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      Longitudinal Development of Human Brain Wiring Continues from Childhood into Adulthood

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      The Journal of Neuroscience
      Society for Neuroscience

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          Abstract

          Healthy human brain development is a complex process that continues during childhood and adolescence, as demonstrated by many cross-sectional and several longitudinal studies. However, whether these changes end in adolescence is not clear. We examined longitudinal white matter maturation using diffusion tensor tractography in 103 healthy subjects aged 5–32 years; each volunteer was scanned at least twice, with 221 total scans. Fractional anisotropy (FA) and mean diffusivity (MD), parameters indicative of factors including myelination and axon density, were assessed in 10 major white matter tracts. All tracts showed significant nonlinear development trajectories for FA and MD. Significant within-subject changes occurred in the vast majority of children and early adolescents, and these changes were mostly complete by late adolescence for projection and commissural tracts. However, association tracts demonstrated postadolescent within-subject maturation of both FA and MD. Diffusion parameter changes were due primarily to decreasing perpendicular diffusivity, although increasing parallel diffusivity contributed to the prolonged increases of FA in association tracts. Volume increased significantly with age for most tracts, and longitudinal measures also demonstrated postadolescent volume increases in several association tracts. As volume increases were not directly associated with either elevated FA or reduced MD between scans, the observed diffusion parameter changes likely reflect microstructural maturation of brain white matter tracts rather than just gross anatomy.

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          Author and article information

          Journal
          J Neurosci
          J. Neurosci
          jneuro
          jneurosci
          J. Neurosci
          The Journal of Neuroscience
          Society for Neuroscience
          0270-6474
          1529-2401
          27 July 2011
          : 31
          : 30
          : 10937-10947
          Affiliations
          [1]Department of Biomedical Engineering, University of Alberta, Edmonton, Alberta T6G 2V2, Canada
          Author notes
          Correspondence should be addressed to Dr. Christian Beaulieu, Department of Biomedical Engineering, Faculty of Medicine and Dentistry, Room 1098, Research Transition Facility, University of Alberta, Edmonton, AB T6G 2V2, Canada. christian.beaulieu@ 123456ualberta.ca

          Author contributions: C.L. and C.B. designed research; C.L. and C.B. performed research; C.L. and C.B. analyzed data; C.L. and C.B. wrote the paper.

          Article
          PMC6623097 PMC6623097 6623097 3712424
          10.1523/JNEUROSCI.5302-10.2011
          6623097
          21795544
          88ec3527-d128-4503-b95c-f860919a81d9
          Copyright © 2011 the authors 0270-6474/11/3110937-11$15.00/0
          History
          : 8 October 2010
          : 29 May 2011
          : 8 June 2011
          Categories
          Articles
          Development/Plasticity/Repair

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