White matter tract myelin maturation and its association with general psychopathology in adolescence and early adulthood

Adolescence is a time period associated with marked brain maturation that coincides with an enhanced risk for onset of psychiatric disorder. White matter tract myelination, a process that continues to unfold throughout adolescence, is reported to be abnormal in several psychiatric disorders. Here, w...

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Bibliographic Details
Published in:Human brain mapping 2020-02, Vol.41 (3), p.827-839
Main Authors: Vanes, Lucy D., Moutoussis, Michael, Ziegler, Gabriel, Goodyer, Ian M., Fonagy, Peter, Jones, Peter B., Bullmore, Edward T., Dolan, Raymond J.
Format: Article
Language:English
Subjects:
Adolescence
Adolescent
Adolescents
Adult
Brain
Child development
Cingulum
Deceleration
Female
general psychopathology
Hippocampus
Human Development - physiology
Humans
Longitudinal Studies
Magnetic Resonance Imaging
Magnetization
Male
Markers
Maturation
Mental disorders
Mental Disorders - physiopathology
Mental illness
Myelin
Myelin Sheath
Myelination
Neural Pathways - diagnostic imaging
Neural Pathways - growth & development
Neuroimaging
Psychological aspects
Psychology, Pathological
Psychopathology
Radiation
structural connectivity
Substantia alba
Thalamus
Trajectory analysis
uncinate fasciculus
White Matter - diagnostic imaging
White Matter - growth & development
Young Adult
Young adults
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Summary:Adolescence is a time period associated with marked brain maturation that coincides with an enhanced risk for onset of psychiatric disorder. White matter tract myelination, a process that continues to unfold throughout adolescence, is reported to be abnormal in several psychiatric disorders. Here, we ask whether psychiatric vulnerability is linked to aberrant developmental myelination trajectories. We assessed a marker of myelin maturation, using magnetisation transfer (MT) imaging, in 10 major white matter tracts. We then investigated its relationship to the expression of a general psychopathology “p‐factor” in a longitudinal analysis of 293 healthy participants between the ages of 14 and 24. We observed significant longitudinal MT increase across the full age spectrum in anterior thalamic radiation, hippocampal cingulum, dorsal cingulum and superior longitudinal fasciculus. MT increase in the inferior fronto‐occipital fasciculus, inferior longitudinal fasciculus and uncinate fasciculus was pronounced in younger participants but levelled off during the transition into young adulthood. Crucially, longitudinal MT increase in dorsal cingulum and uncinate fasciculus decelerated as a function of mean p‐factor scores over the study period. This suggests that an increased expression of psychopathology is closely linked to lower rates of myelin maturation in selective brain tracts over time. Impaired myelin growth in limbic association fibres may serve as a neural marker for emerging mental illness during the course of adolescence and early adulthood.
ISSN:1065-9471
1097-0193
DOI:10.1002/hbm.24842