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Cognitive improvement by activation of alpha7 nicotinic acetylcholine receptors: from animal models to human pathophysiology.

机译:通过激活α7烟碱乙酰胆碱受体改善认知能力:从动物模型到人类病理生理学。

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摘要

Agonists and positive allosteric modulators of the alpha(7) nicotinic acetylcholine receptor (nAChR) are currently being developed for the treatment of cognitive disturbances in patients with schizophrenia or Alzheimer's disease. This review describes the neurobiological properties of the alpha nAChR and the cognitive effects of alpha(7) nAChR activation, focusing on the translational aspects in the development of these drugs. The functional properties and anatomical localization of the alpha(7) nAChR makes it well suited to modulate cognitive function. Accordingly, systemic administration of alpha(7) nAChR agonists improves learning, memory, and attentional function in variety of animal models, and pro-cognitive effects of alpha(7) nAChR agonists have recently been demonstrated in patients with schizophrenia or Alzheimer's disease. The alpha(7) nAChR desensitizes rapidly in vitro, and this has been a major concern in the development of alpha(7) nAChR agonists as putative drugs. Our review of the existing literature shows that development of tolerance to the behavioral effects of alpha(7) nAChR agonists does not occur in animal models or humans. However, the long-term memory-enhancing effects seen in animal models are not mimicked in healthy humans and schizophrenic patients, where attentional improvement predominates. This discrepancy may result from inherent differences in testing methods or from species differences in the level of expression of alpha(7) nAChRs in limbic brain regions, and may hamper preclinical evaluation of alpha(7) nAChR activation. It is therefore important to consider the translational power of the animal models used before entering into a clinical evaluation of the pro-cognitive effects of alpha(7) nAChR activation.
机译:目前正在开发激动剂和α(7)烟碱乙酰胆碱受体(nAChR)的正变构调节剂,用于治疗精神分裂症或阿尔茨海默氏病患者的认知障碍。这篇综述描述了alpha nAChR的神经生物学特性和alpha(7)nAChR激活的认知作用,重点是这些药物开发中的翻译方面。 alpha(7)nAChR的功能特性和解剖定位使其非常适合于调节认知功能。因此,系统地使用alpha(7)nAChR激动剂可以改善各种动物模型的学习,记忆和注意力功能,最近在精神分裂症或阿尔茨海默氏病患者中证明了alpha(7)nAChR激动剂的促认知作用。 alpha(7)nAChR在体外迅速脱敏,这一直是开发推定药物alpha(7)nAChR激动剂的主要问题。我们对现有文献的回顾表明,在动物模型或人类中不会发生对alpha(7)nAChR激动剂的行为影响的耐受性的发展。但是,在动物模型中看到的长期记忆增强作用并未在健康人和精神分裂症患者中被模仿,在这些患者中,注意力的改善是主要的。这种差异可能是由于测试方法的固有差异,也可能是由于边缘大脑区域中的alpha(7)nAChRs表达水平的物种差异引起的,并且可能会妨碍alpha(7)nAChR激活的临床前评估。因此,重要的是在进入对alpha(7)nAChR激活的促认知作用的临床评估之前,考虑所使用动物模型的翻译能力。

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