首页> 外文期刊>Pharmacological reports: PR >A competitive antagonist of NMDA receptors CGP 40116 attenuates experimental symptoms of schizophrenia evoked by MK-801.
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A competitive antagonist of NMDA receptors CGP 40116 attenuates experimental symptoms of schizophrenia evoked by MK-801.

机译:NMDA受体的竞争性拮抗剂CGP 40116可减轻MK-801诱发的精神分裂症的实验症状。

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In the present study, the interaction between a noncompetitive [(+)-MK-801] and a competitive (CGP 40116) NMDA receptor antagonists was tested in two different behavioral paradigms: locomotor activity test and prepulse inhibition of the acoustic startle reflex. Additionally, their effects on working memory and selective attention were evaluated in the delayed alternation task. All above paradigms served to model the symptoms of schizophrenia. It was found that locomotor stimulatory effect of (+)-MK-801 (0.4 mg/kg) was antagonized by prior administration of CGP 40116 (5 mg/kg). Lower doses of CGP 40116 (1.25 and 2.5 mg/kg) were ineffective. CGP 40116 given alone did not influence locomotor activity in rats. It was also shown that CGP 40116 antagonized the disruption of the process of sensorimotor gating evoked by (+)-MK-801. On the contrary, both CGP 40116 and (+)-MK-801 increased a number of errors in the delayed alternation test revealing detrimental effect of CGP 40116 on spatial working memory and selective attention even at a lower dose than that required to antagonize the effects of (+)-MK-801. The presented results indicate that noncompetitive and competitive NMDA receptor antagonists, when used at relatively low doses, may produce qualitatively different behavioral effects, as evidenced by the experiments with locomotor activity and prepulse inhibition. Moreover, the competitive NMDA receptor antagonists may even inhibit some psychotomimetic effects related to the noncompetitive blockade of this receptor. However, therapeutic potential of CGP 40116, a competitive NMDA receptor antagonist, should be considered with caution since in the range of doses effective against the psychotomimetic effects of (+)-MK-801, it impairs rats’ performance in the delayed alternation paradigm, i.e. it worsens efficacy of working memory.
机译:在本研究中,非竞争性[(+)-MK-801]与竞争性(CGP 40116)NMDA受体拮抗剂之间的相互作用在两种不同的行为范式中进行了测试:运动活性测试和听觉惊吓反射的脉冲抑制。此外,在延迟交替任务中评估了它们对工作记忆和选择性注意的影响。以上所有范例都可以用来模拟精神分裂症的症状。发现(+)-MK-801(0.4mg / kg)的运动刺激作用通过事先施用CGP 40116(5mg / kg)而被拮抗。较低剂量的CGP 40116(1.25和2.5 mg / kg)无效。单独使用CGP 40116不会影响大鼠的自发活动。还显示CGP 40116拮抗了(+)-MK-801引起的感觉运动门控过程的破坏。相反,CGP 40116和(+)-MK-801都增加了延迟交替测试中的许多错误,这表明CGP 40116对空间工作记忆和选择性注意的有害作用,即使其剂量低于拮抗作用所需的剂量也是如此。 (+)-MK-801。呈现的结果表明,非竞争性和竞争性NMDA受体拮抗剂以相对低的剂量使用时,可能产生质上不同的行为影响,如运动活动和脉冲前抑制的实验所证明。此外,竞争性NMDA受体拮抗剂甚至可以抑制与该受体非竞争性阻断有关的某些拟精神病作用。但是,应谨慎考虑竞争性NMDA受体拮抗剂CGP 40116的治疗潜力,因为在有效对抗(+)-MK-801拟精神病作用的剂量范围内,它会损害大鼠在延迟交替范式中的表现,即它恶化了工作记忆的功效。

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