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Antipsychotic antidepressant and cognitive-impairment properties of antipsychotics: rat profile and implications for behavioral and psychological symptoms of dementia

机译:抗精神病药的抗精神病药抗抑郁药和认知障碍特性:大鼠概况及其对痴呆症的行为和心理症状的影响

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摘要

Many dementia patients exhibit behavioral and psychological symptoms (BPSD), including psychosis and depression. Although antipsychotics are frequently prescribed off-label, they can have marked side effects. In addition, comparative preclinical studies of their effects are surprisingly scarce, and strategies for discovery of novel pharmacotherapeutics are lacking. We therefore compared eight antipsychotics in rat behavioral tests of psychosis, antidepressant-like activity, and cognitive impairment as a basis for preclinical evaluation of new drug candidates. The methods used in this study include inhibition of MK-801-induced hyperactivity, forced swim test (FST), passive avoidance (PA), spontaneous locomotor activity, and catalepsy. The drugs exhibited antipsychotic-like activity in the MK-801 test but with diverse profiles in the other models. Risperidone impaired PA performance, but with some dose separation versus its actions in the MK-801 test. In contrast, clozapine, olanzapine, lurasidone, and asenapine showed little or no dose separation in these tests. Aripiprazole did not impair PA performance but was poorly active in the MK-801 test. Diverse effects were also observed in the FST: chlorpromazine was inactive and most other drugs reduced immobility over narrow dose ranges, whereas clozapine reduced immobility over a wider dose range, overlapping with antipsychotic activity. Although the propensity of second-generation antipsychotics to produce catalepsy was lower, they all elicited pronounced sedation. Consistent with clinical data, most currently available second-generation antipsychotics induced cognitive and motor side effects with little separation from therapeutic-like doses. This study provides a uniform in vivo comparative basis on which to evaluate future early-stage drug candidates intended for potential pharmacotherapy of BPSD.
机译:许多痴呆症患者表现出行为和心理症状(BPSD),包括精神病和抑郁症。尽管经常将抗精神病药开出标签,但它们可能会产生明显的副作用。此外,其效果的比较临床前研究令人惊讶地稀缺,并且缺乏发现新型药物治疗剂的策略。因此,我们比较了八种抗精神病药在大鼠对精神病,抗抑郁样活性和认知障碍的行为测试中,作为新药临床前评估的基础。本研究中使用的方法包括抑制MK-801诱导的机能亢进,强迫游泳试验(FST),被动回避(PA),自发运动能力和僵直。这些药物在MK-801测试中表现出类似抗精神病药的活性,但在其他模型中却具有多种多样的特征。利培酮削弱了PA的性能,但是在MK-801测试中,其剂量分离与其作用有所不同。相反,氯氮平,奥氮平,卢拉西酮和阿塞那平在这些试验中显示出很少或没有剂量分离。阿立哌唑不损害PA性能,但在MK-801测试中活性较差。在FST中还观察到了多种影响:氯丙嗪没有活性,大多数其他药物在较窄的剂量范围内降低了固定性,而氯氮平在较宽的剂量范围内降低了固定性,同时具有抗精神病活性。尽管第二代抗精神病药产生僵直的倾向较低,但它们均引起明显的镇静作用。与临床数据一致,大多数当前可用的第二代抗精神病药可引起认知和运动方面的副作用,与治疗剂量的剂量几乎没有区别。这项研究提供了一个统一的体内比较基础,可在此基础上评估预期用于BPSD潜在药物疗法的早期候选药物。

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