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大鼠海马切片中CA1中间神经元亚型诱发的膜特性和突触电流。

Membrane properties and synaptic currents evoked in CA1 interneuron subtypes in rat hippocampal slices.

作者信息

Morin F, Beaulieu C, Lacaille J C

机构信息

Centre de Recherche en Sciences Neurologiques, Université de Montréal, Quebec, Canada.

出版信息

J Neurophysiol. 1996 Jul;76(1):1-16. doi: 10.1152/jn.1996.76.1.1.

Abstract
  1. Intrinsic membrane properties and pharmacologically isolated excitatory and inhibitory postsynaptic currents (EPSCs and IPSCs, respectively) were characterized with the use of whole cell current- and voltage-clamp recordings, in combination with biocytin labeling, in different subtypes of CA1 interneurons and pyramidal cells in rat hippocampal slices. 2. Three classes of interneurons were selected on the basis of their soma location in the CA1 region: 1) in stratum (str.) oriens near the alveus (O/A), 2) near str. pyramidale, and 3) near the border of str. radiatum and lacunosum-moleculare. Each class of biocytin-labeled cells demonstrated specific cellular morphology. The somata of all interneurons were nonpyramidal in shape and usually multipolar. However, the pattern of dendritic and axonal arborizations of labeled interneurons differed in each class. 3. In current-clamp recordings, all interneuron subtypes had shorter-duration and smaller-amplitude action potentials than pyramidal cells. Fast- and medium-duration afterhyperpolarizations were larger in amplitude in interneurons. Cell input resistance was greater and membrane time constant was faster in all interneuron subtypes than in pyramidal cells. 4. Depolarizing current pulses evoked regular firing in all classes of interneurons, whereas burst firing was observed in 50% of pyramidal cells. With hyperpolarizing current pulses, all nonpyramidal and pyramidal cell types displayed inward rectification followed by anodal break excitation. 5. Electrical stimulation of nearby afferents evoked excitatory postsynaptic potentials (EPSPs) in all cells. EPSPs were of short duration and usually followed by inhibitory postsynaptic potentials (IPSPs). EPSPs were mediated by glutamate, because they were blocked by non-N-methyl-D-aspartate (non-NMDA) and NMDA antagonists [6-cyano-7-nitroquinoxaline-2,3-dione (CNQX) and (+/-)-2-amino-5-phosphonopentanoic acid (AP5), respectively]. In the presence of these antagonists, IPSPs were evoked in isolation and reversed near -72 mV. 6. In voltage-clamp recordings, non-NMDA EPSCs were isolated pharmacologically in the presence of AP5 and the gamma-aminobutyric acid-A (GABAA) antagonist bicuculline (BIC). Their properties were similar in all interneuron subtypes and pyramidal cells. Current-voltage (I-V) relations were linear, and mean reversal potentials were near 5 mV. Non-NMDA EPSCs were reversibly antagonized by CNQX. 7. NMDA EPSCs were pharmacologically isolated during CNQX and BIC application and were observed in all cell types. I-V relations of NMDA EPSCs demonstrated a region of negative slope at membrane potentials between -80 and -20 mV and their reversal potential was near 7 mV. The rise time of NMDA EPSCs was significantly slower in O/A interneurons than in other cell types. NMDA EPSCs were reversibly antagonized by AP5. 8. GABAA IPSCs were pharmacologically isolated in AP5 and CNQX and their properties were similar in all cell types. I-V relations of GABAA IPSCs were linear with mean reversal potentials near -32 mV. GABAA IPSCs were reversibly blocked by BIC. 9. In conclusion, morphologically different subtypes of interneurons located in O/A, near str. pyramidale, and near the str. radiatum/lacunosum-moleculare border displayed intrinsic membrane properties that were distinct from pyramidal cells, but were similar among them. In contrast, the properties of non-NMDA, NMDA, and GABAA postsynaptic currents were similar between interneurons and pyramidal cells, except for NMDA EPSCs, which had slower rise times in O/A interneurons.
摘要
  1. 运用全细胞电流钳和电压钳记录技术,并结合生物胞素标记,对大鼠海马脑片CA1区不同亚型的中间神经元和锥体细胞的内在膜特性以及药理学分离的兴奋性和抑制性突触后电流(分别为EPSC和IPSC)进行了表征。2. 根据其在CA1区的胞体位置,选择了三类中间神经元:1)在靠近脑室的原层(str.)或iens(O/A),2)靠近锥体层,3)靠近辐射层和分子层的边界。每一类生物胞素标记的细胞都表现出特定的细胞形态。所有中间神经元的胞体形状均为非锥体状,通常为多极。然而,每一类中标记中间神经元的树突和轴突分支模式各不相同。3. 在电流钳记录中,所有中间神经元亚型的动作电位持续时间较短且幅度较小,相比锥体细胞而言。快速和中等持续时间的超极化后电位在中间神经元中的幅度更大。所有中间神经元亚型的细胞输入电阻更大,膜时间常数更快,相比锥体细胞而言。4. 去极化电流脉冲在所有类别的中间神经元中诱发规则放电,而在50%的锥体细胞中观察到爆发性放电。施加超极化电流脉冲时,所有非锥体和锥体细胞类型均表现出内向整流,随后是阳极断裂兴奋。5. 对附近传入神经的电刺激在所有细胞中诱发兴奋性突触后电位(EPSP)。EPSP持续时间较短,通常随后是抑制性突触后电位(IPSP)。EPSP由谷氨酸介导,因为它们分别被非N-甲基-D-天冬氨酸(非NMDA)和NMDA拮抗剂[6-氰基-7-硝基喹喔啉-2,3-二酮(CNQX)和(±)-2-氨基-5-膦酰戊酸(AP5)]阻断。在这些拮抗剂存在的情况下,可单独诱发IPSP,其反转电位接近-72 mV。6. 在电压钳记录中,在AP5和γ-氨基丁酸-A(GABAA)拮抗剂荷包牡丹碱(BIC)存在的情况下,药理学分离出非NMDA EPSC。它们在所有中间神经元亚型和锥体细胞中的特性相似。电流-电压(I-V)关系呈线性,平均反转电位接近5 mV。非NMDA EPSC被CNQX可逆性拮抗。7. 在应用CNQX和BIC期间药理学分离出NMDA EPSC,并在所有细胞类型中观察到。NMDA EPSC的I-V关系在膜电位-80至-20 mV之间显示出负斜率区域,其反转电位接近7 mV。O/A中间神经元中NMDA EPSC的上升时间明显慢于其他细胞类型。NMDA EPSC被AP5可逆性拮抗。8. GABAA IPSC在AP5和CNQX中被药理学分离,其特性在所有细胞类型中相似。GABAA IPSC的I-V关系呈线性,平均反转电位接近-32 mV。GABAA IPSC被BIC可逆性阻断。9. 总之,位于O/A、靠近锥体层和靠近辐射层/分子层边界的形态不同的中间神经元亚型表现出与锥体细胞不同的内在膜特性,但它们之间相似。相比之下,中间神经元和锥体细胞之间非NMDA、NMDA和GABAA突触后电流的特性相似,除了O/A中间神经元中的NMDA EPSC上升时间较慢。

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