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在一类感觉神经元中,神经损伤诱导的GABAA受体介导电导增强。

Enhancement of GABAA receptor-mediated conductances induced by nerve injury in a subclass of sensory neurons.

作者信息

Oyelese A A, Eng D L, Richerson G B, Kocsis J D

机构信息

Department of Neurology, Yale University School of Medicine, New Haven, Connecticut 06510, USA.

出版信息

J Neurophysiol. 1995 Aug;74(2):673-83. doi: 10.1152/jn.1995.74.2.673.

Abstract
  1. The effects of axotomy on the electrophysiologic properties of adult rat dorsal root ganglion (DRG) neurons were studied to understand the changes in excitability induced by traumatic nerve injury. Nerve injury was induced in vivo by sciatic nerve ligation with distal nerve transection. Two to four weeks after nerve ligation, a time when a neuroma forms, lumbar (L4 and L5) DRG neurons were removed and placed in short-term tissue culture. Whole cell patch-clamp recordings were made 5-24 h after plating. 2. DRG neurons were grouped into large (43-65 microns)-, medium (34-42 microns)-, and small (20-32 microns)- sized classes. Large neurons had short duration action potentials with approximately 60% having inflections on the falling phase of their action potentials. In contrast, action potentials of medium and small neurons were longer in duration and approximately 68% had inflections. 3. Pressure microejection of gamma-aminobutyric acid (GABA, 100 microM) or muscimol (100 microM) onto voltage-clamped DRG neurons elicited a rapidly desensitizing inward current that was blocked by 200 microM bicuculline. To measure the peak conductance induced by GABA or muscimol, neurons were voltage-clamped at a holding potential of -60 mV, and pulses to -80 mV and -100 mV were applied at a rate of 2.5 or 5 Hz during drug application. Slope conductances were calculated from plots of whole cell current measured at each of these potentials. 4. GABA-induced currents and conductances of control DRG neurons increased progressively with cell diameter. The mean GABA conductance was 36 +/- 10 nS (mean +/- SE) in small neurons, 124 +/- 21 nS in medium neurons, and 527 +/- 65 nS in large neurons. 5. After axotomy, medium neurons had significantly larger GABA-induced conductances compared with medium control neurons (390 +/- 50 vs. 124 +/- 21; P < 0.001). The increase in GABA conductance of medium neurons was associated with a decrease in duration of action potentials. In contrast, small neurons had no change in GABA conductance or action potential duration after ligation. The GABA conductance of large control neurons was highly variable, and ligation resulted in an increase that was significant only for neurons > 50 microns. The mean action potential duration in large neurons was not significantly changed, but neurons with inflections on the falling phase of the action potential were less common after ligation. There was no difference in resting potential or input resistance between control and ligated groups, except that the resting potential was less negative in small cells after axotomy.(ABSTRACT TRUNCATED AT 400 WORDS)
摘要
  1. 为了解创伤性神经损伤引起的兴奋性变化,研究了轴突切断对成年大鼠背根神经节(DRG)神经元电生理特性的影响。通过坐骨神经结扎并切断远端神经在体内诱导神经损伤。神经结扎后2至4周,即神经瘤形成时,取出腰段(L4和L5)DRG神经元并进行短期组织培养。接种后5 - 24小时进行全细胞膜片钳记录。2. DRG神经元分为大(43 - 65微米)、中(34 - 42微米)、小(20 - 32微米)三种大小类型。大神经元的动作电位持续时间短,约60%的动作电位在下降相有转折。相比之下,中和小神经元的动作电位持续时间更长,约68%有转折。3. 向电压钳制的DRG神经元微量注射γ-氨基丁酸(GABA,100微摩尔)或蝇蕈醇(100微摩尔)可引发快速脱敏的内向电流,该电流可被200微摩尔荷包牡丹碱阻断。为测量GABA或蝇蕈醇诱导的峰值电导,将神经元钳制在-60毫伏的保持电位,在施加药物期间以2.5或5赫兹的频率施加到-80毫伏和-100毫伏的脉冲。根据在这些电位下测量的全细胞电流图计算斜率电导。4. 对照DRG神经元的GABA诱导电流和电导随细胞直径逐渐增加。小神经元的平均GABA电导为36±10纳西门子(平均值±标准误),中神经元为124±21纳西门子,大神经元为527±65纳西门子。5. 轴突切断后,中神经元的GABA诱导电导比对照中神经元显著增大(390±50对124±21;P<0.001)。中神经元GABA电导的增加与动作电位持续时间的缩短相关。相比之下,小神经元在结扎后GABA电导和动作电位持续时间无变化。大对照神经元的GABA电导变化很大,结扎仅导致直径>50微米的神经元GABA电导显著增加。大神经元的平均动作电位持续时间无显著变化,但结扎后动作电位下降相有转折的神经元较少见。对照和结扎组之间的静息电位或输入电阻无差异,只是轴突切断后小细胞的静息电位负性减弱。(摘要截断于400字)
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b596/2605359/38d4e8c3b07d/nihms-80510-f0001.jpg

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