舒必利对单侧额叶皮质消融大鼠旋转行为的逆转作用:其抗抑郁作用药理学机制的另一种解释

S. Kaneno, F. Fukamauchi, H. Komatsu, K. Koyama, K. Ikawa
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引用次数: 3

摘要

舒必利的抗抑郁作用通常被解释为其在低剂量下对自我抑制性突触前多巴胺自受体的优先阻断作用。小剂量氟哌啶醇具有相同的阻断作用。在单侧额叶皮质消融的大鼠中,甲基苯丙胺在手术后10天诱导轻度对侧旋转。我们检查了低剂量的磺胺吡啶和氟哌啶醇是否会对这种旋转模型产生相同的效果。高剂量舒必利(100 mg/kg)或低剂量氟哌啶醇(0.05 mg/kg)阻止甲基苯丙胺诱导的旋转。然而,低剂量(15mg /kg)的舒必利明显逆转了旋转方向。低剂量舒必利的这种逆转作用不能用对多巴胺自受体的优先阻断作用来解释。结果表明,与低剂量氟哌啶醇不同,低剂量舒必利对额叶皮层D2受体有明显的阻断作用。舒必利的这种独特作用可能与其临床低剂量抗抑郁和抗焦虑作用有关。
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Reversal effect of sulpiride on rotational behaviour of rats with unilateral frontal cortex ablation: an alternative explanation for the pharmacological mechanism of its antidepressant effect
The antidepressant effect of sulpiride has been generally explained as the result of its preferential blocking effect on self‐inhibitory presynaptic dopamine autoreceptors at low doses. Low dose haloperidol has the same blocking effect. In rats with unilateral ablation of the frontal cortex, methamphetamine administration induced mild contralateral rotation 10 days after the operation. We examined whether low dose sulpiride and haloperidol would have the same effect on this rotational model. High dose sulpiride (100 mg/kg) or low dose haloperidol (0.05 mg/kg) prevented this methamphetamine‐induced rotation. However, low dose (15 mg/kg) sulpiride clearly reversed the direction of rotation. This reversal effect of low dose sulpiride is not explained by the preferential blocking effect on dopamine autoreceptors. The results suggest that low dose sulpiride, unlike low dose haloperidol, has a prominent blocking effect on D2 receptors in the frontal cortex. This unique effect of sulpiride may be relevant to its clinical antidepressant and anxiolytic effects at low doses.
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