氯化钡和4-氨基吡啶诱发的大鼠输精管相性收缩。

BaCl2- and 4-aminopyridine-evoked phasic contractions in the rat vas deferens.

作者信息

Huang Y

机构信息

Department of Physiology, Chinese University of Hong Kong, Shatin, NT.

出版信息

Br J Pharmacol. 1995 Jul;115(5):845-51. doi: 10.1111/j.1476-5381.1995.tb15010.x.

DOI:10.1111/j.1476-5381.1995.tb15010.x

PMID:8548186

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1908510/

Abstract

The actions of BaCl2 and 4-aminopyridine, blockers of K+ channels, on the mechanical activity of the epididymal half of the rat vas deferens were investigated. 2. Both BaCl2 and 4-aminopyridine dose-dependently evoked phasic contractions. High extracellular potassium (35-40 mM) caused a tonic contraction but abolished the BaCl2- and 4-aminopyridine-induced phasic activity and reduced the BaCl2-induced sustained component of contraction, but increased the 4-aminopyridine-induced tonic contraction. 3. Omission of calcium from the extracellular medium totally abolished the 4-aminopyridine-induced response but only reduced the mean amplitude of phasic contractions induced by BaCl. 4. Procaine (10 mM), an inhibitor of internal calcium release, completely abolished the phasic activity and reduced the sustained contraction induced by BaCl2. The remaining tone was abolished by nifedipine (1 microM). 5. Tetraethylammonium (1 mM) suppressed the amplitude of the BaCl2-induced phasic contractions, and induced a biphasic increase in tonic tension. 6. The BaCl2-induced responses were resistant to prazosin (1 microM), yohimbine (3 microM), propranolol (3 microM) or atropine (3 microM); in contrast, the 4-aminopyridine-induced activity was effectively inhibited by prazosin (1 microM) attenuated by yohimbine (1 microM) and atropine (1 microM) but not by propranolol (3 microM). The 4-aminopyridine-induced response was abolished by pretreatment of the vas deferens with 6-hydroxydopamine (0.5 mM). 7. The results indicate that the BaCl2-evoked activity in the vas deferens was mainly due to blockade of Ba(2+)-sensitive K+ channels on the smooth muscle plasma membrane. Subsequent calcium entry through the depolarized plasma membrane was needed to trigger generation of phasic contractions. 4-Aminopyridine-induced action, however, was largely mediated by neurotransmitters released from the depolarized nerve terminals as a result of blockade of K+ channels.

摘要

研究了钾通道阻滞剂氯化钡（BaCl₂）和4-氨基吡啶对大鼠输精管附睾段机械活性的作用。2. BaCl₂和4-氨基吡啶均剂量依赖性地诱发相位性收缩。高细胞外钾（35 - 40 mM）引起强直性收缩，但消除了BaCl₂和4-氨基吡啶诱导的相位性活动，并降低了BaCl₂诱导的持续性收缩成分，但增加了4-氨基吡啶诱导的强直性收缩。3. 细胞外培养基中去除钙完全消除了4-氨基吡啶诱导的反应，但仅降低了BaCl₂诱导的相位性收缩的平均幅度。4. 普鲁卡因（10 mM），一种细胞内钙释放抑制剂，完全消除了相位性活动并降低了BaCl₂诱导的持续性收缩。剩余的张力被硝苯地平（1 μM）消除。5. 四乙铵（1 mM）抑制了BaCl₂诱导的相位性收缩的幅度，并诱导了强直性张力的双相增加。6. BaCl₂诱导的反应对哌唑嗪（1 μM）、育亨宾（3 μM）、普萘洛尔（3 μM）或阿托品（3 μM）有抗性；相反，4-氨基吡啶诱导的活动被哌唑嗪（1 μM）有效抑制，被育亨宾（1 μM）和阿托品（1 μM）减弱，但不被普萘洛尔（3 μM）抑制。用6-羟基多巴胺（0.5 mM）预处理输精管可消除4-氨基吡啶诱导的反应。7. 结果表明，输精管中BaCl₂诱发的活动主要是由于平滑肌质膜上对Ba(2+)敏感的钾通道被阻断。随后需要通过去极化的质膜进入钙来触发相位性收缩的产生。然而，4-氨基吡啶诱导的作用很大程度上是由去极化神经末梢因钾通道被阻断而释放的神经递质介导的。