首页> 外文期刊>The Journal of Physiology >Sustained outward rectification of oxytocinergic neurones in the rat supraoptic nucleus: ionic dependence and pharmacology.
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Sustained outward rectification of oxytocinergic neurones in the rat supraoptic nucleus: ionic dependence and pharmacology.

机译:大鼠视上核中催产素能神经元的持续向外矫正:离子依赖性和药理学。

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1. Intracellular recordings were obtained in vitro from oxytocin and vasopressin neurones from dioestrous and lactating female rats. Oxytocin neurones were characterized under current clamp by the expression of a depolarization-activated, sustained outward rectification (SOR) and a rebound depolarization (RD). 2. An increment in extracellular K+ shifted the expression of the SOR and RD towards a more depolarized membrane potential, indicating that the mechanisms underlying these events are dependent on extracellular potassium. 3. The SOR and RD were blocked by external tetraethylammonium (10 mM) and Ba2+ (0.1-0.5 mM). Cs+ (2 mM) blocked the hyperpolarization-activated inward rectification without affecting the expression of the SOR and RD. 4. The SOR was not affected by 4-aminopyridine (6 mM). However, the rebound amplitude was significantly enhanced, indicating that the activation of a transient outward current interacts with the expression of the rebound. 5. Iberiotoxin (100 nM) and apamin (50 nM), toxins known to block some calcium-dependent potassium conductances, did not affect the expression of the SOR and RD. 6. The SOR and RD were significantly reduced by Cd2+ (0.5 mM) but not by Ni2+ (0.25 mM). 7. Muscarine (10 microM) did not affect the SOR or the RD. 8. These results indicate that the SOR and RD depend upon a depolarization-activated, sustained outward potassium current, which might be calcium dependent. A current with these characteristics has never been described before in the magnocellular system. Voltage-clamp experiments are needed to completely characterize this potassium conductance selectively expressed by oxytocin neurones.
机译:1.从雌雄同体和哺乳期雌性大鼠的催产素和加压素神经元体外获得细胞内记录。催产素神经元的特征是在电流钳下通过去极化激活,持续向外整流(SOR)和回弹去极化(RD)的表达来表征。 2.细胞外K +的增加使SOR和RD的表达移向更去极化的膜电位,表明这些事件的潜在机制取决于细胞外钾。 3. SOR和RD被外部四乙铵(10 mM)和Ba2 +(0.1-0.5 mM)阻断。 Cs +(2 mM)阻止了超极化激活的向内整流,而不会影响SOR和RD的表达。 4. SOR不受4-氨基吡啶(6 mM)的影响。但是,回弹幅度显着增强,表明瞬态向外电流的激活与回弹的表达相互作用。 5.已知会阻断某些钙依赖性钾电导的毒素伊波利毒素(100 nM)和阿帕明(50 nM)不会影响SOR和RD的表达。 6. Cd2 +(0.5 mM)显着降低了SOR和RD,Ni2 +(0.25 mM)未显着降低SOR和RD。 7.毒蕈碱(10 microM)不影响SOR或RD。 8.这些结果表明,SOR和RD取决于去极化激活的持续向外钾电流,这可能与钙有关。具有这些特征的电流以前从未在大型细胞系统中描述过。需要电压钳实验来完全表征由催产素神经元选择性表达的钾电导。

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