Foti Dan, Carlson Joshua M, Sauder Colin L, Proudfit Greg H
Department of Psychological Sciences, Purdue University, West Lafayette, IN, USA.
Department of Psychology, Northern Michigan University, Marquette, MI, USA.
Neuroimage. 2014 Nov 1;101:50-8. doi: 10.1016/j.neuroimage.2014.06.058. Epub 2014 Jul 1.
Reward dysfunction is thought to play a core role in the pathophysiology of major depressive disorder (MDD). Event-related potential (ERP) and functional magnetic resonance imaging (fMRI) studies have identified reward processing deficits in MDD, but these methods have yet to be applied together in a single MDD sample. We utilized multimodal neuroimaging evidence to examine reward dysfunction in MDD. Further, we explored how neurobiological reward dysfunction would map onto subtypes of MDD. The feedback negativity (FN), an ERP index of reward evaluation, was recorded in 34 unmedicated depressed individuals and 42 never-depressed controls during a laboratory gambling task. Ventral striatal (VS) activation to reward was recorded in a separate fMRI session, using an identical task, among a subgroup of 24 depressed individuals and a comparison group of 18 non-depressed controls. FN amplitude was blunted in MDD. This effect was driven by a MDD subgroup characterized by impaired mood reactivity to positive events, a core feature of melancholic MDD. A similar pattern was observed for VS activation, which was also blunted among the MDD subgroup with impaired mood reactivity. Neither FN amplitude nor VS activation was related to the full, DSM-defined melancholic or atypical MDD subtypes. Across the MDD sample, FN amplitude and VS activation were correlated, indicating convergence across methods. These results indicate that not all MDD is characterized by reward dysfunction, and that there is meaningful heterogeneity in reward processing within MDD. The current study offers neurobiological evidence that impaired mood reactivity is a key phenotypic distinction for subtyping MDD, and further suggests that the existing melancholic phenotype may require further refinement.
奖赏功能障碍被认为在重度抑郁症(MDD)的病理生理学中起核心作用。事件相关电位(ERP)和功能磁共振成像(fMRI)研究已确定MDD存在奖赏处理缺陷,但这些方法尚未在单一MDD样本中联合应用。我们利用多模态神经影像学证据来检查MDD中的奖赏功能障碍。此外,我们还探讨了神经生物学奖赏功能障碍如何映射到MDD的亚型上。在一项实验室赌博任务中,对34名未服药的抑郁症患者和42名从未患过抑郁症的对照者记录了作为奖赏评估ERP指标的反馈负波(FN)。在另一项fMRI实验中,使用相同任务,对24名抑郁症患者亚组和18名非抑郁症对照者比较组记录腹侧纹状体(VS)对奖赏的激活情况。MDD患者的FN波幅减弱。这种效应是由一个以对积极事件的情绪反应受损为特征的MDD亚组驱动的,这是 melancholic MDD的一个核心特征。VS激活也观察到类似模式,在情绪反应受损的MDD亚组中同样减弱。FN波幅和VS激活均与DSM定义的完整 melancholic或非典型MDD亚型无关。在整个MDD样本中,FN波幅和VS激活相关,表明不同方法结果具有一致性。这些结果表明,并非所有MDD都以奖赏功能障碍为特征,且MDD内部奖赏处理存在有意义的异质性。本研究提供了神经生物学证据,表明情绪反应受损是MDD亚型分类的关键表型差异,并进一步表明现有的 melancholic表型可能需要进一步细化。