Resting-state functional connectivity in anxiety disorders: a multicenter fMRI study

眶额皮质 神经科学 静息状态功能磁共振成像 心理学 脑岛 丘脑 扁桃形结构 导水管周围灰质 前额叶皮质 扣带回前部 默认模式网络 功能磁共振成像 惊恐障碍 焦虑 精神科 中脑 中枢神经系统 认知
作者
Till Langhammer,Kevin Hilbert,Dirk Adolph,Volker Arolt,Sophie Bischoff,Joscha Böhnlein,Jan Christopher Cwik,Udo Dannlowski,Jürgen Deckert,Katharina Domschke,Ricarda Evens,Thomas Fydrich,Bettina Gathmann,Alfons O. Hamm,Ingmar Heinig,Martin J. Herrmann,Maike Hollandt,Markus Junghoefer,Tilo Kircher,Katja Koelkebeck
出处
期刊:Molecular Psychiatry [Springer Nature]
卷期号:30 (4): 1548-1557 被引量:12
标识
DOI:10.1038/s41380-024-02768-2
摘要

Abstract Anxiety disorders (AD) are associated with altered connectivity in large-scale intrinsic brain networks. It remains uncertain how much these signatures overlap across different phenotypes due to a lack of well-powered cross-disorder comparisons. We used resting-state functional magnetic resonance imaging (rsfMRI) to investigate differences in functional connectivity (FC) in a cross-disorder sample of AD patients and healthy controls (HC). Before treatment, 439 patients from two German multicenter clinical trials at eight different sites fulfilling a primary diagnosis of panic disorder and/or agoraphobia (PD/AG, N = 154), social anxiety disorder (SAD, N = 95), or specific phobia (SP, N = 190) and 105 HC underwent an 8 min rsfMRI assessment. We performed categorical and dimensional regions of interest (ROI)-to-ROI analyses focusing on connectivity between regions of the defensive system and prefrontal regulation areas. AD patients showed increased connectivity between the insula and the thalamus compared to controls. This was mainly driven by PD/AG patients who showed increased (insula/hippocampus/amygdala—thalamus) and decreased (dorsomedial prefrontal cortex/periaqueductal gray—anterior cingulate cortex) positive connectivity between subcortical and cortical areas. In contrast, SAD patients showed decreased negative connectivity exclusively in cortical areas (insula—orbitofrontal cortex), whereas no differences were found in SP patients. State anxiety associated with the scanner environment did not explain the FC between these regions. Only PD/AG patients showed pronounced connectivity changes along a widespread subcortical-cortical network, including the midbrain. Dimensional analyses yielded no significant results. The results highlighting categorical differences between ADs at a systems neuroscience level are discussed within the context of personalized neuroscience-informed treatments. PROTECT-AD’s registration at NIMH Protocol Registration System: 01EE1402A and German Register of Clinical Studies: DRKS00008743. SpiderVR’s registration at ClinicalTrials.gov: NCT03208400.
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