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Stop signal response inhibition is not modulated by tryptophan depletion or the serotonin transporter polymorphism in healthy volunteers: implications for the 5-HT theory of impulsivity.

机译:在健康志愿者中,色氨酸耗竭或5-羟色胺转运蛋白多态性不会调节终止信号反应抑制:对5-HT冲动理论的影响。

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RATIONALE: Reduced serotonin neurotransmission is implicated in disorders of impulse control, but the involvement of serotonin in inhibitory processes in healthy human subjects remains unclear. OBJECTIVES: To investigate the effects of an acute manipulation of serotonin and genotype at a functional polymorphism in a gene coding for the serotonin transporter (5-HTT) on an established measure of response inhibition. METHODS: Serotonin function was reduced by the acute tryptophan depletion (ATD) procedure in a double-blind, crossover design in 42 healthy subjects. The Stop Signal Task (SST) was administered 5-7 h after drink administration. The influences of 5-HTT polymorphism, gender and trait impulsivity were investigated. RESULTS: ATD was associated with significant depletion of plasma tryptophan levels but did not increase the stop signal reaction time in comparison to the balanced (placebo) amino acid mixture. Subjects possessing the short allele of the 5-HTT polymorphism were not more impulsive on the SST than subjects homozygous for the long allele under placebo conditions and were not disproportionately sensitive to the effects of ATD. There was no effect of gender or trait impulsivity on ATD-induced change. CONCLUSIONS: We find no support for the involvement of brain serotonin neurotransmission in this form of inhibitory control in healthy human subjects.
机译:理由:5-羟色胺的神经传递减少与冲动控制障碍有关,但5-羟色胺是否参与健康人类受试者的抑制过程尚不清楚。目的:探讨在5-羟色胺转运蛋白(5-HTT)编码基因中,功能性多态性对5-羟色胺和基因型的急性操作对确定的反应抑制作用的影响。方法:通过42位健康受试者的双盲交叉设计,通过急性色氨酸耗竭(ATD)程序降低了血清素的功能。饮料给药后5-7小时给予停止信号任务(SST)。研究了5-HTT多态性,性别和性冲动的影响。结果:与平衡的(安慰剂)氨基酸混合物相比,ATD与血浆色氨酸水平的显着减少有关,但没有增加终止信号的反应时间。在安慰剂条件下,具有5-HTT多态性短等位基因的受试者对SST的冲动不比对长等位基因纯合的受试者更冲动,并且对ATD的影响不成比例地敏感。性别或特质冲动对ATD引起的变化没有影响。结论:我们不支持在健康的人类受试者中以这种形式的抑制控制参与脑5-羟色胺神经传递。

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