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尼莫地平以年龄和浓度依赖性方式降低兔海马CA1神经元中的钙动作电位。

Nimodipine decreases calcium action potentials in rabbit hippocampal CA1 neurons in an age-dependent and concentration-dependent manner.

作者信息

Moyer J R, Disterhoft J F

机构信息

Department of Cell, Molecular, and Structural Biology, Northwestern University Medical School, Chicago, Illinois 60611-3008.

出版信息

Hippocampus. 1994 Feb;4(1):11-7. doi: 10.1002/hipo.450040104.

Abstract

Intracellular recordings were made from rabbit hippocampal CA1 neurons in vitro using slices from aging and young adult rabbits. Calcium action potentials were studied in the presence of 4 microns tetrodotoxin using electrodes filled with 2M CsCl. Increasing concentrations of the dihydropyridine L-type calcium channel antagonist nimodipine were tested on the amplitude and time course of calcium action potentials. The calcium action potential (AP) consisted of two components: an initial fast phase followed by a slower plateau phase. No difference in the peak amplitude of the initial fast phase was observed between age groups. The amplitude and duration of the slower plateau phase of the calcium AP was significantly larger in aging neurons. Switching to a zero Ca2+ medium in the presence of 200 microns CdCl2 completely blocked the calcium AP. Nimodipine decreased the plateau phase of the calcium AP at concentrations as low as 100 nm in aging neurons and 10 microns in young neurons. Switching to higher concentrations of nimodipine did not reveal any substantially increased block of the calcium AP plateau phase. These data suggest that enhanced calcium influx through L-type calcium channels is largely responsible for the enhanced calcium action potentials observed in aging CA1 neurons. The action of nimodipine in reducing the plateau phase of the calcium action potential may underlie the drug's notable ability to improve learning in hippocampally dependent tasks in aging animals.

摘要

使用老年和成年幼兔的脑片,对体外培养的兔海马CA1神经元进行细胞内记录。在存在4微米河豚毒素的情况下,使用填充有2M CsCl的电极研究钙动作电位。在钙动作电位的幅度和时程上测试了二氢吡啶L型钙通道拮抗剂尼莫地平浓度的增加情况。钙动作电位(AP)由两个部分组成:一个初始快速相,随后是一个较慢的平台相。在不同年龄组之间,未观察到初始快速相的峰值幅度有差异。老年神经元中钙AP较慢平台相的幅度和持续时间显著更大。在存在200微米氯化镉的情况下切换到零钙培养基,完全阻断了钙AP。尼莫地平在老年神经元中低至100纳米的浓度以及在年轻神经元中10微米的浓度下,均可降低钙AP的平台相。切换到更高浓度的尼莫地平,并未显示出对钙AP平台相的阻断有任何实质性增加。这些数据表明,通过L型钙通道增强的钙内流在很大程度上导致了在老年CA1神经元中观察到的增强的钙动作电位。尼莫地平在降低钙动作电位平台相方面的作用,可能是该药物在改善老年动物海马依赖性任务学习方面显著能力的基础。

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