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血清素转运体剂量调节大鼠和人类的长期决策。

Serotonin transporter dosage modulates long-term decision-making in rat and human.

作者信息

Homberg Judith R, van den Bos Ruud, den Heijer Esther, Suer Remco, Cuppen Edwin

机构信息

Department of Cognitive Neuroscience, Donders Centre for Neuroscience, UMC St. Radboud, Geert Grooteplein 28, 6525 GA Nijmegen, The Netherlands.

出版信息

Neuropharmacology. 2008 Jul;55(1):80-4. doi: 10.1016/j.neuropharm.2008.04.016. Epub 2008 Apr 26.

Abstract

Decision-making plays an important role in everyday life and is often disturbed in psychiatric conditions affected by the common human serotonin transporter promoter length polymorphism (5-HTTLPR). This raises the hypothesis that decision-making is modulated by the serotonergic system, but currently it is unclear how the 5-HTTLPR affects central serotonergic functioning. We tested healthy human volunteers genotyped for the 5-HTTLPR in the Iowa Gambling Task (IGT), which is one of the most frequently used neuropsychological tasks to assess decision-making. Furthermore, we tested female homozygous (SERT(-/-)) and heterozygous (SERT(+/-)) serotonin transporter knockout rats in a rodent version of the IGT. Women homozygous for the short (s) allele of the 5-HTTLPR were found to choose more disadvantageously than women homozygous for the long allele of the 5-HTTLPR as the IGT progressed. In the rat, SERT(-/-) and SERT(+/-) were associated with advantageous decision-making compared to SERT(+/+) as the IGT progressed. Combining the human and rat observations, we show that SERT dosage affects the maintenance of a once established choice option, irrespective of the choice (advantageous or disadvantageous) that has been made. We postulate that the SERT-mediated effects relate to deficits in the processing of choice outcome to guide subsequent choices in this gamble-based test, and that SERT(-/-) and SERT(+/-) rodent models in combination with studies in humans can be used to provide insight in the modulatory effects of 5-HTTLPR.

摘要

决策在日常生活中起着重要作用,而在受常见的人类血清素转运体启动子长度多态性(5-HTTLPR)影响的精神疾病中,决策常常受到干扰。这引发了一个假说,即决策受血清素能系统调节,但目前尚不清楚5-HTTLPR如何影响中枢血清素能功能。我们在爱荷华赌博任务(IGT)中对进行了5-HTTLPR基因分型的健康人类志愿者进行了测试,IGT是评估决策最常用的神经心理学任务之一。此外,我们在IGT的啮齿动物版本中对雌性纯合子(SERT(-/-))和杂合子(SERT(+/-))血清素转运体基因敲除大鼠进行了测试。随着IGT的进行,发现5-HTTLPR短(s)等位基因纯合的女性比5-HTTLPR长等位基因纯合的女性做出更不利的选择。在大鼠中,随着IGT的进行,与SERT(+/+)相比,SERT(-/-)和SERT(+/-)与有利决策相关。综合人类和大鼠的观察结果,我们表明,血清素转运体(SERT)的剂量会影响一旦确立的选择选项的维持,而与所做出的选择(有利或不利)无关。我们推测,SERT介导的效应与在这种基于赌博的测试中处理选择结果以指导后续选择的缺陷有关,并且SERT(-/-)和SERT(+/-)啮齿动物模型与人类研究相结合可用于深入了解5-HTTLPR的调节作用。

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