Positron emission tomography study of the effects of tryptophan depletion on brain serotonin(2) receptors in subjects recently remitted from major depression.

Archives of general psychiatry Pub Date : 2012-06-01 DOI:10.1001/archgenpsychiatry.2011.1493

Lakshmi N Yatham, Peter F Liddle, Vesna Sossi, Jonathan Erez, Nasim Vafai, Raymond W Lam, Stephan Blinder

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引用次数: 18

Abstract

Context: Decreased brain serotonin (5-hydroxytryptamine) levels are considered to mediate depressive relapse induced by the tryptophan depletion paradigm. However, in patients who recently achieved remission from a major depressive episode with antidepressant treatment, only about half become depressed following tryptophan depletion. We hypothesized that downregulation of brain serotonin(2) receptors might be a compensatory mechanism that prevents some patients from becoming depressed with tryptophan depletion.

Objective: To assess, with use of positron emission tomography, whether brain serotonin(2) receptor downregulation occurs in patients with recently remitted depression who do not have depressive relapse, but not in those who become depressed, following tryptophan depletion.

Design: Each patient underwent 2 fluorine 18-labeled- setoperone positron emission tomography scans, one following a tryptophan depletion session and another following a control session. The order of scanning was counterbalanced.

Setting: Academic university hospital with imaging facilities.

Participants: Seventeen patients in recent remission from a DSM-IV major depressive episode following treatment with selective serotonin reuptake inhibitors.

Main outcome measures: Changes in brain serotonin(2) receptor binding.

Results: Of the 17 patients, 8 (47%) became depressed during the tryptophan depletion session, and none developed depression during the control session. The depletion session was associated with a significant reduction in brain serotonin(2) receptor binding compared with the control session for all participants. A subgroup analysis revealed that the reduction in serotonin(2) receptor binding was significant only for the nondepressed group.

Conclusion: Reduction in brain serotonin(2) receptors might be a potential compensatory mechanism to prevent tryptophan depletion-induced depressive relapse.

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正电子发射断层扫描研究色氨酸耗竭对重度抑郁症患者脑血清素(2)受体的影响。

背景:脑血清素(5-羟色胺)水平降低被认为介导了由色氨酸耗竭范式引起的抑郁症复发。然而，在最近通过抗抑郁治疗从重度抑郁发作中获得缓解的患者中，只有大约一半的患者在色氨酸耗竭后变得抑郁。我们假设脑血清素(2)受体的下调可能是一种代偿机制，可以防止一些患者因色氨酸缺乏而变得抑郁。目的:利用正电子发射断层扫描，评估脑血清素(2)受体下调是否发生在新近缓解的抑郁症患者中，这些患者没有抑郁复发，但在色氨酸缺失后出现抑郁。设计:每位患者接受了2次氟18标记的setoperone正电子发射断层扫描，其中一次是色氨酸消耗期，另一次是对照期。扫描的顺序被平衡了。环境:有影像设备的学术大学医院。参与者:17例在接受选择性血清素再摄取抑制剂治疗后，最近从DSM-IV重度抑郁发作缓解的患者。主要观察指标:脑血清素(2)受体结合变化。结果:在17例患者中，8例(47%)在色氨酸消耗阶段出现抑郁，而在对照阶段没有出现抑郁。与对照组相比，所有参与者的脑血清素(2)受体结合明显减少。亚组分析显示，血清素(2)受体结合的减少仅在非抑郁组中显着。结论:脑5 -羟色胺(2)受体的减少可能是防止色氨酸消耗引起的抑郁症复发的潜在代偿机制。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Archives of general psychiatry 医学-精神病学

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4-8 weeks