4.5 Article

An fMRI study of cognitive reappraisal in major depressive disorder and borderline personality disorder

Journal

EUROPEAN PSYCHIATRY
Volume 64, Issue 1, Pages -

Publisher

CAMBRIDGE UNIV PRESS
DOI: 10.1192/j.eurpsy.2021.2231

Keywords

Borderline personality disorder; emotion regulation; fMRI; major depressive disorder; neuroimaging

Categories

Funding

  1. research and innovation program under the Marie Sklowdowska Curie [714673]
  2. Fundacion Bancaria la Caixa
  3. European Regional Development Fund-ERDF
  4. Departament de Salut, Generalitat de Catalunya [PERIS SLT006/17/249]
  5. Agencia de Gestio d'Ajuts Universitaris i de Recerca [2017 SGR 1247]
  6. Agencia Nacional de Promocion de la Investigacion, el Desarrollo Tecnologico y la Innovacion [PICT-2019-02328]
  7. la Caixa Foundation [100010434, LCF/BQ/IN17/11620071]
  8. University of Melbourne McKenzie Fellowship
  9. NHMRC/Medical Research Future Fund (MRFF) [MRF1193736]
  10. Carlos III health Institute [FI17/00294]
  11. Health Department of the Generalitat de Catalunya [SLT002/16/00237]
  12. [PI16/00889]
  13. [PI19/01171]

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This study identified a shared neurobiological contributor to emotion regulation deficits in MDD and BPD characterized by decreased vlPFC activity, while also observing disorder-specific alterations. In MDD, there is a primary deficit in prefrontal activations, while BPD is defined by connectivity disruptions between the vlPFC and temporal emotion processing regions. These findings substantiate the different profiles of emotion regulation alterations observed in these disorders in neurobiological terms.
Background One common denominator to the clinical phenotypes of borderline personality disorder (BPD) and major depressive disorder (MDD) is emotion regulation impairment. Although these two conditions have been extensively studied separately, it remains unclear whether their emotion regulation impairments are underpinned by shared or distinct neurobiological alterations. Methods We contrasted the neural correlates of negative emotion regulation across an adult sample of BPD patients (n = 19), MDD patients (n = 20), and healthy controls (HCs; n = 19). Emotion regulation was assessed using an established functional magnetic resonance imaging cognitive reappraisal paradigm. We assessed both task-related activations and modulations of interregional connectivity. Results When compared to HCs, patients with BPD and MDD displayed homologous decreased activation in the right ventrolateral prefrontal cortex (vlPFC) during cognitive reappraisal. In addition, the MDD group presented decreased activations in other prefrontal areas (i.e., left dorsolateral and bilateral orbitofrontal cortices), while the BPD group was characterized by a more extended pattern of alteration in the connectivity between the vlPFC and cortices of the visual ventral stream during reappraisal. Conclusions This study identified, for the first time, a shared neurobiological contributor to emotion regulation deficits in MDD and BPD characterized by decreased vlPFC activity, although we also observed disorder-specific alterations. In MDD, results suggest a primary deficit in the strength of prefrontal activations, while BPD is better defined by connectivity disruptions between the vlPFC and temporal emotion processing regions. These findings substantiate, in neurobiological terms, the different profiles of emotion regulation alterations observed in these disorders.

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