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Low dose morphine adjuvant therapy for enhanced efficacy of antipsychotic drug action: Potential involvement of endogenous morphine in the pathophysiology of schizophrenia

机译:低剂量吗啡辅助疗法可增强抗精神病药物作用的功效:内源性吗啡可能参与精神分裂症的病理生理

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Major thematic threads linking extensive preclinical and clinical efforts have established a working mechanistic scheme whereby atypical antipsychotic drugs ameliorate negative DSM IV diagnostic criteria by effecting relatively potent blockade of serotonin (5-HT)(2A) receptors coupled with weaker antagonism of dopamine D(2) receptors in frontal cortical areas. These contentions are more or less supported by in vitro binding experiments employing cloned receptors on cultured cells, although significant functional involvement of 5-HT(2C) receptors has also been proposed. It is interesting that a key statistical analysis indicates a major shift in usage back to typical antipsychotic agents for management of schizophrenia from 1995–2008, whereas off-label usage of atypical antipsychotic agents was markedly increased or expanded for bipolar affective disorder. Importantly, meta-analyses generally did not support efficacy differences between the other atypical antipsychotics compared with the older typical agents. A critical examination of putative functional linkages of morphine and its type-selective mu opioid receptor to higher order cortical regulation of cognitive processes may provide novel insights into human behavioral processes that are severely impaired in schizophrenia spectrum disorders.
机译:连接广泛的临床前和临床工作的主要主题线索已建立了一种有效的机制方案,该非典型抗精神病药可通过相对有效地阻断5-羟色胺(5-HT)(2A)受体并减弱多巴胺D(2)的拮抗作用来改善DSM IV阴性诊断标准。 )额叶皮层区域的受体。尽管已提出了5-HT(2C)受体的重要功能参与,但采用在培养细胞上克隆的受体的体外结合实验或多或少地支持了这些争论。有趣的是,一项关键的统计分析表明,从1995年至2008年,用于精神分裂症的典型使用已转向使用典型的抗精神病药,而对于双相情感障碍,非典型抗精神病药的标签外使用明显增加或扩大。重要的是,与较旧的典型药物相比,荟萃分析通常不支持其他非典型抗精神病药之间的疗效差异。对吗啡及其类型选择性μ阿片样物质受体与认知过程的更高阶皮质调节的假定功能性联系进行的严格检查,可能会为精神分裂症谱系障碍中严重受损的人类行为过程提供新的见解。

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