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通过多概率波动分析在大鼠攀缘纤维-浦肯野细胞突触处确定的频率依赖性抑制位点。

Locus of frequency-dependent depression identified with multiple-probability fluctuation analysis at rat climbing fibre-Purkinje cell synapses.

作者信息

Silver R A, Momiyama A, Cull-Candy S G

机构信息

Department of Pharmacology, University College London, Gower Street, London WC1E 6BT, UK.

出版信息

J Physiol. 1998 Aug 1;510 ( Pt 3)(Pt 3):881-902. doi: 10.1111/j.1469-7793.1998.881bj.x.

Abstract
  1. EPSCs were recorded under whole-cell voltage clamp at room temperature from Purkinje cells in slices of cerebellum from 12- to 14-day-old rats. EPSCs from individual climbing fibre (CF) inputs were identified on the basis of their large size, paired-pulse depression and all-or-none appearance in response to a graded stimulus. 2. Synaptic transmission was investigated over a wide range of experimentally imposed release probabilities by analysing fluctuations in the peak of the EPSC. Release probability was manipulated by altering the extracellular [Ca2+] and [Mg2+]. Quantal parameters were estimated from plots of coefficient of variation (CV) or variance against mean conductance by fitting a multinomial model that incorporated both spatial variation in quantal size and non-uniform release probability. This 'multiple-probability fluctuation' (MPF) analysis gave an estimate of 510 +/- 50 for the number of functional release sites (N) and a quantal size (q) of 0.5 +/- 0.03 nS (n = 6). 3. Control experiments, and simulations examining the effects of non-uniform release probability, indicate that MPF analysis provides a reliable estimate of quantal parameters. Direct measurement of quantal amplitudes in the presence of 5 mM Sr2+, which gave asynchronous release, yielded distributions with a mean quantal size of 0.55 +/- 0.01 nS and a CV of 0.37 +/- 0.01 (n = 4). Similar estimates of q were obtained in 2 mM Ca2+ when release probability was lowered with the calcium channel blocker Cd2+. The non-NMDA receptor antagonist 6-cyano-7-nitroquinoxaline-2,3-dione (CNQX; 1 microM) reduced both the evoked current and the quantal size (estimated with MPF analysis) to a similar degree, but did not affect the estimate of N. 4. We used MPF analysis to identify those quantal parameters that change during frequency-dependent depression at climbing fibre-Purkinje cell synaptic connections. At low stimulation frequencies, the mean release probability (pr) was unusually high (0.90 +/- 0.03 at 0.033 Hz, n = 5), but as the frequency of stimulation was increased, pr fell dramatically (0.02 +/- 0.01 at 10 Hz, n = 4) with no apparent change in either q or N. This indicates that the observed 50-fold depression in EPSC amplitude is presynaptic in origin. 5. Presynaptic frequency-dependent depression was investigated with double-pulse and multiple-pulse protocols. EPSC recovery, following simultaneous release at practically all sites, was slow, being well fitted by the sum of two exponential functions (time constants of 0.35 +/- 0.09 and 3.2 +/- 0.4 s, n = 5). EPSC recovery following sustained stimulation was even slower. We propose that presynaptic depression at CF synapses reflects a slow recovery of release probability following release of each quantum of transmitter. 6. The large number of functional release sites, relatively large quantal size, and unusual dynamics of transmitter release at the CF synapse appear specialized to ensure highly reliable olivocerebellar transmission at low frequencies but to limit transmission at higher frequencies.
摘要
  1. 在室温下,于全细胞电压钳模式下,从12至14日龄大鼠的小脑切片中的浦肯野细胞记录兴奋性突触后电流(EPSCs)。来自单个攀缘纤维(CF)输入的EPSCs根据其大尺寸、双脉冲抑制以及对分级刺激的全或无出现来识别。2. 通过分析EPSC峰值的波动,在广泛的实验施加的释放概率范围内研究突触传递。通过改变细胞外[Ca2+]和[Mg2+]来操纵释放概率。通过拟合包含量子大小的空间变化和非均匀释放概率的多项式模型,从变异系数(CV)或方差对平均电导的图中估计量子参数。这种“多概率波动”(MPF)分析得出功能释放位点数量(N)的估计值为510±50,量子大小(q)为0.5±0.03 nS(n = 6)。3. 对照实验以及检查非均匀释放概率影响的模拟表明,MPF分析提供了量子参数的可靠估计。在5 mM Sr2+存在下直接测量量子幅度,其产生异步释放,得到的分布的平均量子大小为0.55±0.01 nS,CV为0.37±0.01(n = 4)。当用钙通道阻滞剂Cd2+降低释放概率时,在2 mM Ca2+中获得了类似的q估计值。非NMDA受体拮抗剂6-氰基-7-硝基喹喔啉-2,3-二酮(CNQX;1 μM)将诱发电流和量子大小(用MPF分析估计)降低到相似程度,但不影响N的估计值。4. 我们使用MPF分析来识别在攀缘纤维-浦肯野细胞突触连接的频率依赖性抑制过程中发生变化的那些量子参数。在低刺激频率下,平均释放概率(pr)异常高(在0.033 Hz时为0.90±0.03,n = 5),但随着刺激频率增加,pr急剧下降(在10 Hz时为0.02±0.01,n = 4),而q或N均无明显变化。这表明观察到的EPSC幅度50倍的抑制起源于突触前。5. 用双脉冲和多脉冲方案研究突触前频率依赖性抑制。在几乎所有位点同时释放后,EPSC恢复缓慢,可以用两个指数函数的和很好地拟合(时间常数分别为0.35±0.09和3.2±0.4 s,n = 5)。持续刺激后的EPSC恢复甚至更慢。我们提出CF突触处的突触前抑制反映了每个量子递质释放后释放概率的缓慢恢复。6. CF突触处大量的功能释放位点、相对较大的量子大小以及递质释放的异常动力学似乎专门用于确保低频时橄榄小脑传递的高度可靠性,但限制高频时的传递。

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