Background: Brooding is a critical symptom and prognostic factor of major depressive disorder (MDD), which involves passively dwelling on self-referential dysphoria and related abstractions. The neurobiology of brooding remains under characterized. We aimed to elucidate neural dynamics underlying brooding, and explore their responses to neurofeedback intervention in MDD. Methods: We investigated functional MRI (fMRI) dynamic functional network connectivity (dFNC) in 36 MDD subjects and 26 healthy controls (HCs) during rest and brooding. Rest was measured before and after fMRI neurofeedback (MDD-active/sham: n=18/18, HC-active/sham: n=13/13). Baseline brooding severity was recorded using Ruminative Response Scale - Brooding subscale (RRS-B). Results: Four recurrent dFNC states were identified. Measures of time spent were not significantly different between MDD and HC for any of these states during brooding or rest. RRS-B scores in MDD showed significant negative correlation with measures of time spent in dFNC state 3 during brooding (r=-0.5, p= 1.7E-3, FDR-significant). This state comprises strong connections spanning several brain systems involved in sensory, attentional and cognitive processing. Time spent in this anti-brooding dFNC state significantly increased following neurofeedback only in the MDD active group (z=-2.09, p=0.037). Limitations: The sample size was small and imbalanced between groups. Brooding condition was not examined post-neurofeedback. Conclusion: We identified a densely connected anti-brooding dFNC brain state in MDD. MDD subjects spent significantly longer time in this state after active neurofeedback intervention, highlighting neurofeedback`s potential for modulating dysfunctional brain dynamics to treat MDD.

The authors have declared no competing interest.

NCT04941066

This work has been supported in part by the Laureate Institute for Brain Research (LIBR), and the National Institute of General Medical Sciences Center Grant Award Number (2P20GM121312). The content is sole responsibility of the authors and does not necessarily represent the official views of the National Institutes of Health (NIH). SG is supported by Australian Research Training Program (RTP) scholarship and Graeme Clark Institute (GCI) top-up scholarship. AZ is supported by the Rebecca L. Cooper Fellowship.

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