolol treatment. Results: Metoprolol reduced CO, maintained MAP and increased systemic vascular resistance (SVR) resulting in a decreased PBrmvO2 in mice. Metoprolol attenuated β-adrenergic mediated vasodilation in both MRAs and PCAs. Conclusions: Metoprolol reduced brain perfusion in mice. A decrease in CO contributed however, metoprolol also inhibited β-adrenergic vasodilation of mesenteric and cerebral arteries. This provides evidence in support of a vascular mechanism for cerebral ischemia in β-blocked patients.

mesenteric resistance artery

beta-blockers

metoprolol

beta-adrenergic receptor

posterior cerebral artery

isoproterenol

0719

Papel dos receptores adrenérgicos b1 e b2 na termogênese facultativa. / Role of adrenergic receptor b1 e b2 in facultative thermogenesis.

Cintia Bagne Ueta

17 March 2009

O peso corporal dos animais tende a ser relativamente estável durante longos períodos de tempo. Situações de restrição calórica ou aumento na ingestão de calorias levam a alterações fisiológicas compensatórias que resistem aos efeitos destas perturbações. De fato, o gasto energético aumenta em animais submetidos à dieta hipercalórica, a chamada termogênese facultativa, de modo a manter os estoques energéticos constantes. É possível que defeitos na termogênese facultativa estejam envolvidos no desenvolvimento da obesidade. O BAT, o principal sítio de termogênese facultativa, é ativado pela liberação de NE pelo Sistema Nervoso Simpático, que se liga aos receptores adrenérgicos b1, b2 e b3 expressos nos adipócitos marrons. Diversos estudos demonstram que os receptores b são importantes na proteção contra a obesidade, mas ainda não é claro qual o papel de cada isoforma neste processo. Assim sendo, o objetivo do nosso trabalho foi avaliar o papel das isoformas b1 e b2 na mediação da termogênese facultativa induzida pela dieta. Para tanto, nós tratamos camundongos com nocaute para o receptor adrenérgico b1 (KOb1) e camundongos com nocaute para o receptor b2 (KOb2) com dieta hipercalórica por 22 semanas. O peso corporal foi medido diariamente e o consumo de oxigênio foi determinado usando-se um sistema de respirometria aberto ao final do experimento. A composição corporal foi determinada pela análise da carcaça. Animais foram expostos ao frio de 4ºC por 4h e sua temperatura corporal foi medida em vários tempos e a resposta térmica do iBAT foi determinada pela infusão de NE ou agonista b adrenérgico. Além disso, foram determinados os níveis de RNAm das isoformas de receptores adrenérgicos b nos animais nocaute. Os resultados obtidos em nosso estudo mostram que os animais KOb1 e KOb2 tratados com dieta hipercalórica não desenvolvem obesidade mais severa do que os animais selvagens mas não são capazes de aumentar o consumo de oxigênio induzido pela dieta, sugerindo que estes receptores não são relevantes na termogênese induzida pela dieta. Por outro lado, nossos dados indicam que a presença do receptor b1 é exigida para termogênese induzida pelo frio, uma vez que os camundongos KOb1 são sensíveis ao frio e a capacidade termogênica do BAT destes animais em reposta à NE é bastante reduzida quando comparados com animais selvagens. A ausência do receptor b2 não piora a resposta dos animais ao frio sugerindo que esta isoforma não esteja envolvida na termogênese induzida pela dieta ou pelo frio. Os nossos achados indicam que a isoforma do receptor adrenérgico b1 é fundamental na termogênese induzida pelo frio, mas não pela dieta. Além disso, é provável que a termogênese induzida pela dieta seja regulada por mecanismos distintos da termogênese induzida pelo frio. / The body weight of animals tends to be relatively stable over long periods of time. Situations of caloric restriction or increase in intake of calories lead to compensatory physiological changes that resist the effects of these disorders. In fact, the energy expenditure increases in animals treated with diet hypercaloric called facultative thermogenesis, in order to keep to energy stock constant. Defects in this facultative thermogenesis may be related to the development of obesity. Brown adipose tissue is the main site of facultative thermogenesis and is activated by signaling of b1, b2 e b3 adrenergic receptors by Norepinephrine released by Sympathetic Nervous System. Several studies showed that the isoforms b of adrenergic receptors are important in mechanisms involved in obesity and also in promoting cold tolerance. Nonetheless, it is unclear the role of each isoform in these process. Therefore, the purpose of our study was to evaluate the role of isoforms b1 and b2 in mediate the facultative thermogenesis. For that, we fed nocaute mice for the adrenergic receptor b1 (KOb1) and nocaute mice for the adrenergic receptor b2 (KOb2) with high fat diet for 22 weeks. During treatment body weight was determined daily. By the end of the experiment oxygen consumption was measured using a system of open respirometry and body composition was determined by analysis of the carcass. We also exposed KOb1 and KOb2 animals to cold (4C). The thermogenic response of iBAT was evaluated through i.v NE infusion. The results obtained in our study showed that the animals KOb1 and KOb2 treated with high fat diet did not gain more fat when compared to wild type animals, but are unable to increase the oxygen consumption, suggesting that these receptors are not relevant in development of obesity. Furthermore, our data indicate that the presence of the b1 receptor is required for cold-induced thermogenesis, since the KOb1 mice are sensitive to cold and BAT thermogenic response is significantly impaired when compared with animals wild type. The absence of b2 receptor does not worsen the response of animals to cold suggesting that this isoform is not involved in the diet- or cold- induced thermogenesis. In conclusion, our findings indicate that the b1 isoform of the adrenergic receptor is critical in the cold-induced thermogenesis, but not in diet induced thermogenesis. Moreover, it is likely that the diet-induced thermogenesis and cold-induced thermogenesis are regulated by different mechanisms.

Nocaute

Tecido adiposo marrom

Termogênese facultativa

Adrenergic receptor

Brown adipose tissue

Facultative thermogenesis

Knockout

Avaliação da interação do hormônio tiroideano com o sistema nervoso simpático, via receptor &#945;2A adrenérgico, na regulação da maturação e crescimento ósseos. / Evaluation of the interaction of thyroid hormone with the sympathetic nervous system , via &#945;2A adrenergic receptor, the regulation of maturation and bone growth.

Marcos Vinicius da Silva

07 July 2016

Sabe-se que o hormônio tireoideano (HT) regula o desenvolvimento e crescimento dos ossos. No estudo, investigamos se o HT interage com o sistema nervoso simpático (SNS) controlando o crescimento longitudinal ósseo (CLO), e se essa possível interação depende do &#945;2A-AR. Para tanto, avaliamos o efeito de 30 dias de hipotireoidismo (HIPO) e hipertireoidismo (HIPER) e &#945;2A-AR-/- de 21 dias de idade. Vimos que os animais &#945;2A-AR-/- apresentam menor comprimento no fêmur, tíbia, rádio, úmero e L4 quando comparados aos animais Selv. Como esperado, o HIPO e HIPER prejudicaram o CLO desses ossos nos camundongos Selv, entretanto, o efeito do HIPO foi mais deletério. A morfologia da LE distal do fêmur mostrou que os animais &#945;2A-AR-/- eutireóideos (EUT) apresentam desorganização de zonas e alterações no número de condrócitos sendo o Hipotireoidismo o tratamento mais deletérios. Dados desse estudos sugerem que as vias PTHrP/Ihh e IGF-1/IGF-1R possam ser vias de convergência do SNS e HT na regulação da morfofisiologia da LE, envolvendo o &#945;2A-AR. Observou-se que os animais &#945;2A-AR-/- apresentam alterações no osso trabecular com potencialização com o hipotireoismo. Além disso, os animais &#945;2A-AR-/- apresentam alterações a conectividade trabecular. Esses achados sugerem que o SNS e interage o HT dependente do &#945;2A-AR. / It is known that the thyroid hormone (TH) regulates the development and growth of bones. In the study, we investigated whether the HT interacts with the sympathetic nervous system (SNS) controlling bone longitudinal growth (CLO), and if this possible interaction depends on &#945;2A-AR -/-. Therefore, we evaluated the effect of 30 days of hypothyroidism (HYPO) and hyperthyroidism (HYPER) and &#945;2A-AR -/- 21 days old. We have seen that &#945;2A-AR -/- animals have shorter femur, tibia, radius, humerus and L4 compared to Selv animals. As expected, the HYPO and HYPER damaged the CLO of these bones in Selv mice, however, the effect of HYPO was more deleterious. The morphology of the distal femur LE showed that &#945;2A-AR -/- animals euthyroid (EUT) have clutter zones and changes in the number of chondrocytes and Hypothyroidism most harmful treatment. Data from this study suggest that PTHrP pathways / Ihh and IGF-1 / IGF-1R can be SNS convergence and HT pathways in the regulation of the CO morphophysiology involving the &#945;2A-AR. It was observed that &#945;2A-AR -/- animals show changes in trabecular bone with augmentation with the hipotireoismo. Furthermore, &#945;2A-AR-/- animals show changes trabecular connectivity. These findings suggest that the SNS and interacts the HT dependent &#945;2A-AR.

Crescimento ósseo

Hormônio tireoideno

Receptor adrenérgico

Adrenergic receptor

Bone growth

Thyroid hormone