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PDE10A 抑制剂对 MK-801 诱导的强迫游泳试验中不动性的影响。

Effect of PDE10A inhibitors on MK-801-induced immobility in the forced swim test.

机构信息

biocrea GmbH, Radebeul, Germany.

出版信息

Psychopharmacology (Berl). 2012 May;221(2):249-59. doi: 10.1007/s00213-011-2567-y. Epub 2011 Nov 16.

DOI:10.1007/s00213-011-2567-y
PMID:22147257
Abstract

RATIONALE

Negative symptoms of schizophrenia are insufficiently treated by current antipsychotics. However, research is limited by the lack of validated models. Clinical data indicate that phencyclidine (PCP) abuse may induce symptoms resembling negative symptoms in humans. Based on that, Noda et al. proposed a model of PCP-induced increase of immobility in the forced swim test in mice as a model of depression-like negative symptoms of schizophrenia.

OBJECTIVES

The aim of the study was to evaluate the effect of phosphodiesterase 10A (PDE10A) inhibition in this model which was modified by using MK-801 instead of PCP.

METHODS

Increase of immobility in the forced swim test was induced by repeated MK-801 treatment followed by a 2-day washout in mice. The effect of haloperidol, clozapine, risperidone and PDE10A inhibitors was evaluated in this model, on open-field activity and acute MK-801-induced hyperactivity.

RESULTS

Repeated MK-801 treatment significantly increased immobility in the forced swim test without affecting open-field activity. It induced hypersensitivity to the dopamine D1 agonist A-68930, suggesting a hypofunction of the D1 pathway. The increase of immobility is reversed by clozapine and PDE10A inhibitors, but not by haloperidol. Clozapine and the PDE10A inhibitors did not enhance activity at effective doses.

CONCLUSION

The possibility to substitute PCP by MK-801 in this model indicates that the effect is mediated by their common mechanism of NMDA antagonism. PDE10A inhibitors similar to clozapine significantly antagonize the increase of immobility, suggesting a therapeutic potential for the treatment of negative symptoms. However, further validation of the model is necessary.

摘要

原理

目前的抗精神病药物对精神分裂症的阴性症状治疗不足。然而,研究受到缺乏经过验证的模型的限制。临床数据表明,苯环己哌啶(PCP)滥用可能会导致人类出现类似阴性症状的症状。基于这一点,Noda 等人提出了一种 PCP 诱导的小鼠强迫游泳试验中不动性增加的模型,作为精神分裂症阴性症状的模型。

目的

本研究旨在评估磷酸二酯酶 10A(PDE10A)抑制在该模型中的作用,该模型通过使用 MK-801 代替 PCP 进行了修改。

方法

通过重复 MK-801 处理并用 2 天的洗脱期在小鼠中诱导强迫游泳试验中的不动性增加。在该模型中评估了氟哌啶醇、氯氮平、利培酮和 PDE10A 抑制剂的作用,包括对旷场活动和急性 MK-801 诱导的过度活动的影响。

结果

重复 MK-801 处理显著增加了强迫游泳试验中的不动性,而不影响旷场活动。它诱导了对多巴胺 D1 激动剂 A-68930 的超敏反应,表明 D1 途径功能低下。氯氮平和 PDE10A 抑制剂逆转了不动性的增加,但氟哌啶醇没有。氯氮平和 PDE10A 抑制剂在有效剂量下不会增强活动。

结论

该模型中用 MK-801 替代 PCP 的可能性表明,这种作用是由它们共同的 NMDA 拮抗作用机制介导的。与氯氮平相似的 PDE10A 抑制剂显著拮抗不动性的增加,表明它们具有治疗阴性症状的潜在治疗作用。然而,该模型还需要进一步验证。

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