White matter integrity in young medication-naïve bipolar II depressed adults

White matter integrity in young medication-naïve bipolar II depressed adults

It is unknown if young medication-naïve bipolar II (BPII) depressed patients have increased white matter (WM) disruptions. 27 each of young (average 23 years) and treatment-naïve BPII depressed, unipolar depressed (UD) patients and age–sex–education matched healthy controls (HC) underwent 3 T MRIs w...

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Published in:Scientific reports Vol. 11; no. 1; p. 1816
Main Authors: Mak, Arthur Dun Ping, Leung, Owen Ngo Wang, Chou, Idy Wing Yi, Wong, Sheila Lok Yiu, Chu, Winnie Chiu-wing, Yeung, David, So, Suzanne Ho-wai, Ma, Suk Ling, Lam, Linda Chiu Wah, Leung, Chi Ming, Lee, Sing
Format: Journal Article
Language:English
Published: London Nature Publishing Group UK 19-01-2021
Nature Publishing Group
Nature Portfolio
Subjects:
692/699/476/1333
692/699/476/1414
Affective disorders
Discriminant analysis
Humanities and Social Sciences
Longitudinal studies
Magnetic resonance imaging
Mental depression
multidisciplinary
Patients
Principal components analysis
Science
Science (multidisciplinary)
Substantia alba
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Summary:It is unknown if young medication-naïve bipolar II (BPII) depressed patients have increased white matter (WM) disruptions. 27 each of young (average 23 years) and treatment-naïve BPII depressed, unipolar depressed (UD) patients and age–sex–education matched healthy controls (HC) underwent 3 T MRIs with diffusion tensor imaging. Diagnostic ratings included Structured Clinical Interview for DSM Disorders (SCID), Montgomery-Åsberg Depression Rating Scale (MADRS), Young Mania Rating Scale (YMRS) and Hamilton Anxiety Rating Scale (HAM-A). Patients were clinically depressed (MADRS-BPII: 26.15 [SD9.25], UD: 25.56 [5.24], p = 0.86). Compared to UD, BPII had increased family bipolarity (BPII 13.6% vs UD 2.5%, p = 0.01, φc = 0.28), hypomanic symptoms (YMRS-BPII: 4.22 [4.24], UD: 1.33 [2], p = 0.02, d = 0.87), lifetime number of depressive episodes (BPII: 2.37 [1.23], UD: 1.44 [0.75], p = 0.02, d = 0.91), lifetime and current-year number of episodes (lifetime BPII: 50.85 [95.47], UD: 1.7 [1.03]; current-year BPII: 9.93 [16.29], UD: 1.11 [0.32], ps = 0.04, ds = 0.73–0.77) and longer illness duration (BPII: 4.96 years [3.96], UD: 2.99 [3.33], p = 0.15, d = 0.54). BPII showed no increased WM disruptions vs UD or HC in any of the 15 a priori WM tracts. UD had lower right superior longitudinal fasciculus (SLF) (temporal) axial diffusivity (AD) (1.14 vs 1.17 (BPII), 1.16 (HC); F = 6.93, 95% CI of F B : 0.00073, 5.22, ηp 2  = 0.15). Principal component analysis followed by exploratory linear discriminant analysis showed that increased R-SLF (temporal) AD, YMRS and family bipolarity distinguished BPII from UD (81.5% sensitivity, 85.2% specificity) independent of episode number and frequency. Young, medication-naïve adults with BPII depression did not show the WM disruptions distinguishing more chronically ill BP patients from UD. These WM disruptions may therefore be partly attributable to illness chronicity. Longitudinal studies should examine the trajectory of WM changes in BPII and UD and predictive validity of these baseline clinical and imaging parameters.
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ISSN:2045-2322
2045-2322
DOI:10.1038/s41598-021-81355-9