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Electrophysiological Brain Responses as Neural Markers of Depression and Aging

Year of publication

2020

Authors

Ruohonen, Elisa

Abstract

Depression is one of the most common mental disorders. Currently, the diagnosis of depression is based on a clinical interview, and no reliable objective depression biomarkers have been recognized. Brain’s event-related potentials (ERPs) could potentially be used as neural markers for diagnosing and planning treatment options for depression. ERPs could also potentially be used to differentiate depression-related alterations from aging-related alterations. In study I, ERPs to sound intensity changes were compared between first-episode and recurrent depression groups and non-depressed controls. Larger brain responses (N1 response) to rare sounds were found in the first-episode depression group, compared to the other groups. Sound intensity processing has been suggested to reflect monoaminergic neurotransmission and therefore the enlarged responses can reflect monoaminergic deficits. In study II, ERPs to sound intensity changes were compared between younger and older depressed adults and age-matched non-depressed adults. Augmented N1 responses were found in both older adults and depressed adults, indicating similar effects for aging and depression on intensity processing. The augmentation could index an inability to suppress activity in response to irrelevant stimuli (also called sensory gating). In study III, ERPs to emotional facial expressions were compared between depressed and non-depressed groups. In addition, changes in the brain responses were investigated by conducting follow-up measurements after 2 and 39 months. It was also investigated whether the baseline brain responses were associated with later response to a brief psychological intervention. Larger P1 responses to sad faces, compared to neutral faces, were found in the depressed group, indicating a negative bias in the automatic processing of facial expressions. The bias was corrected in the follow-up measurements after symptom reduction. Compared to the non-depressed control group, a larger negative bias was found in the group that did not recover after the intervention. However, the recovered and nonrecovered groups did not differ in brain responses. The results of this thesis indicate that electrical brain responses related to early information processing can be used to study depression- and aging-related alterations in brain function and the brain responses can reflect illness state. Therefore, these responses have the potential to be further developed for clinical practice as neural markers for depression.
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Organizations and authors

Publication type

Publication format

Monograph

Audience

Scientific

MINEDU's publication type classification code

G5 Doctoral dissertation (articles)

Publication channel information

Journal

JYU Dissertations

Publisher

Jyväskylän yliopisto

Open access

Open access in the publisher’s service

Yes

Open access of publication channel

Fully open publication channel

Self-archived

No

Other information

Fields of science

Psychology

Keywords

[object Object],[object Object],[object Object]

Publication country

Finland

Internationality of the publisher

Domestic

Language

English

International co-publication

No

Co-publication with a company

No

The publication is included in the Ministry of Education and Culture’s Publication data collection

Yes