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培养的小鼠脊髓神经元单个γ-氨基丁酸A型(GABAA)受体通道的苯二氮䓬类和β-咔啉调节作用

Benzodiazepine and beta-carboline regulation of single GABAA receptor channels of mouse spinal neurones in culture.

作者信息

Rogers C J, Twyman R E, Macdonald R L

机构信息

Department of Neurology, University of Michigan Medical Center, Ann Arbor 48104-1687.

出版信息

J Physiol. 1994 Feb 15;475(1):69-82. doi: 10.1113/jphysiol.1994.sp020050.

Abstract
  1. The effects of the benzodiazepine receptor agonist, diazepam (DZ), and the inverse agonist, methyl-6,7-dimethoxy-4-ethyl-beta-carboline-3-carboxylate (DMCM), on gamma-aminobutyric acid (GABAA) receptor single channel currents were characterized. Outside-out patches were obtained from somata of cultured mouse spinal cord neurones and voltage clamped at -75 mV (ECl = 0 mV). 2. GABA (2 microM) alone or with DZ (20-1000 nM) or DMCM (20-100 nM) was applied to patches by pressure ejection from blunt micropipettes. DZ enhanced GABAA receptor currents with an inverted U-shaped concentration-response curve. Mean steady-state currents were increased by low concentrations of DZ (20-50 nM). At higher concentrations of DZ, the enhancement was diminished. Mean steady-state currents were decreased by DMCM at all concentrations. 3. GABAA receptor channels opened most frequently to a 27 pS main conductance level and less frequently to a 19 pS subconductance level. Neither DZ nor DMCM altered the proportion of time spent at either of the conductance levels. The kinetic properties of the main conductance level were studied. 4. Neither DZ nor DMCM altered the mean GABAA receptor channel open or burst durations. Sums of three exponential functions were required to fit best open and burst duration-frequency histograms for GABA alone or with DZ or DMCM. No significant changes in the three time constants or areas of the three exponential functions for open or burst duration histograms were produced by DZ or DMCM. 5. With increasing concentrations of DZ up to 50 nM, GABA evoked an increased frequency of channel openings and bursts. With higher DZ concentrations, the magnitudes of the increase in channel opening and burst frequencies were reduced. At all concentrations of DMCM, GABA evoked a decreased frequency of channel openings and bursts. 6. Closed duration-frequency histograms for GABA alone or with DZ or DMCM were best fitted by sums of at least six exponential functions. The three shortest closed duration time constants were unchanged by DZ or DMCM. The three longest closed duration time constants were altered by DZ and DMCM, consistent with alterations in opening frequency. 7. DZ increased and DMCM decreased steady-state GABAA receptor current by increasing or decreasing channel opening frequency without altering mean channel open duration. We propose that DZ and DMCM alter GABAA receptor current by acting reciprocally to increase or decrease only, respectively, the apparent agonist association rate at the first of two proposed GABA binding steps without altering channel gating.(ABSTRACT TRUNCATED AT 400 WORDS)
摘要
  1. 研究了苯二氮䓬受体激动剂地西泮(DZ)和反向激动剂甲基 - 6,7 - 二甲氧基 - 4 - 乙基 - β - 咔啉 - 3 - 羧酸酯(DMCM)对γ - 氨基丁酸(GABAA)受体单通道电流的影响。从培养的小鼠脊髓神经元胞体获取外向型膜片,并将膜片钳制在 - 75 mV(氯离子平衡电位ECl = 0 mV)。2. 通过钝头微管压力喷射将单独的GABA(2 μM)或与DZ(20 - 1000 nM)或DMCM(20 - 100 nM)一起施加到膜片上。DZ增强GABAA受体电流,呈现倒U形浓度 - 反应曲线。低浓度的DZ(20 - 50 nM)可增加平均稳态电流。在较高浓度的DZ时,增强作用减弱。在所有浓度下,DMCM均降低平均稳态电流。3. GABAA受体通道最常开放至27 pS的主电导水平,较少开放至19 pS的次电导水平。DZ和DMCM均未改变在任一电导水平所花费时间的比例。研究了主电导水平的动力学特性。4. DZ和DMCM均未改变GABAA受体通道的平均开放或爆发持续时间。单独的GABA或与DZ或DMCM一起时,需要三个指数函数的总和来最佳拟合开放和爆发持续时间 - 频率直方图。DZ或DMCM未使开放或爆发持续时间直方图的三个时间常数或三个指数函数的面积产生显著变化。5. 随着DZ浓度增加至50 nM,GABA诱发通道开放和爆发的频率增加。在更高的DZ浓度下,通道开放和爆发频率增加的幅度减小。在所有DMCM浓度下,GABA诱发通道开放和爆发的频率降低。6. 单独的GABA或与DZ或DMCM一起时的关闭持续时间 - 频率直方图最好用至少六个指数函数的总和来拟合。DZ或DMCM未改变三个最短关闭持续时间时间常数。DZ和DMCM改变了三个最长关闭持续时间时间常数,这与开放频率的改变一致。7. DZ通过增加通道开放频率而增加稳态GABAA受体电流,DMCM通过降低通道开放频率而降低稳态GABAA受体电流,且两者均未改变平均通道开放持续时间。我们提出,DZ和DMCM通过分别仅增加或降低在两个假定的GABA结合步骤中的第一个步骤的表观激动剂结合速率来相互作用地改变GABAA受体电流,而不改变通道门控。(摘要截短至400字)

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