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三硝基苯类似物在青蛙神经肌肉接头处的突触前效应。

Presynaptic effects of a trinitrobenzene analogue at the frog neuromuscular junction.

作者信息

Osanai M, Tsuji A, Suzuki N, Kijima H

机构信息

Department of Physics, School of Science, Nagoya University, Japan.

出版信息

J Neurophysiol. 1996 Sep;76(3):1735-43. doi: 10.1152/jn.1996.76.3.1735.

Abstract
  1. Application of 0.15 mM 1-(hydroxyethylamino)-2,4,6-trinitrobenzene (HEATNB) to the frog neuromuscular junction induced a marked increase (4.0-fold) in the amplitude of nerve-evoked end-plate potentials (EPPs) obtained from intracellular and extracellular records, but only a slight increase (1.9-fold) in the frequency of miniature EPPs (MEPPs) obtained from intracellular records. The effects of HEATNB on EPP amplitude and MEPP frequency showed a similar time course, reaching a plateau level approximately 40 min after the start of application and returning to the control level after wash. The difference in the effects of HEATNB on EPP and MEPP frequency suggests that it specifically enhances synchronous transmitter release. 2. Comparing the effects and structure of HEATNB with those of 2,4,6-trinitrobenzene-1-sulfonic acid, we conclude that the observed increase in transmitter release is due to the effects of the trinitrobenzene moiety of those reagents. 3. The distribution of MEPP amplitude was unchanged by HEATNB treatment, indicating that its effects are presynaptic. 4. Among four components of short-term synaptic plasticity, HEATNB greatly decreased (approximately 70%) augmentation and increased (approximately 50%) potentiation, but had little effect on fast and slow facilitations. These results suggest that each of the short-term plasticities has a different mechanism and that HEATNB affects the same mechanisms as those of augmentation. 5. Even when a calcium chelator, bis-(o-aminophenoxy)-N,N,N',N'-tetraacetic acid, was loaded into the presynaptic nerve terminal, the effects of HEATNB were not changed in nature, suggesting that effects of HEATNB persist independently of intracellular Ca2+ concentration. 6. These observations suggest that HEATNB may affect specific protein(s) involved primarily in synchronous transmitter release and not asynchronous release.
摘要
  1. 将0.15 mM的1-(羟乙氨基)-2,4,6-三硝基苯(HEATNB)应用于青蛙神经肌肉接头,可使细胞内和细胞外记录得到的神经诱发终板电位(EPPs)幅度显著增加(4.0倍),但仅使细胞内记录得到的微小终板电位(MEPPs)频率略有增加(1.9倍)。HEATNB对EPP幅度和MEPP频率的影响呈现相似的时间进程,在应用开始后约40分钟达到平台期水平,冲洗后恢复到对照水平。HEATNB对EPP和MEPP频率影响的差异表明它特异性增强了同步递质释放。2. 通过比较HEATNB与2,4,6-三硝基苯-1-磺酸的作用和结构,我们得出观察到的递质释放增加是由于这些试剂的三硝基苯部分的作用。3. HEATNB处理后MEPP幅度的分布未改变,表明其作用是突触前的。4. 在短期突触可塑性的四个成分中,HEATNB使增强作用大幅降低(约70%),使易化作用增加(约50%),但对快速和慢速易化作用影响很小。这些结果表明每种短期可塑性具有不同的机制,且HEATNB影响与增强作用相同的机制。5. 即使将钙螯合剂双-(邻氨基苯氧基)-N,N,N',N'-四乙酸加载到突触前神经末梢,HEATNB的作用本质上也未改变,表明HEATNB的作用独立于细胞内Ca2+浓度持续存在。6. 这些观察结果表明,HEATNB可能影响主要参与同步递质释放而非异步释放的特定蛋白质。

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