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小鼠运动神经末梢递质释放与Ca2+内流的关系:导致异质性的随机因素的作用

The relation between transmitter release and Ca2+ entry at the mouse motor nerve terminal: role of stochastic factors causing heterogeneity.

作者信息

Quastel D M, Guan Y Y, Saint D A

机构信息

Department of Pharmacology & Therapeutics, Faculty of Medicine, University of British Columbia, Vancouver, Canada.

出版信息

Neuroscience. 1992 Dec;51(3):657-71. doi: 10.1016/0306-4522(92)90305-l.

Abstract

The relation between quantal transmitter release and presynaptic Ca2+/Ba2+ entry at the mouse neuromuscular junction was studied, making use of the finding that in the presence of Ba2+ trains of nerve stimuli or brief nerve terminal depolarizations elicit "tails" of raised miniature end-plate potential frequency (fm) that reflect entry of Ba2+ per pulse, and hence effectiveness of pulses in opening Ca2+/Ba2+ channels; at the same time these pulses elicit end-plate potentials. With nerve stimulation in the presence of Ba2+ and Ca2+ and modulation of release by raised Mg2+ or bekanamycin, slopes of log quantal content (m) vs log apparent Ba2+ entry per pulse were close to 4, which is the same as the Hill coefficient for Ba2+ cooperativity derived from other data. With depolarizing pulses of varied intensity, however, similar plots gave slopes close to 2, with Ba2+ alone or in a mixture of Ca2+ and Ba2+. Thus, the relation between transmitter release and Ca2+ (or Ba2+) entry apparently depends upon how entry is varied; varying the numbers of channels opened is not the same as varying ion entry per channel. A mathematical model was developed to examine the consequences of heterogeneity of local Ca2+ (or Ba2+) between release sites, arising because of stochastic variation of number and time course of Ca2+ channels opened per site; the experimental results were consistent with this model. It was therefore concluded that release is normally governed by intracellular Ca2+ close to points of Ca2+ entry through channels; stochastic factors give rise to more release than if Ca2+ were homogeneously distributed. If Ca2+ channels are uniformly close to release sites the average number of channels opened per site per action potential may be as low as 4.

摘要

利用以下发现,研究了小鼠神经肌肉接头处量子化递质释放与突触前Ca2+/Ba2+内流之间的关系:在Ba2+存在的情况下,一连串的神经刺激或短暂的神经末梢去极化会引发微小终板电位频率(fm)升高的“尾状”现象,这反映了每个脉冲Ba2+的内流情况,从而反映了脉冲在打开Ca2+/Ba2+通道方面的有效性;与此同时,这些脉冲会引发终板电位。在Ba2+和Ca2+存在的情况下进行神经刺激,并通过升高Mg2+或贝卡霉素来调节释放,量子含量对数(m)与每个脉冲表观Ba2+内流对数的斜率接近4,这与从其他数据得出的Ba2+协同作用的希尔系数相同。然而,对于强度不同的去极化脉冲,无论是单独使用Ba2+还是在Ca2+和Ba2+的混合物中,类似的图表给出的斜率都接近2。因此,递质释放与Ca2+(或Ba2+)内流之间的关系显然取决于内流的变化方式;改变打开的通道数量与改变每个通道的离子内流情况不同。开发了一个数学模型来研究由于每个释放位点打开的Ca2+通道数量和时间进程的随机变化而导致的释放位点之间局部Ca2+(或Ba2+)异质性的后果;实验结果与该模型一致。因此得出结论,释放通常受靠近通过通道进入的Ca2+点的细胞内Ca2+控制;随机因素导致的释放比Ca2+均匀分布时更多。如果Ca2+通道均匀地靠近释放位点,每个动作电位每个位点打开的通道平均数量可能低至4个。

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