Efeitos das frações I, II, III e IV do Parotin sobre a incorporação de glicose e consumo de oxigenio pelo tecido adiposo de ratos normais e diabeticos

Orientador: Decio TeixeiraTese (doutorado) - Universidade Estadual de Campinas, Faculdade de Odontologia de PiracicabaResumo: O presente trabalho foi realizado com a finali dade de se verificar," In Vitro" , os eventuais efeitos das diferentes Frações do princípio ativo Parotin, sobre a incorporação de glicose e o consumo de oxigênio pelo tecido adiposo do epidídimo de ratos normais e diabéticos. Foram utilizados 70 ratos machos (Rattus, norvegicus, albinus, Wistar) com, aproximadamente 3 meses de idade, pesando entre 150 e 200 gramas, que foram aleatóriamen-te, distribuídos em dois grupos experimentais: Grupo I - Contrôle (normais)l e Grupo 11 - Diabéticos (aloxânicos). Os animais pertencentes aos dois grupos, -após jejum de 24 horas, foram sacrificados, por decapitação, e o tecido adiposo da cabeça do epidídimo foi removido e mantido em sôro fisiológico à 40C. A seguir, os tecidos foram incubados em frascos de Warburg, afim de se determinar "In Vitro", o consumo de oxigênio, e a incorporação de glicose frente ,as diferentes Frações do Parotin. O sistema experimental para a determinação do consumo de oxigênio e da incorporação de glicose para ambos os grupos, constou de: a) Endogeno (5ratos); b)Glicose (5 ratos); c) Glicose + Insulina (5 ratos); d) Glicose + Fração I do Parotin (5 ratos) . e) Glicose + Fração II do Parotin (5 ratos) f) Glicose + Fração III do Parotin (5 ratos); g) Glicose + Fração IV do Parotin (5 ratos) . Nas condições experimentais utilizadas verificou-se que as Frações do Parotin, principalmente a Fração II e a Fração III.que mostraram maior atividade, aumentaram significativamente a incorporação de glicose e o consumo de oxignio pelo epidídimo ae ratos normais e diabéticos, enquanto que as frações I e IV foram menos efetivas. Foi observado também que as Frações do Parotin e a Insulina foram mais efetivas em aumentar a incorporação de glicose e o consumo de oxigênio nos animais diabéticosAbstract: Not informed.DoutoradoFarmacologiaDoutor em Ciência

Influence of ethanol and morphine on pain perception evoked by deep tissue injury

O objetivo deste estudo foi avaliar o efeito do etanol e da morfina sobre as respostas comportamentais nociceptivas provocadas pelo teste da formalina na ATM de ratos (Teste da formalina na ATM). No experimento 1, os animais receberam uma solução de etanol 6,5 % ou água comum para beber durante 4 e 10 dias, antes da realização do teste da formalina na ATM. No grupo tratado por 4 dias, observou-se analgesia significativa ao teste da formalina, enquanto que no grupo tratado por 10 dias esse efeito não ocorreu, demonstrando o desenvolvimento de tolerância aos efeitos antinociceptivos do etanol. No experimento 2, os animais foram submetidos ao regime crônico de etanol (6,5% por 10 dias) e o grupo controle recebeu água comum para beber. Após esse período, foi administrado morfina (10 mg/kg i.p.) 30 minutos antes da realização do teste da formalina na ATM. A morfina teve o mesmo efeito analgésico nos 2 grupos, demonstrando que o tratamento com etanol não foi capaz de alterar a potência analgésica da morfina. Os resultados mostraram que o etanol é capaz de alterar as respostas nociceptivas relacionadas à dor proveniente de tecidos profundos, como a ATM, e a ausência de interação entre o etanol e a morfina indica que a analgesia induzida pelo etanol é mediada por mecanismos não-opióides.The aim of this study was to evaluate the effect of ethanol and morphine on nociceptive behavioral responses evoked by the injection of formalin into the temporomandibular joint region of rats (the TMJ formalin test). In experiment 1, animals were given an ethanol solution (6.5%) or tap water to drink for 4 and 10 days, before the procedure for TMJ pain. In the group treated for 4 days, significant analgesia was observed in the TMJ formalin test, whereas the group treated for 10 days did not show this effect, revealing the development of tolerance to ethanol antinociceptive effects. In experiment 2, animals were submitted to chronic regimen of ethanol (6.5% for 10 days) and the control group was given tap water to drink. After this period, morphine (10 mg/kg i.p.) was administrated 30 minutes before the TMJ formalin test. Morphine had the same analgesic effect in both groups, showing that the treatment with ethanol was not able to alter the analgesic potency of morphine. The results showed that ethanol can affect nociceptive behavioral responses related to pain from deep tissues, like the TMJ, and the absence of interaction between ethanol and morphine suggest that ethanol-induced analgesia was mediated by nonopiate mechanisms

Purificação e caracterização de um peptidio de glandulas submandibulares de camundongos machos com atividade toxica renal

Orientador: Carlos Eduardo PinheiroDissertação (mestrado) - Universidade Estadual de Campinas, Instituto de BiologiaResumo: O presente trabalho teve a finalidade de isolar e caracterizar um peptídio do extrato de glândulas submandibulares de camundongos machos adultos, com ação sobre o rim. A purificação deste peptídio compreende as seguintes etapas: Homogeneização de glândulas submandibulares se camundongos em álcool etílico; Extração do precipitado alcoólico com tampão Tris ¿ HCl; Precipitação com sulfato de amônio à 75%; Aquecimento durante 10 min. à '60GRAUS¿C; Filtração em gel ¿Sephadex G-25¿. Pela análise dos resultados podemos concluir que: As glândulas submandibulares de camundongos machos, possuem um peptidio de P.M em torno de 2800. Este peptídio apresenta um componente básico e um componente acido, de pH isoelétrico em torno de 8,7 e 3,2 respectivamente. Quando injetado subcutaneamente na dose de 1,5 mg/Kg de peso em ratos, este peptído provoca poliúria e albuminuria. A ação tóxica deste peptidio sobre as estruturas renais e albuminuria. A ação tóxica deste pepticio sobre as estruturas renais é evidenciada por: desorganização do feixe capilar intra-capsular; aumento da permeabilidade capilar glomerular, ectasia tubular acentuada, vacuolização das células dos túbulos proximaisAbstract: Not informed.MestradoFisiologiaMestre em Ciências Biológica

Influence of sex on temporomandibular disorder pain: a review of occurrence and development

Aim: The aim of this study was to develop a narrative literature review using international research to present the influence of sex on occurrence and development of temporomandibular disorder (TMD) pain. Methods: The data sources were computer-based searches in PubMed between 1987 and Feb 2008 using appropriate keywords. For inclusion in this review, articles had to meet the following criteria: be written in English; include human and nonhuman subjects; be published a full-text paper in a peer-reviewed medical journal. Results: The studies considered eligible for this narrative review presented results in agreement with the difference in sex and orofacial pain. Patients were almost always adults, with particular focus on patients' sex. Clinical conditions were predominantly TDM pain. Since sexual dimorphism was detected in TMD pain, the results are focused on women. Conclusion: The findings of this review suggest that there is difference in the occurrence and development of pain according to the individual's sex, women being more susceptible to TMD pain

Influence of ethanol and morphine on pain perception evoked by deep tissue injury A influência do etanol e da morfina sobre a percepção dolorosa provocada por injúria tecidual profunda

The aim of this study was to evaluate the effect of ethanol and morphine on nociceptive behavioral responses evoked by the injection of formalin into the temporomandibular joint region of rats (the TMJ formalin test). In experiment 1, animals were given an ethanol solution (6.5%) or tap water to drink for 4 and 10 days, before the procedure for TMJ pain. In the group treated for 4 days, significant analgesia was observed in the TMJ formalin test, whereas the group treated for 10 days did not show this effect, revealing the development of tolerance to ethanol antinociceptive effects. In experiment 2, animals were submitted to chronic regimen of ethanol (6.5% for 10 days) and the control group was given tap water to drink. After this period, morphine (10 mg/kg i.p.) was administrated 30 minutes before the TMJ formalin test. Morphine had the same analgesic effect in both groups, showing that the treatment with ethanol was not able to alter the analgesic potency of morphine. The results showed that ethanol can affect nociceptive behavioral responses related to pain from deep tissues, like the TMJ, and the absence of interaction between ethanol and morphine suggest that ethanol-induced analgesia was mediated by nonopiate mechanisms.<br>O objetivo deste estudo foi avaliar o efeito do etanol e da morfina sobre as respostas comportamentais nociceptivas provocadas pelo teste da formalina na ATM de ratos (Teste da formalina na ATM). No experimento 1, os animais receberam uma solução de etanol 6,5 % ou água comum para beber durante 4 e 10 dias, antes da realização do teste da formalina na ATM. No grupo tratado por 4 dias, observou-se analgesia significativa ao teste da formalina, enquanto que no grupo tratado por 10 dias esse efeito não ocorreu, demonstrando o desenvolvimento de tolerância aos efeitos antinociceptivos do etanol. No experimento 2, os animais foram submetidos ao regime crônico de etanol (6,5% por 10 dias) e o grupo controle recebeu água comum para beber. Após esse período, foi administrado morfina (10 mg/kg i.p.) 30 minutos antes da realização do teste da formalina na ATM. A morfina teve o mesmo efeito analgésico nos 2 grupos, demonstrando que o tratamento com etanol não foi capaz de alterar a potência analgésica da morfina. Os resultados mostraram que o etanol é capaz de alterar as respostas nociceptivas relacionadas à dor proveniente de tecidos profundos, como a ATM, e a ausência de interação entre o etanol e a morfina indica que a analgesia induzida pelo etanol é mediada por mecanismos não-opióides

Effects of ethanol on deep pain evoked by formalin injected in TMJ of rat

It has been reported that ethanol can alter nociceptive sensitivity from superficial tissues, such as skin and subcutaneous region. However, the influence of ethanol on deep pain conditions is not understood. The aim of this study was to demonstrate the acute, chronic and ethanol withdrawal effects on nociceptive behavioral responses induced by the injection of formalin into the temporomandibular joint (TMJ) region of rats. In experiment 1, rats were injected with ethanol (2,5 g/Kg, i.p.) or an equal volume of saline 15 min before the administration of formalin (1.5%) into the TMJ. Rats pretreated with ethanol showed a decrease in nociceptive behavioral responses. In experiment 2, rats were given an ethanol solution (6.5%) or tap water to drink for 4 and 10 days. On day 4, the animals (ethanol group) showed amounts of analgesia when submitted to the TMJ formalin test. Tolerance to the antinociceptive effects was observed on day 10. Behavioral hyperalgesia was verified 12 hr after withdrawal in another group that drank ethanol for 10 days. These results show that ethanol can affect the nociceptive responses related to deep pain evoked by the TMJ formalin test.It has been reported that ethanol can alter nociceptive sensitivity from superficial tissues, such as skin and subcutaneous region. However, the influence of ethanol on deep pain conditions is not understood. The aim of this study was to demonstrate the acute, chronic and ethanol withdrawal effects on nociceptive behavioral responses induced by the injection of formalin into the temporomandibular joint (TMJ) region of rats. In experiment 1, rats were injected with ethanol (2,5 g/Kg, IP) or an equal volume of saline 15 min before the administration of formalin (1,5%) into the TMJ. Rats pretreated with ethanol showed a decrease in nociceptive behavioral responses. In experiment 2, rats were given an ethanol solution (6,5%) or tap water to drink for 4 and 10 days. On day 4, the animals (ethanol group) showed amounts of analgesia when submitted to the TMJ formalin test. Tolerance to the antinociceptive effects was observed on day 10. Behavioral hyperalgesia was verified 12 hr after withdrawal in another group that drank ethanol for 10 days. These results show that ethanol can affect the nociceptive responses related to deep pain evoked by the TMJ formalin test73263351336

Involvement of peripheral TRPV1 in TMJ hyperalgesia induced by ethanol withdrawal

CNPQ - CONSELHO NACIONAL DE DESENVOLVIMENTO CIENTÍFICO E TECNOLÓGICOEthanol withdrawal increases nociception after the injection of formalin into the rat's temporomandibular joint (TMJ). Little is known about the neurological basis for hyperalgesia induced by ethanol withdrawal, but it has been reported that ethanol can potentiate the response of transient receptor potential vanilloid receptor-1 (TRPV1) in superficial tissues. The present study was designed to test the hypothesis that peripheral TRPV1 could be involved on nociceptive behavioral responses induced by the injection of formalin into the TMJ region of rats exposed to chronic ethanol administration and ethanol withdrawal. Behavioral hyperalgesia was verified 12 h after ethanol withdrawal in rats that drank an ethanol solution (6.5%) for 10 days. In another group submitted to the same ethanol regimen, the selective vanilloid receptor antagonist capsazepine (300, 600 or 1200 microg/25 microl) or an equal volume of vehicle were injected into the TMJ regions 30 min before the TMJ formalin test. The local injections of capsazepine reduced the increased nociceptive responses induced by ethanol withdrawal. The effect of capsazepine on rats that did not drink ethanol was not significant. These results indicate that the peripheral TRPV1 can contribute to the hyperalgesia induced by ethanol withdrawal on deep pain conditions.Ethanol withdrawal increases nociception after the injection of formalin into the rat's temporomandibular joint (TMJ). Little is known about the neurological basis for hyperalgesia induced by ethanol withdrawal, but it has been reported that ethanol can potentiate the response of transient receptor potential vanilloid receptor-1 (TRPV1) in superficial tissues. The present study was designed to test the hypothesis that peripheral TRPV1 could be involved on nociceptive behavioral responses induced by the injection of formalin into the TMJ region of rats exposed to chronic ethanol administration and ethanol withdrawal. Behavioral hyperalgesia was verified 12 h after ethanol withdrawal in rats that drank an ethanol solution (6.5%) for 10 days. In another group submitted to the same ethanol regimen, the selective vanilloid receptor antagonist capsazepine (300, 600 or 1200 μg/25 μl) or an equal volume of vehicle were injected into the TMJ regions 30 min before the TMJ formalin test. The local injections of capsazepine reduced the increased nociceptive responses induced by ethanol withdrawal. The effect of capsazepine on rats that did not drink ethanol was not significant. These results indicate that the peripheral TRPV1 can contribute to the hyperalgesia induced by ethanol withdrawal on deep pain conditions8123-2416221626CNPQ - CONSELHO NACIONAL DE DESENVOLVIMENTO CIENTÍFICO E TECNOLÓGICOCNPQ - CONSELHO NACIONAL DE DESENVOLVIMENTO CIENTÍFICO E TECNOLÓGICOsem informaçã

The effects of restraint stress on nociceptive responses induced by formalin injected in rat's TMJ

CNPQ - CONSELHO NACIONAL DE DESENVOLVIMENTO CIENTÍFICO E TECNOLÓGICOFAPESP - FUNDAÇÃO DE AMPARO À PESQUISA DO ESTADO DE SÃO PAULOIt has been reported that stress can alter nociception from superficial tissues, such as skin and subcutaneous region. However, the influence of stress on an experimental deep nociception model is not understood. In this study, the temporomandibular joint (TMJ) formalin test was used to evaluate the effects of acute and chronic restraint stress on nociceptive responses in rats. Animals were initially submitted to one session of acute restraint stress (1 h) or exposed to chronic stress (40 days-1 h/day). Then, animals were killed immediately to collect blood for hormonal determinations by radioimmunoassay, or submitted to the TMJ formalin test to evaluate nociception. Rats submitted to acute restraint presented a performance similar to unstressed controls in the TMJ formalin test, whereas chronically stressed rats showed an increase in nociceptive responses. After 40 days of restraint, morphine was injected i.p. (1, 5 mg/kg or saline). The stressed rats displayed decreased morphine effects on nociception compared to unstressed controls. These findings suggest that repeated stress can produce hyperalgesia, which is, at least in part, due to alterations in the activity of opioid systems. This model may help elucidate the underlying neural mechanisms that mediate the effects of repeated stress on orofacial pain.It has been reported that stress can alter nociception from superficial tissues, such as skin and subcutaneous region. However, the influence of stress on an experimental deep nociception model is not understood. In this study, the temporomandibular joint (TMJ) formalin test was used to evaluate the effects of acute and chronic restraint stress on nociceptive responses in rats. Animals were initially submitted to one session of acute restraint stress (1 h) or exposed to chronic stress (40 days—1 h/day). Then, animals were killed immediately to collect blood for hormonal determinations by radioimmunoassay, or submitted to the TMJ formalin test to evaluate nociception. Rats submitted to acute restraint presented a performance similar to unstressed controls in the TMJ formalin test, whereas chronically stressed rats showed an increase in nociceptive responses. After 40 days of restraint, morphine was injected i.p. (1, 5 mg/kg or saline). The stressed rats displayed decreased morphine effects on nociception compared to unstressed controls. These findings suggest that repeated stress can produce hyperalgesia, which is, at least in part, due to alterations in the activity of opioid systems. This model may help elucidate the underlying neural mechanisms that mediate the effects of repeated stress on orofacial pain822338344CNPQ - CONSELHO NACIONAL DE DESENVOLVIMENTO CIENTÍFICO E TECNOLÓGICOFAPESP - FUNDAÇÃO DE AMPARO À PESQUISA DO ESTADO DE SÃO PAULOCNPQ - CONSELHO NACIONAL DE DESENVOLVIMENTO CIENTÍFICO E TECNOLÓGICOFAPESP - FUNDAÇÃO DE AMPARO À PESQUISA DO ESTADO DE SÃO PAUL

Peripheral sympathetic component of the temporomandibular joint inflammatory pain in rats

The aim of this study was to further validate our carrageenan-induced temporomandibular joint (TMJ) inflammatory hyperalgesia model in rats by showing that administration of indomethacin before the initiation of inflammation would diminish the TMJ hyperalgesia. Using this model, we investigated whether norepinephrine and local beta-adrenoceptors contribute to the development of inflammatory TMJ hyperalgesia. Carrageenan-induced TMJ hyperalgesia was assessed by measuring the behavioral nociceptive responses, such as rubbing the orofacial region and flinching the head, induced by the injection of a low dose of 5-hydroxytryptamine into the TMJ sensitized 1 h before by a TMJ injection of carrageenan. Blockade of prostaglandin synthesis by indomethacin prior to initiation of inflammation by carrageenan significantly attenuated the TMJ hyperalgesia. The guanethidine depletion of norepinephrine or the blockade of beta(2)but not the blockade of the beta(1)-adrenoceptor by the selective adrenoceptor antagonists ICI 118.55 and atenolol, respectively, significantly reduced carrageenan-induced TMJ hyperalgesia. In the present study, we further validated our carrageenan-induced TMJ hyperalgesia model to study the mechanisms involved in inflammatory TMJ hyperalgesia and to test the analgesic effect of different types of peripheral analgesics. We also demonstrated that norepinephrine released at the site of injury contributes to the development of the inflammatory TMJ hyperalgesia by the activation of beta(2)-adrenoceptors. The findings that local sympathomimetic amines contribute to the inflammatory TMJ hyperalgesia by activating beta(2)-adrenoceptors may be relevant to clinical TMJ inflammatory pain states less sensitive to nonsteroidal anti-inflammatory drugs.The aim of this study was to further validate our carrageenan-induced temporomandibular joint (TMJ) inflammatory hyperalgesia model in rats by showing that administration of indomethacin before the initiation of inflammation would diminish the TMJ hyperalgesia. Using this model, we investigated whether norepinephrine and local β-adrenoceptorscontribute to the development of inflammatory TMJ hyperalgesia. Carrageenan-induced TMJ hyperalgesia was assessed by measuring the behavioral nociceptive responses, such as rubbing the orofacial region and flinching the head, induced by the injection of a low dose of 5-hydroxytryptamine into the TMJ sensitized 1 h before by a TMJ injection of carrageenan. Blockade of prostaglandin synthesis by indomethacin prior to initiation of inflammation by carrageenan significantly attenuated the TMJ hyperalgesia. The guanethidine depletion of norepinephrine or the blockade of β2but not the blockade of the β1-adrenoceptor by the selective adrenoceptor antagonists ICI 118.55 and atenolol, respectively, significantly reduced carrageenan-induced TMJ hyperalgesia. In the present study, we further validated our carrageenan-induced TMJ hyperalgesia model to study the mechanisms involved in inflammatory TMJ hyperalgesia and to test the analgesic effect of different types of peripheral analgesics. We also demonstrated that norepinephrine released at the site of injury contributes to the development of the inflammatory TMJ hyperalgesia by the activation of β2-adrenoceptors71292993

The Effects Of Acute Restraint Stress On Nociceptive Responses Evoked By The Injection Of Formalin Into The Temporomandibular Joint Of Female Rats.

The temporomandibular joint (TMJ) formalin test was used to evaluate the effects of acute restraint stress on the nociceptive behavioral responses of female rats during proestrus and estrus phases of the estrous cycle. Rats were subjected to one session of restraint stress (15, 30 min or 1 h). They were then either immediately killed to allow the collection of blood for hormonal radioimmunoassay determinations or subjected to TMJ formalin test to evaluate nociception. All stress protocols significantly raised the plasma concentrations of corticosterone. The performance of rats subjected to 15 and 30 min of restraint stress was similar to that of control rats, whereas rats that were stressed for 1 h showed a decrease in nociceptive responses, during both proestrus and estrus phases. The stress-induced analgesia (SIA) was greater in the proestrus phase. To evaluate the role of kappa-opioid receptors, the selective receptor kappa-opioid antagonist nor-binaltorphimine (nor-BNI; 200 microg or saline) was injected into the TMJ 24 h prior to the 1 h stress period and the TMJ formalin test. The local administration of nor-BNI partially reversed the SIA during the proestrus phase. These findings suggest that (1) acute stress for 1 h can produce analgesia both during proestrus and estrus phases; this effect is greater during the proestrus phase and (2) kappa-opioid receptor activation is involved in the SIA observed in the proestrus phase.13269-7