The action of four proposed chloride movement modifiers on acetylcholine responses of central neurones of Helix aspersa

Comparative biochemistry and physiology. C: Comparative pharmacology Pub Date : 1993-06-01 DOI:10.1016/0742-8413(93)90213-5

N.J.D. Wright , R.J. Walker

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引用次数: 2

Abstract

1. Intracellular recordings were made from identified neurones in the visceral, (abdominal) ganglion of the snail, Helix aspersa. The hyperpolarising response of neurone E4 is a pure chloride event and has a reversal potential, (E_Cl), of −69.7 ± 1.7mV, (n = 4). This can be compared to depolarising responses of neurones E1 and E2 which are sodium mediated.

2. Four membrane transport system antagonists, all thought to affect trans-membrane chloride movement, were investigated with respect to the two different acetylcholine responses described.

3. Piretanide irreversibly blocks the hyperpolarising response in cell E4, (1–10 μM), increasing its inhibition with time but without changing E_Cl.

4. Furosemide irreversibly blocks both types of acetylcholine responses at concentrations in the nanomolar range; no change in E_Cl or E_Na was associated with the inhibition but the “passive” membrane resistance appeared to decrease. Inhibition increased with time, normally causing a significant effect after 10–30 min.

5. S.I.T.S. and ethacrynic acid appear very similar in effect; both reversibly block the two responses to acetylcholine and recovery after washing is virtually complete. The onset of antagonism is rapid and both compounds are slightly more effective against the hyperpolarising (“H”), response than the depolarising (“D”) response (threshold ∼10⁻⁵ M compared to ∼ 10⁻⁴ M). No change in E_Cl or E_Na was noted.

6. Piretanide and furosemide probably exert their effect by interactions with the neuronal cell membrane, disrupting the integrity of this structure, whereas S.I.T.S. and ethacrynic acid may interact more specifically with the acetylcholine receptor protein.

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四种氯离子运动调节剂对螺旋树中枢神经元乙酰胆碱反应的影响

1. 在蜗牛的内脏(腹部)神经节中对已识别的神经元进行细胞内记录。神经元E4的超极化反应是一个纯氯事件，其反转电位(ECl)为- 69.7±1.7mV， (n = 4)。这可以与钠介导的神经元E1和E2的去极化反应进行比较。四种膜运输系统拮抗剂，都被认为影响跨膜氯离子运动，研究了两种不同的乙酰胆碱反应。吡雷他尼不可逆地阻断细胞E4的超极化反应，(1-10 μM)，随着时间的推移增强其抑制作用，但不改变ECl.4。速尿在纳摩尔浓度范围内不可逆地阻断两种类型的乙酰胆碱反应;ECl和ENa的变化与抑制无关，但“被动”膜抗性似乎有所下降。抑制作用随时间增加而增加，通常在10-30分钟后产生显著效果5。S.I.T.S.和乙稀酸的效果非常相似;两者都可逆地阻断对乙酰胆碱的两种反应，洗涤后几乎完全恢复。拮抗作用起效迅速，两种化合物对超极化反应(“H”)比去极化反应(“D”)更有效(阈值为~ 10−5 M与~ 10−4 M相比)。ECl或ENa没有变化。吡雷他胺和速尿可能通过与神经元细胞膜的相互作用来发挥作用，破坏这种结构的完整性，而S.I.T.S.和乙酸可能与乙酰胆碱受体蛋白更特异性地相互作用。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Comparative biochemistry and physiology. C: Comparative pharmacology

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