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Serotonin receptors represent highly favorable molecular targets for cognitive enhancement in schizophrenia and other disorders.

机译:5-羟色胺受体代表用于精神分裂症和其他疾病的认知增强的高度有利的分子靶标。

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RATIONALE. Current treatments for schizophrenia adequately treat the positive symptoms of schizophrenia but only modestly improve cognitive deficits. This review provides evidence for and against the use of selective 5-HT receptor drugs as cognition enhancing agents for schizophrenia and other disorders. METHODS. Pre-clinical and clinical literature concerned with the role of the serotonergic system in cognition and memory as it relates to schizophrenia is reviewed. Individual 5-HT receptor subtypes for which selective drugs are available that are likely to improve cognition are reviewed. Recommendations for clinical testing are proposed. RESULTS AND CONCLUSIONS. Four 5-HT receptor systems (5-HT(1A), 5-HT(2A), 5-HT(4), 5-HT(6)) are highlighted as suitable targets for enhancing cognition and memory. Because many clinically available antipsychotic drugs already target 5-HT(1A), 5-HT(2A) and 5-HT(6) receptors, design of clinical trials will need to take into account the serotonergic pharmacology of concurrently administered antipsychotic medications. 5-HT(1A) partial agonists and 5-HT(2A) antagonists have shown modest effectiveness in improving cognition in schizophrenia. 5-HT(6)-selective compounds for cognition enhancement are in late-stage clinical trials, while 5-HT(4) compounds have not yet been tested in humans for cognition enhancement. RECOMMENDATIONS. For stand-alone therapy for enhancing cognition, 5-HT(1A) partial agonists, 5-HT(2A) antagonists, 5-HT(4) partial agonists and 5-HT(6) antagonists are all likely to induce at least modest improvement in cognition in schizophrenia. If "add-on therapy" is contemplated, antipsychotic drugs with weak affinities for serotonin receptors should be used to avoid confounds. It is likely that serotonergic drugs will soon be available as cognition enhancing medications for disorders other than schizophrenia (e.g. dementia).
机译:理据。当前的精神分裂症治疗足以治疗精神分裂症的阳性症状,但仅适度地改善认知缺陷。这篇综述提供了支持和反对使用选择性5-HT受体药物作为精神分裂症和其他疾病的认知增强剂的证据。方法。审查了有关血清素能系统在与精神分裂症有关的认知和记忆中的作用的临床前和临床文献。审查了个别5-HT受体亚型,这些亚型有可能改善认知能力的选择性药物。提出了临床测试的建议。结果与结论。强调了四个5-HT受体系统(5-HT(1A),5-HT(2A),5-HT(4),5-HT(6))作为增强认知和记忆的合适目标。由于许多临床上可用的抗精神病药物已经靶向5-HT(1A),5-HT(2A)和5-HT(6)受体,因此临床试验的设计将需要考虑同时服用抗精神病药物的血清素能药理学。 5-HT(1A)部分激动剂和5-HT(2A)拮抗剂在改善精神分裂症认知方面显示出适度的有效性。 5-HT(6)-选择性增强认知能力的化合物正在后期临床试验中,而5-HT(4)-化合物尚未在人体中测试过认知增强的能力。建议。对于增强认知的独立疗法,5-HT(1A)部分激动剂,5-HT(2A)拮抗剂,5-HT(4)部分激动剂和5-HT(6)拮抗剂都可能诱导至少适度的精神分裂症认知的改善。如果考虑采用“附加疗法”,则应使用对5-羟色胺受体亲和力弱的抗精神病药,以避免混淆。血清素能药物很可能很快将作为精神分裂症以外的疾病(例如痴呆)的认知增强药物。

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