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首页> 外文期刊>European neuropsychopharmacology: the journal of the European College of Neuropsychopharmacology >Acute and chronic effects of NMDA receptor antagonists in rodents, relevance to negative symptoms of schizophrenia: A translational link to humans
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Acute and chronic effects of NMDA receptor antagonists in rodents, relevance to negative symptoms of schizophrenia: A translational link to humans

机译:NMDA受体拮抗剂在啮齿动物中的急性和慢性作用,与精神分裂症的阴性症状相关:与人类的翻译联系

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Negative symptoms of schizophrenia remain an unmet clinical need as they are common, persistent, respond poorly to existing treatments and lead to disability. Blunted affect, alogia, asociality, anhedonia and avolition are regarded as key negative symptoms despite DSM-IV-TR specifying a more limited range. The key to development of improved therapies is improved animal models that mimic the human condition in terms of behaviour and pathology and that predict efficacy of novel treatments in patients. Accumulating evidence shows that NMDA receptor (NMDAR) antagonists mimic cognitive deficits of relevance to schizophrenia in animals, along with associated pathological changes. This review examines evidence for the ability of NMDAR antagonists to mimic anhedonia and asociality, two negative symptoms of schizophrenia, in animals. The use of various species, paradigms and treatment regimens are reviewed. We conclude that sub-chronic treatment with NMDAR antagonists, typically PCP, induces social withdrawal in animals but not anhedonia. NMDAR antagonists have further effects in paradigms such as motivational salience that may be useful for mimicking other aspects of negative symptoms but these require further development. Sub-chronic treatment regimens of NMDAR antagonists also have some neurobiological effects of relevance to negative symptoms. It is our view that a sub-chronic treatment regime with NMDAR antagonists, particularly PCP, with animals tested following a wash-out period and in a battery of tests to assess certain behaviours of relevance to negative symptoms and social withdrawal (the animal equivalent of asociality) is valuable. This will enhance our understanding of the psycho and neuropathology of specific negative symptom domains and allow early detection of novel pharmacological targets.
机译:精神分裂症的阴性症状是常见的,持久的,对现有疗法的不良反应并导致残疾,因此仍未满足临床需求。尽管DSM-IV-TR规定的范围较窄,但钝化的情感,失语,社交性,快感不足和轻视被视为关键的负面症状。改进疗法发展的关键是改进动物模型,该动物模型在行为和病理方面模拟人类状况,并预测患者新疗法的疗效。越来越多的证据表明,NMDA受体(NMDAR)拮抗剂模拟与动物精神分裂症相关的认知缺陷以及相关的病理变化。这项审查审查了NMDAR拮抗剂模仿动物的精神分裂症的两个负面症状,快感和社交性的能力的证据。审查了各种物种,范例和治疗方案的使用。我们得出结论,用NMDAR拮抗剂(通常为PCP)进行亚慢性治疗可诱发动物社交退缩,但不会引起快感缺乏。 NMDAR拮抗剂在诸如动机显着性的范例中可能具有进一步的作用,这可能对模仿负面症状的其他方面很有用,但这些都需要进一步发展。 NMDAR拮抗剂的亚慢性治疗方案也具有与阴性症状相关的一些神经生物学作用。我们认为,使用NMDAR拮抗剂(尤其是PCP)进行亚慢性治疗的方案是,在冲洗期后对动物进行测试,并进行一系列测试以评估与阴性症状和社交退缩相关的某些行为(相当于动物社交性)很有价值。这将增强我们对特定阴性症状域的心理和神经病理学的理解,并允许及早发现新的药理学靶标。

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