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首页> 外文期刊>The Journal of Physiology >Inhibition of N- and P/Q-type calcium channels by postsynaptic GABAB receptor activation in rat supraoptic neurones.
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Inhibition of N- and P/Q-type calcium channels by postsynaptic GABAB receptor activation in rat supraoptic neurones.

机译:大鼠超视神经元中突触后GABA B受体激活对N和P / Q型钙通道的抑制作用。

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1. Voltage-dependent Ca2+ currents of dissociated rat supraoptic nucleus (SON) neurones were measured using the whole-cell configuration of the patch-clamp technique to examine direct postsynaptic effects of GABAB receptor activation on SON magnocellular neurones. 2. The selective GABAB agonist baclofen reversibly inhibited voltage-dependent Ca2+ currents elicited by voltage steps from a holding potential of -80 mV to depolarized potentials in a dose-dependent manner. The ED50 of baclofen for inhibiting Ca2+ currents was 1.4 x 10-6 M. Baclofen did not inhibit low threshold Ca2+ currents elicited by voltage steps from -120 to -40 mV. 3. Inhibition of high threshold Ca2+ currents by baclofen was rapidly and completely reversed by the selective GABAB antagonists, CGP 35348 and CGP 55845A, when the antagonists were added at the molar ratio vs. baclofen of 10 : 1 and 0.01 : 1, respectively. It was also reversed by a prepulse to +150 mV lasting for 100 ms. 4. The inhibition of Ca2+ currents was abolished when the cells were pretreated with pertussis toxin for longer than 20 h or with N-ethylmaleimide for 2 min. It was also abolished when GDPbetaS was included in the patch pipette. When GTPgammaS was included in the patch pipette, baclofen produced irreversible inhibition of Ca2+ currents and this inhibition was again reversed by the prepulse procedure. 5. The inhibition of N-, P/Q-, L- and R-type Ca2+ channels by baclofen (10-5 M) was 24.1, 10.5, 3.1 and 3. 6 %, respectively, of the total Ca2+ currents. Only the inhibition of N- and P/Q-types was significant. 6. These results suggest that GABAB receptors exist in the postsynaptic sites of the SON magnocellular neurones and mediate selective inhibitory actions on voltage-dependent Ca2+ channels of N- and P/Q-types via pertussis toxin-sensitive G proteins, and that such inhibitory mechanisms may play a role in the regulation of SON neurones by the GABA neurones.
机译:1.使用膜片钳技术的全细胞配置测量离解的大鼠视上核(SON)神经元的电压依赖性Ca2 +电流,以检查GABAB受体激活对SON巨细胞神经元的直接突触后影响。 2.选择性GABA B激动剂巴氯芬以剂量依赖性方式可逆地抑制电压阶跃引起的电压依赖性Ca 2+电流,该电压阶跃从-80 mV的保持电势到去极化电势。巴氯芬抑制Ca2 +电流的ED50为1.4 x 10-6M。巴氯芬不抑制从-120至-40 mV的电压阶跃引起的低阈值Ca2 +电流。 3.当分别以相对于巴氯芬的摩尔比为10:1和0.01:1加入拮抗剂时,选择性GABAB拮抗剂CGP 35348和CGP 55845A迅速并完全逆转了巴氯芬对高阈值Ca2 +电流的抑制作用。还可以通过预脉冲将其反转至+150 mV,持续100 ms。 4.当用百日咳毒素预处理细胞超过20小时或用N-乙基马来酰亚胺预处理2分钟时,对Ca2 +电流的抑制作用就消失了。当贴片移液器中包含GDPbetaS时,它也被取消。当贴片移液器中包含GTPgammaS时,巴氯芬对Ca2 +电流产生不可逆的抑制作用,并且该抑制作用可通过预脉冲程序再次消除。 5.巴氯芬(10-5 M)对N型,P / Q型,L型和R型Ca2 +通道的抑制分别为总Ca2 +电流的24.1%,10.5%,3.1%和3.6%。仅对N和P / Q型的抑制是显着的。 6.这些结果表明,GABAB受体存在于SON巨细胞神经元的突触后位点,并通过百日咳毒素敏感的G蛋白介导N和P / Q型电压依赖性Ca2 +通道的选择性抑制作用,并且这种抑制作用机制可能在GABA神经元对SON神经元的调节中起作用。

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