急性色氨酸耗竭对健康成人行为抑制的影响

T. J. Gaber
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引用次数: 3

摘要

5-羟色胺能(5-HT)神经传递的改变被认为在情感性障碍和冲动控制中起决定性作用。然而,关于大脑5-羟色胺可用性的参与及其对健康受试者行为抑制的影响的研究结果不一致。似乎中枢神经5 -羟色胺能神经传递与行为抑制的情境特异性方面有关,而不是单独的运动反应抑制。Crockett等人使用固定剂量的急性色氨酸消耗(ATD)程序,旨在解开5-羟色胺在单一行为Go-NoGo任务中运动反应抑制、惩罚诱导的不适当反应抑制以及对厌恶结果敏感性方面的参与。虽然运动反应抑制不受影响,但据报道,ATD可以消除惩罚诱导的抑制。目的应用新制定的改良体重调整ATD方案(Moja-De)。我们的目标是在年轻健康成人的可比样本中使用Go-NoGo任务复制Crockett等人的实验。方法24名健康志愿者采用随机、双盲、重复测量设计,采用与体重相适应的ATD方法降低中枢神经5-羟色胺合成。色氨酸平衡氨基酸饮料作为对照条件。上述Go-NoGo任务在饮料摄入后180分钟进行。在四个时间点采集血液样本:基线、90分钟、180分钟和270分钟。结果与平衡氨基酸负荷(BAL)相比,ATD后各时间点血浆总色氨酸和游离色氨酸水平均显著降低。虽然Go-NoGo的总体性能准确性不受ATD的影响,但响应时间显著缩短。此外,在大脑5-羟色胺合成减少后,调整行为反应的能力(关于厌恶结果的大小)和错误偶发惩罚后的行为调整保持不变。然而,没有观察到ATD对惩罚诱导抑制的解离作用。我们的研究使用了最近开发的一种改进的和单独调整的色氨酸消耗程序,评估了与Crockett等人使用的相同的行为任务,与原始研究相比,在5-羟色胺在行为抑制中的作用方面产生了具有挑战性的结果。我们的研究结果表明,与BAL相比,ATD Moja-De在同样低的性能准确性下促进了足够的响应(改进的响应时间)。在本样本中没有观察到惩罚诱导的抑制的特异性减少,因此挑战了原始研究中5-HT与抑制行为的厌恶背景相关的作用。总的来说,我们的研究结果表明,体重调整后的Moja-De色氨酸消耗不会导致惩罚相关行为功能的破坏。使用一种更精细和单独调整的消耗程序可能,至少部分地解释两项研究之间的差异。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Effects of Acute Tryptophan Depletion Moja-De on Behavioral Inhibition in Healthy Adults
Background Alterations in serotonergic (5-HT) neurotransmission are thought to play a decisive role in affective disorders and impulse control. However, the studies on the involvement of cerebral 5-HT availability and its effects on behavioral inhibition in healthy subjects yielded inconsistent findings. It appears that central nervous serotonergic neurotransmission is rather related to context-specific aspects of suppression of behavior than motor response inhibition alone. Crockett et al. aimed to disentangle the involvement of 5-HT on aspects of motor response inhibition, punishment-induced suppression of inappropriate responses, and sensitivity toward aversive outcomes in a single behavioral Go-NoGo task using a fixed dosage acute tryptophan depletion (ATD) procedure. While motor response inhibition was unaffected, punishmentinduced inhibition was reported to be abolished by ATD. Objective A recently developed refined and body-weight-adjusted ATD protocol (Moja-De) was applied. We aimed to replicate the experiment of Crockett et al. using a Go-NoGo task in a comparable sample of young healthy adults. Methods Central nervous 5-HT synthesis was lowered by administering a body-weight-adapted ATD procedure in a randomized, double-blind, within-subject, repeated measures design in 24 healthy volunteers. A tryptophan-balanced amino acid beverage served as a control condition. The above-mentioned Go-NoGo task was administered 180 minutes after beverage intake. Blood samples were obtained at four time points: baseline, 90 minutes, 180 minutes, and 270 minutes after beverage administration. Results ATD produced significant depletion of plasma levels of both total and free tryptophan at all post-ATD time points, compared with a balanced amino acid load (BAL). While overall Go-NoGo performance accuracy was not affected by ATD, response times significantly decreased. Also, the ability to adjust behavioral responding in regard to aversive outcome magnitude and behavioral adjustments following error contingent punishment remain intact after decreased brain 5-HT synthesis. However, no dissociation effect of ATD on punishment-induced inhibition was observed. Conclusion Our study using a recently developed refined and individually adjusted tryptophan depletion procedure assessed with the identical behavioral task as used by Crockett et al. yielded challenging results compared with the original study in terms of the role of 5-HT in behavioral inhibition. Our findings suggest that ATD Moja-De facilitates adequate responding (improved response times) at equally low performance accuracy, compared with BAL. ATD-specific reductions in punishment-induced inhibition were not observed in the present sample, thus challenging the suggested role of 5-HT related to the aversive context of inhibitory behavior in the original study. Overall, our results suggest that body weight adjusted Moja-De trypthophan depletion does not result in disruptions of punishment related behavioral functioning. The use of a more refined and individually adjusted depletion procedure might, at least in part, explain the discrepancies between the two studies.
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