氨氯地平类似物对豚鼠气道传入神经元机械激活的抑制作用。
Inhibition of mechanical activation of guinea-pig airway afferent neurons by amiloride analogues.
作者信息
Carr M J, Gover T D, Weinreich D, Undem B J
机构信息
Johns Hopkins Asthma and Allergy Center, 5501 Hopkins Bayview Circle, Baltimore, MD 21224, USA.
出版信息
Br J Pharmacol. 2001 Aug;133(8):1255-62. doi: 10.1038/sj.bjp.0704197.
Abstract
- The aim of this study was to investigate a role for Epithelial Sodium Channels (ENaCs) in the mechanical activation of low-threshold vagal afferent nerve terminals in the guinea-pig trachea/bronchus. 2. Using extracellular single-unit recording techniques, we found that the ENaC blocker amiloride, and its analogues dimethylamiloride and benzamil caused a reduction in the mechanical activation of guinea-pig airway afferent fibres. 3. Amiloride and it analogues also reduced the sensitivity of afferent fibres to electrical stimulation such that greater stimulation voltages were required to induce action potentials from their peripheral terminals within the trachea/bronchus. 4. The relative potencies of these compounds for inhibiting electrical excitability of afferent nerves were similar to that observed for inhibition of mechanical stimulation (dimethylamiloride approximately benzamil > amiloride). This rank order of potency is incompatible with the known rank order of potency for blockade of ENaCs (benzamil > amiloride >> dimethylamiloride). 5. As voltage-gated sodium channels play an important role in determining the electrical excitability of neurons, we used whole-cell patch recordings of nodose neuron cell bodies to investigate the possibility that amiloride analogues caused blockade of these channels. At the concentration required to inhibit mechanical activation of vagal nodose afferent fibres (100 microM), benzamil caused significant inhibition of voltage-gated sodium currents in neuronal cell bodies acutely isolated from guinea-pig nodose ganglia. 6. Combined, our findings suggest that amiloride and its analogues did not selectively block mechanotransduction in airway afferent neurons, but rather they reduced neuronal excitability, possibly by inhibiting voltage-gated sodium currents.
摘要
- 本研究的目的是探究上皮钠通道(ENaCs)在豚鼠气管/支气管中低阈值迷走传入神经末梢机械激活过程中的作用。2. 使用细胞外单单位记录技术,我们发现ENaC阻滞剂氨氯吡脒及其类似物二甲基氨氯吡脒和苄氯噻嗪可降低豚鼠气道传入纤维的机械激活。3. 氨氯吡脒及其类似物还降低了传入纤维对电刺激的敏感性,以至于需要更高的刺激电压才能从气管/支气管内的外周末梢诱发动作电位。4. 这些化合物抑制传入神经电兴奋性的相对效力与抑制机械刺激时观察到的效力相似(二甲基氨氯吡脒≈苄氯噻嗪>氨氯吡脒)。这种效力顺序与已知的ENaCs阻断效力顺序(苄氯噻嗪>氨氯吡脒>>二甲基氨氯吡脒)不相符。5. 由于电压门控钠通道在决定神经元电兴奋性方面起重要作用,我们使用结状神经元胞体的全细胞膜片钳记录来研究氨氯吡脒类似物是否会阻断这些通道。在抑制迷走结状传入纤维机械激活所需的浓度(100μM)下,苄氯噻嗪可显著抑制从豚鼠结状神经节急性分离的神经元胞体中的电压门控钠电流。6. 综合来看,我们的研究结果表明氨氯吡脒及其类似物并未选择性地阻断气道传入神经元的机械转导,而是通过抑制电压门控钠电流降低了神经元的兴奋性。
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