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本文引用的文献

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Patch Clamp Recordings from the Epithelium of the Lens Obtained using Glasses Selected for Low Noise and Improved Sealing Properties.使用具有低噪声和改善的密封特性的玻璃电极从晶状体上皮进行膜片钳记录。
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Calcium-antagonists and islet function-XII. Comparison between nifedipine and chemically related drugs.钙拮抗剂与胰岛功能 - XII. 硝苯地平与化学相关药物的比较。
Biochem Pharmacol. 1981 May 15;30(10):1039-41. doi: 10.1016/0006-2952(81)90439-1.
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Persistent slow inward calcium current in voltage-clamped hippocampal neurones of the guinea-pig.豚鼠海马神经元电压钳制下持续存在的缓慢内向钙电流。
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Thyrotropin-releasing hormone mobilizes Ca2+ from endoplasmic reticulum and mitochondria of GH3 pituitary cells: characterization of cellular Ca2+ pools by a method based on digitonin permeabilization.促甲状腺激素释放激素从GH3垂体细胞的内质网和线粒体中动员Ca2+:基于洋地黄皂苷通透法对细胞Ca2+池的表征
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Electrical behaviour in a line of anterior pituitary cells (GH cells) and the influence of the hypothalamic peptide, thyrotrophin releasing factor.垂体前叶细胞系(生长激素细胞)中的电活动及下丘脑肽促甲状腺激素释放因子的影响
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Gas and liquid chromatographic analyses of nimodipine calcium antagonist in blood plasma and cerebrospinal fluid.血浆和脑脊液中钙拮抗剂尼莫地平的气相色谱和液相色谱分析。
J Chromatogr. 1984 Jan 13;305(1):105-18. doi: 10.1016/s0378-4347(00)83318-6.
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Excitable membrane properties of cultured central nervous system neurons and clonal pituitary cells.
Cold Spring Harb Symp Quant Biol. 1983;48 Pt 1:259-68. doi: 10.1101/sqb.1983.048.01.028.
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A low voltage-activated calcium conductance in embryonic chick sensory neurons.胚胎期鸡感觉神经元中的低电压激活钙电导。
Biophys J. 1984 Sep;46(3):413-8. doi: 10.1016/S0006-3495(84)84037-0.
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Nifedipine and endocrine status in diabetic patients.硝苯地平与糖尿病患者的内分泌状态
Br J Clin Pharmacol. 1984 Oct;18(4):648-50. doi: 10.1111/j.1365-2125.1984.tb02523.x.
10
Relationship of thyrotropin-releasing hormone-induced spike and plateau phases in cytosolic free Ca2+ concentrations to hormone secretion. Selective blockade using ionomycin and nifedipine.促甲状腺激素释放激素诱导的胞质游离钙离子浓度尖峰和平台期与激素分泌的关系。使用离子霉素和硝苯地平进行选择性阻断。
J Biol Chem. 1984 Dec 25;259(24):15350-63.

尼莫地平对大鼠垂体前叶细胞钙通道的阻滞作用

Nimodipine block of calcium channels in rat anterior pituitary cells.

作者信息

Cohen C J, McCarthy R T

机构信息

Miles Institute for Preclinical Pharmacology, New Haven, CT 06509.

出版信息

J Physiol. 1987 Jun;387:195-225. doi: 10.1113/jphysiol.1987.sp016570.

DOI:10.1113/jphysiol.1987.sp016570
PMID:2443679
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1192501/
Abstract
  1. Ca channels were studied in the GH4C1 clonal cell line derived from rat anterior pituitary cells. The whole-cell variation of the patch-electrode voltage-clamp technique was used. 2. Two types of Ca channels were found. One type ('slowly inactivating' channels) is insensitive to changes in holding potential, does not inactivate during test pulses lasting several seconds, and deactivates very quickly upon repolarization. For holding potentials less than -40 mV, a second type of Ca channel is available for opening. This population ('transient' channels) differs from the first type in that it activates at more negative potentials, inactivates rapidly with either Ca or Ba as the charge carrier, deactivates about 10 times more slowly upon repolarization, and is less selective for Ba over Cs. 3. Nimodipine preferentially blocks the slowly inactivating channels. Block of these channels is time- and voltage-dependent, such that block is maximized by long depolarizations. 4. A comparison of the voltage dependence of steady-state nimodipine block with the voltage dependence of channel activation indicates that channel block is directly proportional to the number of open channels. The results are accounted for by a model that postulates 1:1 high-affinity drug binding to open Ca channels. The apparent dissociation constant for binding to open channels is 517 pM. Similar binding constants were previously reported for the inhibition of high-K-induced hormone secretion and high-affinity ligand binding of [3H]nimodipine to isolated plasma membranes. 5. The rate of onset of nimodipine block increases with the test potential, in quantitative agreement with the model of open-channel block. The apparent association rate is about 9.6 X 10(7) M-1 s-1; the dissociation rate is about 0.050 s-1. At therapeutic concentrations (less than 10 nM) nimodipine block takes many seconds to reach equilibrium. 6. Nimodipine should have little effect on stimulus-secretion coupling in healthy pituitary cells in vivo because: (a) the drug binds very weakly to the transient channels that are open at normal resting potentials, and (b) negligible high-affinity binding occurs during spontaneous activity because the onset of block is very slow.
摘要
  1. 在源自大鼠垂体前叶细胞的GH4C1克隆细胞系中研究了钙通道。采用膜片钳电压钳技术的全细胞记录模式。2. 发现了两种类型的钙通道。一种类型(“缓慢失活”通道)对钳制电位的变化不敏感,在持续数秒的测试脉冲期间不失活,复极化时失活非常迅速。对于小于-40 mV的钳制电位,第二种类型的钙通道可被激活。这群通道(“瞬时”通道)与第一种类型的不同之处在于,它在更正的电位时被激活,以钙或钡作为载流子时迅速失活,复极化时失活速度慢约10倍,对钡和铯的选择性较低。3. 尼莫地平优先阻断缓慢失活通道。这些通道的阻断具有时间和电压依赖性,因此长时间去极化时阻断作用最大。4. 稳态尼莫地平阻断的电压依赖性与通道激活的电压依赖性的比较表明,通道阻断与开放通道的数量成正比。结果可以用一个假设1:1高亲和力药物与开放钙通道结合的模型来解释。与开放通道结合的表观解离常数为517 pM。先前曾报道过类似的结合常数,用于抑制高钾诱导的激素分泌以及[3H]尼莫地平与分离的质膜的高亲和力配体结合。5. 尼莫地平阻断的起始速率随测试电位增加,与开放通道阻断模型在数量上一致。表观结合速率约为9.6×10(7) M-1 s-1;解离速率约为0.050 s-1。在治疗浓度(小于10 nM)下,尼莫地平阻断需要数秒才能达到平衡。6. 尼莫地平对体内健康垂体细胞的刺激-分泌偶联应该影响很小,因为:(a) 该药物与在正常静息电位时开放的瞬时通道结合非常弱,以及(b) 在自发活动期间可忽略不计的高亲和力结合发生,因为阻断的起始非常缓慢。