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豚鼠交感神经元上P2X三磷酸腺苷受体与烟碱受体的相互阻断

Mutual occlusion of P2X ATP receptors and nicotinic receptors on sympathetic neurons of the guinea-pig.

作者信息

Searl T J, Redman R S, Silinsky E M

机构信息

Department of Molecular Pharmacology, Northwestern University Medical School, 303 East Chicago Avenue, Chicago, IL 60611, USA.

出版信息

J Physiol. 1998 Aug 1;510 ( Pt 3)(Pt 3):783-91. doi: 10.1111/j.1469-7793.1998.783bj.x.


DOI:10.1111/j.1469-7793.1998.783bj.x
PMID:9660893
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2231072/
Abstract
  1. The interaction of ion channels activated by nicotinic receptor agonists with ion channels gated by extracellular ATP (i.e. P2X receptors) was studied on sympathetic neurons acutely dissociated from coeliac ganglia of the guinea-pig. Patch clamp methods were used to measure the inward current generated through these non-selective cationic channels under voltage clamp. 2. At the whole cell level, the specific nicotinic receptor agonists nicotine (5-100 microM) or cytisine (50-75 microM) and the P2X receptor agonists ATP (0.1-7 microM) or alpha,beta-methylene ATP (6 microM) were examined separately and in the presence of the other receptor activator. When a nicotinic and P2X receptor agonist were applied together, mutually occlusive effects were generally observed. This occurred even with concentrations of agonists that in themselves generated little to no inward current. 3. The occlusive effects of nicotinic agonists on ATP-gated currents were blocked by the nicotinic receptor/ion channel blocker hexamethonium (150 microM). The occlusive effects of ATP analogues on inward currents generated by nicotinic agonists were blocked by the P2X receptor antagonist suramin (100 microM). 4. Mutual occlusion of the effects of nicotinic agonists and ATP analogues were also observed when currents through single channels were studied in excised (outside-out) patches. 5. The results suggest that nicotinic receptors and P2X ATP receptors do not act independently in these sympathetic neurons.
摘要
  1. 在从豚鼠腹腔神经节急性分离的交感神经元上,研究了烟碱样受体激动剂激活的离子通道与细胞外ATP门控的离子通道(即P2X受体)之间的相互作用。采用膜片钳技术在电压钳制下测量通过这些非选择性阳离子通道产生的内向电流。2. 在全细胞水平,分别以及在另一种受体激活剂存在的情况下,检测了特异性烟碱样受体激动剂尼古丁(5 - 100微摩尔)或金雀花碱(50 - 75微摩尔)以及P2X受体激动剂ATP(0.1 - 7微摩尔)或α,β - 亚甲基ATP(6微摩尔)。当同时应用烟碱样和P2X受体激动剂时,通常会观察到相互阻断效应。即使使用本身产生很少或不产生内向电流的激动剂浓度时也会发生这种情况。3. 烟碱样受体/离子通道阻滞剂六甲铵(150微摩尔)可阻断烟碱样激动剂对ATP门控电流的阻断作用。P2X受体拮抗剂苏拉明(100微摩尔)可阻断ATP类似物对烟碱样激动剂产生的内向电流的阻断作用。4. 在切除的(外侧向外)膜片中研究单通道电流时,也观察到了烟碱样激动剂和ATP类似物效应的相互阻断。5. 结果表明,在这些交感神经元中,烟碱样受体和P2X ATP受体并非独立发挥作用。

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[1]
Mutual occlusion of P2X ATP receptors and nicotinic receptors on sympathetic neurons of the guinea-pig.

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[2]
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[4]
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[6]
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[7]
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[10]
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[3]
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[4]
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[5]
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[6]
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Purinergic Signal. 2012-5-1

[7]
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[8]
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[9]
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[10]
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本文引用的文献

[1]
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[2]
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