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Inhibition of spontaneous EPSCs and IPSCs by presynaptic GABAB receptors on rat supraoptic magnocellular neurons.

机译:突触前GABA B受体对大鼠视上巨细胞神经元的自发性EPSC和IPSC的抑制作用。

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1. The function of presynaptic GABA receptors in the regulation of transmitter release in supraoptic nucleus (SON) magnocellular neurons was investigated by recording spontaneous postsynaptic currents from rat magnocellular SON neurons in a slice preparation (150 microns thick, 1.8 mm in diameter) using the whole-cell patch-clamp technique. 2. Both the spontaneous EPSCs and IPSCs were TTX resistant. The EPSCs were abolished by 6-cyano-7-nitroquinoxaline-2,3-dione (CNQX), whereas the IPSCs were abolished by picrotoxin, suggesting that the EPSCs and IPSCs are synaptic inputs from glutamatergic and GABAergic neurons, respectively. 3. The selective GABAB agonist, baclofen, reduced the frequency of both the EPSCs and IPSCs without affecting the amplitude. The time constant of the decay phase of both the EPSCs and IPSCs remained unchanged after baclofen application. 4. The reduction of the frequency of the synaptic currents by baclofen was dose dependent (10 nM to 100 microM) and the EC50 values were 5.8 and 8.5 microM for the EPSCs and IPSCs, respectively. 5. The effect of baclofen (10 microM) was antagonized by the selective GABAB antagonist, 2-hydroxy-saclofen (2OH-saclofen), at 300 microM. 6. When given alone, 2OH-saclofen (100 microM) increased the frequency of both the EPSCs and IPSCs without affecting their amplitude, suggesting that endogenously released GABA in the slice acts on presynaptic GABAB receptors. 7. The GABAA agonist, muscimol, reduced the frequency of EPSCs, and picrotoxin increased the frequency of the EPSCs, suggesting that GABAA receptors also participate in the presynaptic inhibition of glutamate release. 8. Taken together, these data suggest that GABAB receptors are present on the presynaptic terminals of both GABA and glutamate neurons in the SON, and that these presynaptic GABAB receptors play an important role in the regulation of the neuronal activity in SON magnocellular neurons.
机译:1.通过记录切片制备(150微米厚,直径1.8毫米)中大鼠大细胞SON神经元的自发突触后电流,来研究突触前GABA受体在视上核(SON)神经元神经元中递质释放调节中的功能。全细胞膜片钳技术。 2.自发EPSC和IPSC均具有抗TTX的能力。 EPSC被6-氰基-7-硝基喹喔啉-2,3-二酮(CNQX)废除了,而IPSC被微毒素废除了,这表明EPSC和IPSC分别是来自谷氨酸能和GABA能神经元的突触输入。 3.选择性GABAB激动剂巴氯芬可降低EPSC和IPSC的频率,而不会影响振幅。施用巴氯芬后,EPSC和IPSC的衰减相的时间常数保持不变。 4.巴氯芬对突触电流频率的降低是剂量依赖性的(10 nM至100 microM),EPSC和IPSC的EC50值分别为5.8和8.5 microM。 5.选择性GABAB拮抗剂2-hydroxy-saclofen(2OH-saclofen)以300 microM拮抗巴氯芬(10 microM)的作用。 6.当单独给予时,2OH-沙氯芬(100 microM)会增加EPSC和IPSC的频率,而不会影响它们的振幅,表明切片中内源释放的GABA作用于突触前GABA B受体。 7. GABAA激动剂麝香酚降低了EPSC的频率,微毒素增加了EPSC的频率,这表明GABAA受体也参与了谷氨酸释放的突触前抑制。 8.综上所述,这些数据表明GABAB受体同时存在于SON中的GABA和谷氨酸神经元的突触前末端,并且这些突触前GABAB受体在SON巨细胞神经元的神经元活性的调节中起着重要作用。

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