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海马锥体细胞突触后去极化GABA反应的离子基础。

Ionic basis of the postsynaptic depolarizing GABA response in hippocampal pyramidal cells.

作者信息

Perkins K L, Wong R K

机构信息

Department of Pharmacology, State University of New York Health Science Center, Brooklyn 11203, USA.

出版信息

J Neurophysiol. 1996 Dec;76(6):3886-94. doi: 10.1152/jn.1996.76.6.3886.

Abstract
  1. Whole cell voltage-clamp recording with recording pipette solutions of differing ionic composition was used to determine the ionic basis of the depolarizing gamma-aminobutyric acid (GABA) response. In the presence of 4-aminopyridine and excitatory amino acid receptor blockers, giant GABA-mediated postsynaptic currents (GPSCs) were recorded from CA3 pyramidal neurons in hippocampal slices from adult guinea pigs. With the GABAB component blocked, the GPSC was composed of an initial outward current (GABAA component) that peaked at 115 ms followed by a late inward current (GABAD component) that peaked at 400-600 ms. 2. Reduction of the intracellular concentration of potassium ([K+]i)resulted in no significant change in the reversal potential of the GABAD component of the GPSC, indicating that it is not a nonspecific cation current. 3. The HCO3- permeability of the channel mediating the GABAD response was assessed by using recording pipette solutions containing three different concentrations of bicarbonate ([HCO3-], 19, 49, and 102 mM). The reversal potential of the GABAD response shifted in the depolarizing direction as the HCO3- equilibrium potential was shifted in the depolarizing direction, indicating that the channel mediating the GABAD response is permeable to HCO3-. The reversal potential of the GABAD response was more sensitive to changes in recording pipette [HCO3-] than the reversal potential of the GABAA response, indicating that the GABAD response is carried by HCO3- to a greater extent than the GABAA response. 4. The outward current-inward current sequence of the biphasic GPSC was reversed to an inward current-outward current sequence by using a high [Cl-]/low [HCO3-] recording pipette solution (40 mM Cl-/6 mM HCO3-), indicating that the GABAA component is more sensitive to changes in [Cl-]i, and the GABAD component is more sensitive to changes in [HCO3-]i. 5. These data indicate that the GABAD component of the GPSC is predominantly carried by HCO3-. While this result supports the recently propsed chloride accumulation model, the model in its present form cannot explain the inward current-outward current polarity sequence of the GPSC recorded with the high [Cl-]/low [HCO3-] intracellular solution. The data obtained using that solution reveal the need for a more expansive chloride accumulation/ depletion model or for a model utilizing two distinct ionotropic GABA channels with different anion permeability ratios to account for the biphasic nature of the GPSC.
摘要
  1. 采用全细胞电压钳记录技术,使用具有不同离子组成的记录电极溶液,以确定去极化γ-氨基丁酸(GABA)反应的离子基础。在4-氨基吡啶和兴奋性氨基酸受体阻滞剂存在的情况下,从成年豚鼠海马切片的CA3锥体神经元记录到巨大的GABA介导的突触后电流(GPSCs)。在GABAB成分被阻断的情况下,GPSC由一个初始外向电流(GABAA成分)组成,该电流在115毫秒时达到峰值,随后是一个晚期内向电流(GABAD成分),在400 - 600毫秒时达到峰值。2. 降低细胞内钾离子浓度([K⁺]i)导致GPSC的GABAD成分的反转电位没有显著变化,表明它不是非特异性阳离子电流。3. 通过使用含有三种不同浓度碳酸氢盐([HCO₃⁻],19、49和102 mM)的记录电极溶液,评估介导GABAD反应的通道的HCO₃⁻通透性。随着HCO₃⁻平衡电位向去极化方向移动,GABAD反应的反转电位也向去极化方向移动,表明介导GABAD反应的通道对HCO₃⁻具有通透性。GABAD反应的反转电位比GABAA反应的反转电位对记录电极[HCO₃⁻]的变化更敏感,表明GABAD反应比GABAA反应在更大程度上由HCO₃⁻携带。4. 通过使用高[Cl⁻]/低[HCO₃⁻]记录电极溶液(40 mM Cl⁻/6 mM HCO₃⁻),双相GPSC的外向电流-内向电流顺序被反转成内向电流-外向电流顺序,表明GABAA成分对[Cl⁻]i的变化更敏感,而GABAD成分对[HCO₃⁻]i的变化更敏感。5. 这些数据表明,GPSC的GABAD成分主要由HCO₃⁻携带。虽然这一结果支持了最近提出的氯离子积累模型,但该模型的现有形式无法解释用高[Cl⁻]/低[HCO₃⁻]细胞内溶液记录的GPSC的内向电流-外向电流极性顺序。使用该溶液获得的数据表明,需要一个更扩展的氯离子积累/消耗模型,或者一个利用两个具有不同阴离子通透性比的不同离子型GABA通道的模型来解释GPSC的双相性质。

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