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      Association of Heavy Drinking With Deviant Fiber Tract Development in Frontal Brain Systems in Adolescents

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          Most cited references49

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          Brain development during childhood and adolescence: a longitudinal MRI study.

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            Diffusion tensor imaging of the brain.

            Diffusion tensor imaging (DTI) is a promising method for characterizing microstructural changes or differences with neuropathology and treatment. The diffusion tensor may be used to characterize the magnitude, the degree of anisotropy, and the orientation of directional diffusion. This review addresses the biological mechanisms, acquisition, and analysis of DTI measurements. The relationships between DTI measures and white matter pathologic features (e.g., ischemia, myelination, axonal damage, inflammation, and edema) are summarized. Applications of DTI to tissue characterization in neurotherapeutic applications are reviewed. The interpretations of common DTI measures (mean diffusivity, MD; fractional anisotropy, FA; radial diffusivity, D(r); and axial diffusivity, D(a)) are discussed. In particular, FA is highly sensitive to microstructural changes, but not very specific to the type of changes (e.g., radial or axial). To maximize the specificity and better characterize the tissue microstructure, future studies should use multiple diffusion tensor measures (e.g., MD and FA, or D(a) and D(r)).
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              Microstructural maturation of the human brain from childhood to adulthood.

              Brain maturation is a complex process that continues well beyond infancy, and adolescence is thought to be a key period of brain rewiring. To assess structural brain maturation from childhood to adulthood, we charted brain development in subjects aged 5 to 30 years using diffusion tensor magnetic resonance imaging, a novel brain imaging technique that is sensitive to axonal packing and myelination and is particularly adept at virtually extracting white matter connections. Age-related changes were seen in major white matter tracts, deep gray matter, and subcortical white matter, in our large (n=202), age-distributed sample. These diffusion changes followed an exponential pattern of maturation with considerable regional variation. Differences observed in developmental timing suggest a pattern of maturation in which areas with fronto-temporal connections develop more slowly than other regions. These in vivo results expand upon previous postmortem and imaging studies and provide quantitative measures indicative of the progression and magnitude of regional human brain maturation.
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                Author and article information

                Journal
                JAMA Psychiatry
                JAMA Psychiatry
                American Medical Association (AMA)
                2168-622X
                December 30 2020
                Affiliations
                [1 ]Department of Psychiatry & Behavioral Sciences, Stanford University School of Medicine, Stanford, California
                [2 ]Center for Health Sciences, SRI International, Menlo Park, California
                [3 ]Department of Psychiatry & Behavioral Sciences, Duke University, Durham, North Carolina
                [4 ]Department of Radiology, Duke University, Durham, North Carolina
                [5 ]Department of Psychology, University of North Carolina, Wilmington
                [6 ]Department of Psychiatry, University of California San Diego, La Jolla
                [7 ]Department of Psychology, University of California San Diego, La Jolla
                [8 ]Division of Biostatistics, Department of Family Medicine and Public Health, University of California San Diego, La Jolla
                [9 ]Departments of Psychiatry and Behavioral Neuroscience, Oregon Health & Sciences University, Portland
                [10 ]Department of Psychiatry, University of Pittsburgh, Pittsburgh, Pennsylvania
                Article
                10.1001/jamapsychiatry.2020.4064
                33377940
                c9994a1a-b913-4055-bc03-b5d688078452
                © 2020
                History

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