Higuchi’s fractal dimension, but not frontal or posterior alpha asymmetry, predicts PID-5 anxiousness more than depressivity

Higuchi’s fractal dimension, but not frontal or posterior alpha asymmetry, predicts PID-5 anxiousness more than depressivity

Depression is a major cause of health disability. EEG measures may provide one or more economical biomarkers for the diagnosis of depression. Here we compared frontal alpha asymmetry (FAA), posterior alpha asymmetry (PAA), and Higuchi’s fractal dimension (HFD) for their capacity to predict PID-5 dep...

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Bibliographic Details
Published in:Scientific reports Vol. 9; no. 1; pp. 19666 - 7
Main Authors: Kawe, Tame N. J., Shadli, Shabah M., McNaughton, Neil
Format: Journal Article
Language:English
Published: London Nature Publishing Group UK 23-12-2019
Nature Publishing Group
Subjects:
692/53/2421
692/699/476/1300
692/699/476/1414
Adolescent
Adult
Alpha Rhythm
Anxiety
Anxiety - diagnosis
Asymmetry
Depression - diagnosis
EEG
Electroencephalography - statistics & numerical data
Female
Fourier Analysis
Fractals
Humanities and Social Sciences
Humans
Male
Mental depression
multidisciplinary
Personality Inventory - statistics & numerical data
Science
Science (multidisciplinary)
Young Adult
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Summary:Depression is a major cause of health disability. EEG measures may provide one or more economical biomarkers for the diagnosis of depression. Here we compared frontal alpha asymmetry (FAA), posterior alpha asymmetry (PAA), and Higuchi’s fractal dimension (HFD) for their capacity to predict PID-5 depressivity and for the specificity of these predictions relative to PID-5 anxiousness. University students provided 8 or 10 minutes of resting EEG and PID-5 depressivity and PID-5 anxiousness questionnaire scores. FAA and PAA had no significant correlations with the measures at any electrode pair. There were distinct frontal and posterior factors underlying HFD that correlated significantly with anxiousness and with each other. Posterior HFD also correlated significantly with depressivity, though this was weaker than the correlation with anxiousness. The portion of depressivity variance accounted for by posterior HFD was not unique but shared with anxiousness. Inclusion of anxiety disorder patients into the sample rendered the frontal factor somewhat more predictive than the posterior one but generally strengthened the prior conclusions. Contrary to our predictions, none of our measures specifically predicted depressivity. Previous reports of links with depression may involve confounds with concurrent anxiety. Indeed, HFD may be a better measure of anxiety than depression; and its previous linkage to depression may be due to a confound between the two, given the high incidence of depression in cases of severe anxiety.
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ISSN:2045-2322
2045-2322
DOI:10.1038/s41598-019-56229-w