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论钡在支持运动神经冲动引发乙酰胆碱量子异步释放中的作用。

On the role of barium in supporting the asynchronous release of acetylcholine quanta by motor nerve impulses.

作者信息

Silinsky E M

出版信息

J Physiol. 1978 Jan;274:157-71. doi: 10.1113/jphysiol.1978.sp012141.

Abstract
  1. The effect of Ba2+ on the evoked secretion of individual acetylcholine (ACh) quanta was studied on frog neuromuscular junctions using conventional electro-physiological techniques. 2. In solutions containing 1.8 mM-Ba2+ and no added Ca2+, 1 Hz stimulation for less than 1 min elevated miniature end-plate potential (m.e.p.p.) frequencies to 5-20 times the control level (seven experiments). Similar results were obtained when a Ca2+-chelating agent was added to the Ba2+ solution. 3. Repetitive nerve stimulation at frequencies greater than 1 Hz in concentrations of Ba2+ greater than or equal to 1.8 mM elevated m.e.p.p. frequencies to unmeasurable levels (greater than 100/sec). Such high m.e.p.p. frequencies were accompanied by a steady depolarization of the post-synaptic membrane, which was used to estimate the number of ACh quanta released. 4. The number of ACh quanta released asynchronously by nerve impulses was directly related to the external concentration of Ba2+ in a non-linear fashion. 5. Ba2+ was two orders of magnitude more effective than Ca2+ in supporting the evoked discharge of m.e.p.p.s. Ca2+ was a potent antagonist of asynchronous release in Ba2+ solutions. 6. Mg2+ and Co2+ both competitively antagonized evoked release in Ba2+ solutions. The equilibrium dissociation constant for each ion as an antagonist of asynchronous, Ba2+-dependent release was similar to its corresponding value as an antagonist of synchronous, Ca2+-mediated release. 7. It is suggested that Ba2+ supports dispersed, quantal ACh release directly by acting through the same conductance pathway normally traversed by Ca2+.
摘要
  1. 运用传统电生理技术,在青蛙神经肌肉接头处研究了Ba2+对单个乙酰胆碱(ACh)量子诱发分泌的影响。2. 在含有1.8 mM - Ba2+且未添加Ca2+的溶液中,1 Hz刺激不到1分钟可使微小终板电位(m.e.p.p.)频率升高至对照水平的5 - 20倍(七次实验)。当向Ba2+溶液中添加Ca2+螯合剂时,也得到了类似结果。3. 在浓度大于或等于1.8 mM的Ba2+溶液中,频率大于1 Hz的重复神经刺激可使m.e.p.p.频率升高至无法测量的水平(大于100/秒)。如此高的m.e.p.p.频率伴随着突触后膜的稳定去极化,后者被用于估计释放的ACh量子数量。4. 神经冲动异步释放的ACh量子数量与Ba2+的外部浓度呈非线性直接相关。5. 在支持m.e.p.p.s的诱发释放方面,Ba2+的效力比Ca2+高两个数量级。Ca2+是Ba2+溶液中异步释放的有效拮抗剂。6. Mg2+和Co2+在Ba2+溶液中均竞争性拮抗诱发释放。作为异步的、依赖Ba2+释放的拮抗剂,每种离子的平衡解离常数与其作为同步的、Ca2+介导释放的拮抗剂的相应值相似。7. 有人提出,Ba2+通过作用于通常由Ca2+穿过的相同电导途径,直接支持分散的、量子化的ACh释放。

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