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新型二氢吡啶衍生物FRC8653对兔基底动脉记录的Ba2+电流的双重作用。

Dual action of FRC8653, a novel dihydropyridine derivative, on the Ba2+ current recorded from the rabbit basilar artery.

作者信息

Oike M, Inoue Y, Kitamura K, Kuriyama H

机构信息

Department of Pharmacology, Faculty of Medicine, Kyushu University, Fukuoka, Japan.

出版信息

Circ Res. 1990 Oct;67(4):993-1006. doi: 10.1161/01.res.67.4.993.

Abstract

Actions of FRC8653 on the macroscopic and unitary Ba2+ currents were studied using the rabbit basilar artery. Application of (+/-)-FRC8653 (less than 1 microM) increased the amplitude of the inward current when depolarization pulses more negative than -10 mV were applied but inhibited it when depolarization was more positive than 0 mV (in each case from a holding potential of -80 mV). At a holding potential of -40 mV, (+/-)-FRC8653 (greater than 0.1 nM) consistently inhibited the inward current. (-)-FRC8653 (greater than 1 nM) inhibited the amplitude of the inward current evoked by a depolarizing pulse more positive than -10 mV (the holding potential being -80 mV). At the holding potential of -80 mV, but not at -40 mV, (+)-FRC8653 (1 microM) enhanced the current amplitude evoked by a depolarizing pulse more negative than -10 mV but inhibited the current evoked by a pulse more positive than 0 mV. (+/-)-FRC8653 shifted the voltage-dependent inhibition curves to the left, and the slope of the curve became steeper (test pulse of +10 mV). Two types of single Ca2+ channel currents (12 and 23 pS) were recorded from the basilar artery by the cell-attached patch-clamp method. Opening of the 12-pS channel occurred with a depolarizing pulse (-20 mV) from a holding potential of -80 mV, but not from one of -60 mV. (+)-FRC8653 activated, and (-)-FRC8653 inhibited, the 23-pS channel.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

使用兔基底动脉研究了FRC8653对宏观和单一Ba2 +电流的作用。施加(±)-FRC8653(小于1μM)时,当施加比 -10 mV更负的去极化脉冲时,内向电流幅度增加,但当去极化比0 mV更正时则抑制内向电流(在每种情况下,保持电位为 -80 mV)。在 -40 mV的保持电位下,(±)-FRC8653(大于0.1 nM)持续抑制内向电流。(-)-FRC8653(大于1 nM)抑制由比 -10 mV更正的去极化脉冲诱发的内向电流幅度(保持电位为 -80 mV)。在 -80 mV的保持电位下,但不在 -40 mV时,(+)-FRC8653(1μM)增强了由比 -10 mV更负的去极化脉冲诱发的电流幅度,但抑制了由比0 mV更正的脉冲诱发的电流。(±)-FRC8653将电压依赖性抑制曲线向左移动,并且曲线斜率变得更陡(测试脉冲为 +10 mV)。通过细胞贴附式膜片钳方法从基底动脉记录到两种类型的单Ca2 +通道电流(12和23 pS)。12-pS通道的开放发生在从 -80 mV的保持电位施加去极化脉冲(-20 mV)时,但不是从 -60 mV的保持电位。(+)-FRC8653激活,而(-)-FRC8653抑制23-pS通道。(摘要截断于250字)

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