镧作为钙的替代物在小鼠运动神经末梢递质释放中的作用
Lanthanum as a surrogate for calcium in transmitter release at mouse motor nerve terminals.
作者信息
Curtis M J, Quastel D M, Saint D A
出版信息
J Physiol. 1986 Apr;373:243-60. doi: 10.1113/jphysiol.1986.sp016045.
The mechanism by which lanthanum (La3+) causes an increased frequency of miniature end-plate potentials (m.e.p.p.s) was studied at the mouse neuromuscular junction. At concentrations as low as 0.25 microM, La3+ caused a progressive rise in m.e.p.p. frequency, to a maximum of several hundred per second. 'Washing' with solution containing EDTA arrested the rise, but did not substantially reduce the raised m.e.p.p. frequency. At partially 'lanthanized' junctions high frequencies of m.e.p.p.s were maintained indefinitely, even in 0 Ca2+/EDTA solutions. The rate of development of high m.e.p.p. frequency was increased by repetitive nerve stimulation or by depolarization of the nerve terminal (high K+ or focally applied current), and appeared to be proportional to the concentration of La3+ over the range of 0.25-5 microM. At low concentrations of La3+ the rise of m.e.p.p. frequency depended upon the co-presence of a small amount of Ca2+ (greater than 10 microM) and was slowed and partially blocked by Cd2+, or by Ca2+ at about 10 microM. The quantal content of end-plate potentials was usually reduced in the presence of La3+, but was increased over control values after removal of La3+ by 'washing' with solution containing EDTA, once a raised m.e.p.p. frequency had developed. At partially lanthanized junctions the absolute increases in m.e.p.p. frequency produced by Ca2+ (in raised K+), ethanol, or by nerve stimulation in the presence of Ba2+, were greater than at control junctions, but in each case the increases in the logarithm of m.e.p.p. frequency were less than at control junctions. It is concluded that La3+ causes transmitter release only after entry into the nerve terminal via voltage-sensitive channels, probably those that normally admit Ca2+, that La3+ and Ca2+ may co-operate at internal sites to induce transmitter release, and that these ions both co-operate and compete at external sites that regulate their entry into the nerve terminal.
在小鼠神经肌肉接头处研究了镧(La3+)导致微小终板电位(m.e.p.p.s)频率增加的机制。在低至0.25微摩尔的浓度下,La3+使m.e.p.p.频率逐渐升高,最高可达每秒数百次。用含有乙二胺四乙酸(EDTA)的溶液“冲洗”可使升高停止,但不会使升高的m.e.p.p.频率大幅降低。在部分“镧化”的接头处,即使在0钙离子/EDTA溶液中,m.e.p.p.s的高频也能无限期维持。重复神经刺激或神经末梢去极化(高钾或局部施加电流)可加快高m.e.p.p.频率的发展速度,且在0.25 - 5微摩尔范围内,其发展速度似乎与La3+浓度成正比。在低浓度的La3+时,m.e.p.p.频率的升高依赖于少量钙离子(大于10微摩尔)的共存,并且会被镉离子(Cd2+)或约10微摩尔的钙离子减缓并部分阻断。在存在La3+的情况下,终板电位的量子含量通常会降低,但在用含有EDTA的溶液“冲洗”去除La3+后,一旦m.e.p.p.频率升高,其量子含量会比对照值增加。在部分镧化的接头处,由钙离子(在高钾中)、乙醇或在钡离子(Ba2+)存在下神经刺激所产生的m.e.p.p.频率的绝对增加量大于对照接头,但在每种情况下,m.e.p.p.频率对数的增加量小于对照接头。得出的结论是,La3+只有在通过电压敏感通道进入神经末梢后才会导致递质释放,可能是那些通常允许钙离子进入的通道,La3+和钙离子可能在内部位点协同作用以诱导递质释放,并且这些离子在调节它们进入神经末梢的外部位点既协同又竞争。
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