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γ-氨基丁酸(GABA)对加州海兔胆碱能突触的抑郁、易化和强直后增强的突触前调节作用。

Presynaptic modulating effects of GABA on depression, facilitation, and posttetanic potentiation of a cholinergic synapse in Aplysia californica.

作者信息

Tremblay J P, Plourde G

出版信息

Can J Physiol Pharmacol. 1977 Dec;55(6):1286-301. doi: 10.1139/y77-174.

Abstract

The effects of gamma-aminobutyric acid (GABA) have been studied on the synaptic depression, frequency facilitation, and posttetanic potentiation (PTP) of a unitary, monosynaptic, and presumably cholinergic excitatory postsynaptic potential (EPSP). This EPSP, produced by minimal stimulation of the right visceropleural connective, was recorded in cell R 15 of Aplysia californica. Perfusion with GABA (10(-4)-10(-3) M) reduces the size of all EPSPs produced by a train of 100 stimuli at 1/s. It also reduced the synaptic depression and PTP, and increases the frequency facilitation seen during the train. GABA does not significantly effect the membrane resistance (mean 102%) but it slightly depolarizes (mean 6 mV) the postsynaptic cell. GABA does not reduce an acetylcholine iontophoretic potential produced on R15. The effects of GABA are reduction when chloride is replaced by acetate but they remain significant. Picrotoxin and bicuculline fail to antagonize GABA. Addition of sodium azide or dinitrophenol does not reduce the action of GABA and even prolongs it. The effects of GABA are attributed to two sites of action: a postsynaptic one, responsible for the small change in potential and partially responsible for the reduction of EPSP size; and a presynaptic one, responsible for a further reduction of EPSP size and the changes of depression, facilitation, and PTP.

摘要

已经研究了γ-氨基丁酸(GABA)对单一、单突触且可能为胆碱能兴奋性突触后电位(EPSP)的突触抑制、频率易化和强直后增强(PTP)的影响。这种EPSP是通过对右侧内脏胸膜结缔组织进行最小刺激产生的,记录于加州海兔的R15细胞中。用GABA(10⁻⁴ - 10⁻³ M)灌注可减小由每秒1次的100次刺激序列产生的所有EPSP的大小。它还减少了突触抑制和PTP,并增强了刺激序列期间出现的频率易化。GABA对膜电阻没有显著影响(平均为102%),但它使突触后细胞轻微去极化(平均6 mV)。GABA不会降低在R15上通过离子电泳施加乙酰胆碱产生的电位。当氯离子被乙酸根取代时,GABA的作用减弱,但仍然显著。印防己毒素和荷包牡丹碱不能拮抗GABA。添加叠氮化钠或二硝基苯酚不会降低GABA的作用,甚至会延长其作用。GABA的作用归因于两个作用位点:一个是突触后位点,负责电位的微小变化并部分负责EPSP大小的减小;另一个是突触前位点,负责EPSP大小的进一步减小以及抑制、易化和PTP的变化。

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