大鼠海马体中两种GABAA介导的抑制性突触后电流的使用依赖性抑制的不同机制。
Different mechanisms for use-dependent depression of two GABAA-mediated IPSCs in rat hippocampus.
作者信息
Pearce R A, Grunder S D, Faucher L D
机构信息
Department of Anesthesiology, University of Wisconsin School of Medicine, Madison, USA.
出版信息
J Physiol. 1995 Apr 15;484 ( Pt 2)(Pt 2):425-35. doi: 10.1113/jphysiol.1995.sp020675.
Abstract
- The mechanisms involved in the use-dependent depression of GABAA,fast and GABAA,slow, two GABAA-mediated IPSCs in the rat hippocampal slice preparation, were investigated by observing the effects of paired-pulse depression and of baclofen and CGP 35348 on monosynaptic inhibitory currents recorded from CA1 pyramidal neurons. 2. The second of a pair of evoked responses that consisted of both inhibitory components was depressed and decayed more rapidly compared to the first at an interpulse interval (IpI) of 200 ms. This effect was due to a decrease in the amplitude of GABAA,slow, with no effect on the time constant of decay or on the amplitude or time constant of GABAA,fast. 3. The time course of paired-pulse depression of both components at IpIs ranging from 5 to 2560 ms was compared. GABAA,slow was depressed maximally by 55% at IpIs of 80-160 ms. GABAA,fast was depressed maximally by 38% at 5 ms, and recovered exponentially with a time constant of 130 ms. 4. GABAA,slow was more sensitive than GABAA,fast to depression by baclofen. GABAA,slow was susceptible to complete block, with an ED50 of approximately 200 nM for (+/-)-baclofen and 100 nM for the active enantiomer, (R)-(+)-baclofen. GABAA,fast was blocked by only 50% by the highest concentrations of baclofen tested (10-100 microM (R)-(+)-baclofen), with an ED50 of approximately 2 microM for (+/-)-baclofen and 1 microM for (R)-(+)-baclofen. Paired-pulse depression of GABAA,fast was not occluded by 10 or 100 microM (R)-(+)-baclofen. 5. The GABAB antagonist CGP 35348 (0.4-1 mM), prevented paired-pulse depression of GABAA,slow at IpIs of 160 to 200 ms, and reversed the depression of GABAA,fast by baclofen, but had no effect on paired-pulse depression of GABAA,fast at IpIs of 20 to 40 ms. 6. It is concluded that use-dependent depression of GABAA,slow, but not GABAA,fast, is mediated by a presynaptic GABAB receptor. It is speculated that use-dependent depression of GABAA,fast, which occurs only over a much faster time scale, may be due to rapid postsynaptic GABAA receptor desensitization.
摘要
- 通过观察配对脉冲抑制以及巴氯芬和CGP 35348对从大鼠海马脑片制备中CA1锥体神经元记录的单突触抑制电流的影响,研究了参与大鼠海马脑片制备中GABAA快速型和GABAA慢速型这两种GABAA介导的抑制性突触后电流(IPSCs)的使用依赖性抑制的机制。2. 一对由两个抑制成分组成的诱发反应中的第二个,在200毫秒的脉冲间隔(IpI)下,与第一个相比,被抑制且衰减更快。这种效应是由于GABAA慢速型的幅度减小,而对衰减时间常数或GABAA快速型的幅度和时间常数没有影响。3. 比较了在5至2560毫秒的IpI范围内两种成分的配对脉冲抑制的时间进程。GABAA慢速型在80 - 160毫秒的IpI时最大被抑制55%。GABAA快速型在5毫秒时最大被抑制38%,并以130毫秒的时间常数呈指数恢复。4. GABAA慢速型比GABAA快速型对巴氯芬的抑制更敏感。GABAA慢速型易被完全阻断,(±)-巴氯芬的半数有效剂量(ED50)约为200纳摩尔,活性对映体(R)-(+)-巴氯芬的ED50为100纳摩尔。测试最高浓度的巴氯芬(10 - 100微摩尔(R)-(+)-巴氯芬)仅使GABAA快速型被阻断50%,(±)-巴氯芬的ED50约为2微摩尔,(R)-(+)-巴氯芬的ED50为1微摩尔。10或100微摩尔(R)-(+)-巴氯芬不会使GABAA快速型的配对脉冲抑制发生重叠。5. GABAB拮抗剂CGP 35348(0.4 - 1毫摩尔)可防止在160至200毫秒的IpI时GABAA慢速型的配对脉冲抑制,并逆转巴氯芬对GABAA快速型的抑制,但对20至40毫秒的IpI时GABAA快速型的配对脉冲抑制没有影响。6. 得出结论,GABAA慢速型而非GABAA快速型的使用依赖性抑制是由突触前GABAB受体介导的。推测仅在快得多的时间尺度上发生的GABAA快速型的使用依赖性抑制可能是由于突触后GABAA受体的快速脱敏。
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