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细胞外pH对西帕曲明和拉莫三嗪与大鼠皮层解离神经元中高电压激活(HVA)钙通道相互作用的影响。

Effects of extracellular pH on the interaction of sipatrigine and lamotrigine with high-voltage-activated (HVA) calcium channels in dissociated neurones of rat cortex.

作者信息

Hainsworth A H, Spadoni F, Lavaroni F, Bernardi G, Stefani A

机构信息

Section of Pharmacology, School of Pharmacy, De Montfort University, Leicester LE1 9BH, UK.

出版信息

Neuropharmacology. 2001 May;40(6):784-91. doi: 10.1016/s0028-3908(01)00004-1.

Abstract

Acidic extracellular pH reduced high-voltage-activated (HVA) currents in freshly isolated cortical pyramidal neurones of adult rats, shifting activation to more positive voltages (V(1/2)=-18 mV at pH 7.4, -11 mV at pH 6.4). Sipatrigine inhibited HVA currents, with decreasing potency at acidic pH (IC(50) 8 microM at pH 7.4, 19 microM at pH 6.4) but the degree of maximal inhibition was >80% in all cases (pH 6.4-8.0). Sipatrigine has two basic groups (pK(A) values 4.2, 7.7) and at pH 7.4 is 68% in monovalent cationic form and 32% uncharged. From simple binding theory, the pH dependence of sipatrigine inhibition indicates a protonated group with pK(A) 6.6. Sipatrigine (50 microM) shifted the voltage dependence of channel activation at pH 7.4 (-7.6 mV shift) but not at pH 6.4. Lamotrigine has one basic site (pK(A) 5.5) and inhibited 34% of the HVA current, with similar potency over the pH range 6.4--7.4 (IC(50) 7.5--9 microM). These data suggest that the sipatrigine binding site on HVA calcium channels binds both cationic and neutral forms of sipatrigine, interacts with a group with pK(A)=6.6 and with the channel activation process, and differs from that for lamotrigine.

摘要

酸性细胞外pH值降低了成年大鼠新鲜分离的皮质锥体神经元中的高电压激活(HVA)电流,使激活向更正的电压偏移(pH 7.4时V(1/2)= -18 mV,pH 6.4时为-11 mV)。西帕曲明抑制HVA电流,在酸性pH下效力降低(pH 7.4时IC(50)为8 μM,pH 6.4时为19 μM),但在所有情况下(pH 6.4 - 8.0)最大抑制程度均>80%。西帕曲明有两个碱性基团(pK(A)值分别为4.2、7.7),在pH 7.4时68%为单价阳离子形式,32%不带电荷。根据简单的结合理论,西帕曲明抑制的pH依赖性表明存在一个pK(A)为6.6的质子化基团。西帕曲明(50 μM)在pH 7.4时改变了通道激活的电压依赖性(-7.6 mV的偏移),但在pH 6.4时未改变。拉莫三嗪有一个碱性位点(pK(A) 5.5),抑制了34%的HVA电流,在pH 6.4 - 7.4范围内效力相似(IC(50) 7.5 - 9 μM)。这些数据表明HVA钙通道上的西帕曲明结合位点既能结合西帕曲明的阳离子形式也能结合中性形式,与一个pK(A)=6.6的基团以及通道激活过程相互作用,且与拉莫三嗪的结合位点不同。

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