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大鼠背外侧隔区神经元中烟碱受体介导的抑制作用的药理学

Pharmacology of nicotinic receptor-mediated inhibition in rat dorsolateral septal neurones.

作者信息

Wong L A, Gallagher J P

机构信息

Department of Pharmacology and Toxicology, University of Texas Medical Branch, Galveston.

出版信息

J Physiol. 1991 May;436:325-46. doi: 10.1113/jphysiol.1991.sp018553.

Abstract
  1. Intracellular electrophysiological techniques were employed to investigate the effects of nicotinic receptor stimulation on rat dorsolateral septal nucleus (DLSN) neurones in a submerged rat brain slice preparation. 2. Acetylcholine (in the presence of the muscarinic antagonist, atropine), nicotine or dimethylphenylpiperazinium (DMPP), applied either by pressure ejection or superfusion, produced predominantly a membrane potential hyperpolarization. 3. Following concentration-response comparisons, DMPP appeared to exhibit fewer desensitizing properties and greater efficacy than nicotine with half-maximal hyperpolarizing responses attainable at 3 and 10 microM, respectively. 4. Pharmacological analyses revealed that the agonist-induced membrane hyperpolarization was sensitive to antagonism by mecamylamine (50-100 microM) and neuronal bungarotoxin (0.2-0.3 microM), but not alpha-bungarotoxin (0.5-1.0 microM), curare (10-50 microM) or dihydro-beta-erythroidine (50-100 microM). 5. Hyperpolarizing responses to DMPP were found to reverse near the equilibrium potential for potassium and were sensitive to changes in extracellular potassium concentration as predicted by the Nernst equation. Under single-electrode voltage clamp, application of DMPP produced an outward current (75-100 pA) which approached reversal at around -88 mV. These findings indicated that the hyperpolarizing response to nicotinic receptor stimulation was mediated by changes in membrane permeability to potassium. 6. DMPP-induced membrane hyperpolarization resulted from a direct action on postsynaptic DLSN neurones since the response persisted under conditions of superfusion with calcium-free/high-magnesium media or tetrodotoxin; both conditions blocked orthodromically induced neurotransmission. The hyperpolarizing response remained unaltered in TTX but was diminished in calcium-free/high-magnesium media. Further studies revealed blockade of the DMPP response following intracellular injection of EGTA. This response was also sensitive to antagonism by various calcium-dependent potassium channel blockers including apamin, barium and tetraethylammonium. 7. Our studies reveal a novel class of CNS nicotinic receptor whose action upon stimulation by an agonist results in a membrane hyperpolarization via a calcium-dependent increase in potassium ion conductance.
摘要
  1. 采用细胞内电生理技术,在浸没的大鼠脑片标本中研究烟碱样受体刺激对大鼠背外侧隔核(DLSN)神经元的影响。2. 通过压力喷射或灌流施加乙酰胆碱(在毒蕈碱拮抗剂阿托品存在下)、尼古丁或二甲基苯基哌嗪(DMPP),主要产生膜电位超极化。3. 经浓度 - 反应比较,DMPP似乎比尼古丁表现出更少的脱敏特性和更高的效能,分别在3和10微摩尔时可达到半数最大超极化反应。4. 药理学分析表明,激动剂诱导的膜超极化对美加明(50 - 100微摩尔)和神经元型银环蛇毒素(0.2 - 0.3微摩尔)的拮抗敏感,但对α - 银环蛇毒素(0.5 - 1.0微摩尔)、箭毒(10 - 50微摩尔)或二氢 - β - 红古豆碱(50 - 100微摩尔)不敏感。5. 发现对DMPP的超极化反应在钾的平衡电位附近反转,并且如能斯特方程所预测的那样,对细胞外钾浓度的变化敏感。在单电极电压钳制下,施加DMPP产生外向电流(75 - 100皮安),在约 - 88毫伏时接近反转。这些发现表明,对烟碱样受体刺激的超极化反应是由膜对钾的通透性变化介导的。6. DMPP诱导的膜超极化是对突触后DLSN神经元的直接作用,因为在无钙/高镁培养基或河豚毒素灌流条件下该反应持续存在;这两种条件均阻断了顺向诱导的神经传递。在河豚毒素中,超极化反应保持不变,但在无钙/高镁培养基中减弱。进一步研究发现,细胞内注射乙二醇双四乙酸(EGTA)后DMPP反应被阻断。该反应对包括蜂毒明肽、钡和四乙铵在内的各种钙依赖性钾通道阻滞剂的拮抗也敏感。7. 我们的研究揭示了一类新型的中枢神经系统烟碱样受体,其在激动剂刺激下的作用通过钙依赖性增加钾离子电导导致膜超极化。

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