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首页> 外文期刊>Sleep & breathing =: Schlaf & Atmung >Differential respiratory control of the upper airway and diaphragm muscles induced by 5-HT1A receptor ligands.
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Differential respiratory control of the upper airway and diaphragm muscles induced by 5-HT1A receptor ligands.

机译:5-HT1A受体配体诱导的上呼吸道和diaphragm肌的差分呼吸控制。

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摘要

Serotonin (5-HT) has a role in respiratory function and dysfunction. Although 5-HT affects respiratory drive to both phrenic and cranial motoneurons, relatively little is known about the role of 5-HT receptor subtypes in the control of upper airway muscle (UAM) respiratory activity.Here, we performed central injections of 5-HT1A agonist (8-OHDPAT) or antagonist (WAY100635) in anesthetized rats and analyzed changes in the electromyographic activity of several UAM and other cardiorespiratory parameters. We also compared the pattern of Fos expression induced after central injection of a control solution or 8-OHDPAT.Results showed that 8-OHDPAT induced a robust increase in UAM activity, associated with either tachypnea under volatile anesthesia or bradypnea under liquid anesthesia. Injection of WAY100635 switched off UAM respiratory activity and led to bradypnea, suggesting a tonic excitatory role of endogenous 5-HT1A receptor activation. Co-injection of the agonist and the antagonist blocked the effects produced by each drug alone. Besides drug-induced changes in respiratory frequency, only slight increases in surface of diaphragm bursts were observed. Significant increases in Fos expression after 5-HT1A receptor activation were seen in the nucleus tractus solitarius, nucleus raphe pallidus, parapyramidal region, retrotrapezoid nucleus, lateral parabrachial, and K?lliker-Fuse nuclei. This restricted pattern of Fos expression likely identified the neural substrate responsible for the enhancement of UAM respiratory activity observed after 8-OHDPAT injection.These findings suggest an important role for the 5-HT1A receptors in the neural control of upper airway patency and may be relevant to counteract pharyngeal atonia during obstructive sleep apneas.
机译:血清素(5-HT)在呼吸功能和功能障碍中起作用。尽管5-HT影响respiratory和颅神经元的呼吸驱动,但对5-HT受体亚型在控制上呼吸道肌肉(UAM)呼吸活动中的作用的了解还很少。在这里,我们进行了5-HT1A的中央注射激动剂(8-OHDPAT)或拮抗剂(WAY100635)在麻醉的大鼠中进行,并分析了一些UAM的肌电图活性和其他心肺参数的变化。我们还比较了集中注射对照溶液或8-OHDPAT后诱导的Fos表达模式。结果显示8-OHDPAT诱导UAM活性强劲增加,与挥发性麻醉下的呼吸急促或液体麻醉下的呼吸急促有关。注射WAY100635会关闭UAM呼吸活动并导致呼吸短促,表明内源性5-HT1A受体激活会产生兴奋性兴奋作用。激动剂和拮抗剂的共同注射阻断了每种药物单独产生的作用。除了药物引起的呼吸频率变化外,仅观察到of肌爆发表面的轻微增加。 5-HT1A受体激活后,在孤核、,核,锥体束旁区域,梯形后核,臂旁旁核和K?lliker-Fuse核中,Fos表达显着增加。 Fos表达的这种受限模式可能确定了注射8-OHDPAT后观察到的UAM呼吸活动增强的神经底物。这些发现表明5-HT1A受体在上呼吸道通畅神经控制中的重要作用,可能与以抵消阻塞性睡眠呼吸暂停期间的咽部肌萎缩。

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