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首页> 外文期刊>The Journal of Pharmacology and Experimental Therapeutics: Official Publication of the American Society for Pharmacology and Experimental Therapeutics >Orexins depolarize rostral ventrolateral medulla neurons and increase arterial pressure and heart rate in rats mainly via orexin 2 receptors.
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Orexins depolarize rostral ventrolateral medulla neurons and increase arterial pressure and heart rate in rats mainly via orexin 2 receptors.

机译:食欲素主要通过食欲素2受体使大鼠前额腹外侧延髓神经元去极化,并增加动脉压和心率。

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摘要

An injection of orexin A or B into the cisterna magna or the rostral ventrolateral medulla (RVLM), where bulbospinal vasomotor neurons are located, elevated arterial pressure (AP) and heart rate (HR). We examined how orexins affected RVLM neurons to regulate cardiovascular functions by using in vitro recordings of neuronal activity of the RVLM and in vivo measurement of cardiovascular functions in rats. Orexin A and B concentration-dependently depolarized RVLM neurons. At 100 nM, both peptides excited 42% of RVLM neurons. Tetrodotoxin failed to block orexin-induced depolarization. In the presence of N-(2-methyl-6-benzoxazolyl)-N'-1, 5-naphthyridin-4-yl urea (SB-334867), an orexin 1 receptor (OX(1)R) antagonist, orexin A depolarized 42% of RVLM neurons with a smaller, but not significantly different, amplitude (4.9 +/- 0.8 versus 7.2 +/- 1.1 mV). In the presence of (2S)-1- (3,4-dihydro-6,7-dimethoxy-2(1H)-isoquinolinyl)-3,3-dimethyl-2-[(4-pyridinylmethy l)amino]-1-butanone hydrochloride (TCS OX2 29), an orexin 2 receptor (OX(2)R) antagonist, orexin A depolarized 25% of RVLM neurons with a significantly smaller amplitude (1.7 +/- 0.5 mV). Coapplication of both antagonists completely eliminated orexin A-induced depolarization. An OX(2)R agonist, [Ala(11),D-Leu(15)]-orexin B, concentration-dependently depolarized RVLM neurons. Regarding neuronal phenotypes, orexins depolarized 88% of adrenergic, 43% of nonadrenergic, and 36 to 41% of rhythmically firing RVLM neurons. Intracisternal TCS OX2 29 (3 and 10 nmol) suppressed intracisternal orexin A-induced increases of AP and HR, whereas intracisternal SB-334867 (3 and 10 nmol) had no effect on the orexin A-induced increase of HR but suppressed the orexin A-induced pressor response at 10 nmol. We concluded that orexins directly excite RVLM neurons, which include bulbospinal vasomotor neurons, and regulate cardiovascular function mainly via the OX(2)R, with a smaller contribution from the OX(1)R.
机译:将食欲素A或B注射到巨大的水罐或延髓的腹侧延髓(RVLM)中,这是球囊顶血管舒缩神经元的所在,动脉压(AP)和心率(HR)升高。我们通过使用RVLM神经元活性的体外记录和大鼠心血管功能的体内测量,研究了orexins如何影响RVLM神经元以调节心血管功能。食欲素A和B依赖浓度的去极化RVLM神经元。在100 nM时,两种肽均激发42%的RVLM神经元。河豚毒素不能阻止由食欲素引起的去极化。在N-(2-甲基-6-苯并恶唑基)-N'-1、5-萘啶-4-基尿素(SB-334867),一种orexin 1受体(OX(1)R)拮抗剂,orexin A的存在下去极化42%的RVLM神经元,其幅度较小,但差异不显着(4.9 +/- 0.8对7.2 +/- 1.1 mV)。在(2S)-1-(3,4-二氢-6,7-二甲氧基-2(1H)-异喹啉基)-3,3-二甲基-2-[[(4-吡啶基甲基)氨基] -1的存在下-盐酸丁酮(TCS OX2 29),orexin 2受体(OX(2)R)拮抗剂orexin A使25%的RVLM神经元去极化,幅度明显较小(1.7 +/- 0.5 mV)。两种拮抗剂的共同应用完全消除了食欲素A引起的去极化。 OX(2)R激动剂,[Ala(11),D-Leu(15)]-orexin B,浓度依赖性去极化RVLM神经元。关于神经元表型,食欲素使88%的肾上腺素能去极化,43%的非肾上腺素能去极化以及有节奏地激发RVLM神经元的36-41%。颅内TCS OX2 29(3和10 nmol)抑制了脑内食欲素A引起的AP和HR升高,而脑内SB-334867(3和10 nmol)对食欲素A引起的HR升高没有影响,但抑制了Orexin A诱导的10 nmol升压反应。我们得出的结论是,orexin可以直接激发RVLM神经元,其中包括球形脊髓血管舒缩神经元,并主要通过OX(2)R调节心血管功能,而OX(1)R的贡献较小。

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