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脑组胺与精神分裂症:用BF2.649研究H3受体反向激动剂的潜在治疗应用

Brain histamine and schizophrenia: potential therapeutic applications of H3-receptor inverse agonists studied with BF2.649.

作者信息

Ligneau Xavier, Landais Laurent, Perrin David, Piriou Johanne, Uguen Marilyne, Denis Emmanuel, Robert Philippe, Parmentier Régis, Anaclet Christelle, Lin Jian-Sheng, Burban Aude, Arrang Jean-Michel, Schwartz Jean-Charles

机构信息

Bioprojet-Biotech, Saint Grégoire Cedex, France.

出版信息

Biochem Pharmacol. 2007 Apr 15;73(8):1215-24. doi: 10.1016/j.bcp.2007.01.023. Epub 2007 Jan 21.

Abstract

BF2.649, a high affinity and selective non-imidazole histamine H(3)-receptor antagonist/inverse agonist, was found to easily enter the brain after oral administration to mice: it displayed a ratio of brain/plasma levels of about 25 when considering either C(max) or AUC values. At low oral doses (2.5-20mg/kg), it elicited in mice a dose-dependent wakening effect accompanied with a shift towards high frequency waves of the EEG, a sign of cortical activation. DOPAC/dopamine ratios were enhanced in the prefrontal cortex but not in the striatum, indicating a selective activation of a sub-population of dopaminergic neurons. BF2.649 showed significant inhibitory activity in several mouse models of schizophrenia. It reduced locomotor hyperactivity elicited by methamphetamine or dizolcipine without significantly affecting spontaneous locomotor activity when administered alone. It also abolished the apomorphine-induced deficit in prepulse inhibition. These observations suggest that H(3)-receptor inverse agonists/antagonists deserve attention as a novel class of antipsychotic drugs endowed with pro-cognitive properties.

摘要

BF2.649是一种高亲和力、选择性非咪唑类组胺H(3)受体拮抗剂/反向激动剂,经口服给予小鼠后,发现其能轻松进入大脑:考虑C(max)或AUC值时,其脑/血浆水平比值约为25。在低口服剂量(2.5 - 20mg/kg)下,它能在小鼠中引发剂量依赖性的觉醒效应,并伴有脑电图向高频波的转变,这是皮质激活的迹象。前额叶皮质中的DOPAC/多巴胺比值升高,但纹状体中未升高,表明多巴胺能神经元亚群被选择性激活。BF2.649在几种精神分裂症小鼠模型中显示出显著的抑制活性。单独给药时,它能降低由甲基苯丙胺或地佐环平引起的运动亢进,而不显著影响自发运动活性。它还消除了阿扑吗啡诱导的前脉冲抑制缺陷。这些观察结果表明,H(3)受体反向激动剂/拮抗剂作为一类具有促认知特性的新型抗精神病药物值得关注。

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