美索铵化合物对大鼠下颌下神经节细胞的通道阻断作用。
The channel-blocking action of methonium compounds on rat submandibular ganglion cells.
作者信息
Gurney A M, Rang H P
出版信息
Br J Pharmacol. 1984 Jul;82(3):623-42. doi: 10.1111/j.1476-5381.1984.tb10801.x.
The effects of drugs of the polymethylene bis-trimethylammonium (methonium) series on the characteristics of the synaptic currents (e.s.cs) recorded from voltage-clamped rat submandibular ganglion cells have been studied. The drugs studied were from C4 to C10 (decamethonium). All of the drugs except C4 shortened the initial decay phase of the e.s.c.; C9 and C10 produced an additional slowly decaying component. These effects were interpreted in terms of an open channel block mechanism, the calculated rate constants for association with the open channel at -80 mV being fairly similar (5.9 X 10(6) to 18.1 X 10(6)M-1S-1) for all of the compounds except C4, which had no effect on the e.s.c. decay. All of the compounds produced use-dependent block when tested with short trains of stimuli at 10 Hz, or with trains of ionophoretic pulses of acetylcholine, consistent with their channel blocking property. Tubocurarine had a similar effect, but not trimetaphan or mecamylamine. Recovery from use-dependent block with short chain methonium compounds, up to C8, was very slow in the absence of agonist, being incomplete even after several minutes. With C9 or C10 or tubocurarine, recovery from use-dependent block was complete within a few seconds. With C6 recovery in the absence of agonist was unaffected by membrane potential, but could be accelerated by applying acetylcholine with the cell depolarized to -40 mV. This persistent block was ascribed to the ability of the blocking molecule to become trapped by closure of the channel. With C9 and C10 it is assumed that their presence inhibits channel closure, so they can escape without the help of agonist. When use-dependent block is avoided by leaving the ganglion unstimulated during equilibration with the blocking drug, the first e.s.c. elicited shows no appreciable reduction of amplitude, though with C6, C7 or C8 subsequent responses elicited at 0.1 Hz become progressively more blocked. Even at 1 mM, C6 does not prevent acetylcholine from opening ionic channels. It is concluded that all of the effects on e.s.c. amplitude can be interpreted in terms of channel block, there being no evidence of any receptor blocking action.
研究了聚亚甲基双三甲基铵(甲铵)系列药物对电压钳制的大鼠下颌下神经节细胞记录的突触电流(e.s.cs)特性的影响。所研究的药物从C4到C10(十烃季铵)。除C4外,所有药物均缩短了e.s.c.的初始衰减期;C9和C10产生了一个额外的缓慢衰减成分。这些效应根据开放通道阻断机制进行解释,在-80 mV下与开放通道结合的计算速率常数对于除C4外的所有化合物相当相似(5.9×10⁶至18.1×10⁶M⁻¹S⁻¹),C4对e.s.c.衰减没有影响。当用10 Hz的短串刺激或乙酰胆碱离子电泳脉冲串进行测试时,所有化合物均产生使用依赖性阻断,这与其通道阻断特性一致。筒箭毒碱有类似作用,但三甲噻方或美加明没有。在没有激动剂的情况下,短链甲铵化合物(直至C8)从使用依赖性阻断中的恢复非常缓慢,即使几分钟后也不完全。使用C9或C10或筒箭毒碱时,可以在几秒钟内从使用依赖性阻断中完全恢复。使用C6时,在没有激动剂的情况下,恢复不受膜电位影响,但当细胞去极化至-40 mV并施加乙酰胆碱时可以加速恢复。这种持续性阻断归因于阻断分子被通道关闭捕获的能力。对于C9和C10,假定它们的存在抑制通道关闭,因此它们可以在没有激动剂帮助的情况下逃脱。当在与阻断药物平衡期间不刺激神经节以避免使用依赖性阻断时,诱发的第一个e.s.c.幅度没有明显降低,尽管使用C6、C7或C8时,以0.1 Hz诱发的后续反应逐渐被更多地阻断。即使在1 mM时,C6也不会阻止乙酰胆碱打开离子通道。得出的结论是,对e.s.c.幅度的所有影响都可以根据通道阻断来解释,没有任何受体阻断作用的证据。
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