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Blue Again: Perturbational Effects of Antidepressants Suggest Monoaminergic Homeostasis in Major Depression

机译:再次变蓝:抗抑郁药的微扰作用提示严重抑郁症中单胺能稳态

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摘要

Some evolutionary researchers have argued that current diagnostic criteria for major depressive disorder (MDD) may not accurately distinguish true instances of disorder from a normal, adaptive stress response. According to disorder advocates, neurochemicals like the monoamine neurotransmitters (serotonin, norepinephrine, and dopamine) are dysregulated in major depression. Monoamines are normally under homeostatic control, so the monoamine disorder hypothesis implies a breakdown in homeostatic mechanisms. In contrast, adaptationist hypotheses propose that homeostatic mechanisms are properly functioning in most patients meeting current criteria for MDD. If the homeostatic mechanisms regulating monoamines are functioning properly in these patients, then oppositional tolerance should develop with prolonged antidepressant medication (ADM) therapy. Oppositional tolerance refers to the forces that develop when a homeostatic mechanism has been subject to prolonged pharmacological perturbation that attempt to bring the system back to equilibrium. When pharmacological intervention is discontinued, the oppositional forces cause monoamine levels to overshoot their equilibrium levels. Since depressive symptoms are under monoaminergic control, this overshoot should cause a resurgence of depressive symptoms that is proportional to the perturbational effect of the ADM. We test this prediction by conducting a meta-analysis of ADM discontinuation studies. We find that the risk of relapse after ADM discontinuation is positively associated with the degree to which ADMs enhance serotonin and norepinephrine in prefrontal cortex, after controlling for covariates. The results are consistent with oppositional tolerance, and provide no evidence of malfunction in the monoaminergic regulatory mechanisms in patients meeting current diagnostic criteria for MDD. We discuss the evolutionary and clinical implications of our findings.
机译:一些进化研究人员认为,当前对重度抑郁症(MDD)的诊断标准可能无法准确地区分正常的适应性应激反应。根据失调症的拥护者,在重度抑郁症中,神经化学物质如单胺神经递质(血清素,去甲肾上腺素和多巴胺)失调。单胺通常处于稳态控制下,因此单胺疾病假说暗示了稳态机制的崩溃。相反,适应主义者的假说提出,在满足当前MDD标准的大多数患者中,体内平衡机制均能正常发挥作用。如果调节单胺的稳态机制在这些患者中正常发挥作用,那么长期的抗抑郁药(ADM)治疗应发展为对立耐受性。对立耐受性是指当体内稳态机制受到长时间的药理扰动(试图使系统恢复平衡)时产生的力。停止药理干预时,对立作用力会导致单胺水平超过其平衡水平。由于抑郁症状在单胺能控制下,因此这种过冲会导致抑郁症状重新出现,与ADM的摄动作用成正比。我们通过对ADM停产研究进行荟萃分析来检验这一预测。我们发现,在控制协变量后,停用ADM后复发的风险与ADM增强额叶皮层中5-羟色胺和去甲肾上腺素的程度呈正相关。结果与对立的耐受性一致,并且在满足当前MDD诊断标准的患者中,单胺能调节机制没有任何故障的证据。我们讨论了我们发现的进化和临床意义。

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