4.4 Article

Older age, male sex, and cerebral microbleeds predict white matter loss after traumatic brain injury

Journal

GEROSCIENCE
Volume 44, Issue 1, Pages 83-102

Publisher

SPRINGER
DOI: 10.1007/s11357-021-00459-2

Keywords

Diffusion tensor imaging; Fractional anisotropy; Susceptibility-weighted imaging; Sensory integration; Executive function

Funding

  1. National Institutes of Health [R01 NS 100973]
  2. Department of Defense [W81-XWH-1810413]
  3. James J. and Sue Femino Foundation
  4. Hanson-Thorell Research Scholarship
  5. Undergraduate Research Associate Program (URAP) at the University of Southern California
  6. Center for Undergraduate Research in Viterbi Engineering (CURVE) at the University of Southern California
  7. National Institute of Biomedical Imaging and Bioengineering [P41 EB 015902, P41 EB 015898, P41 EB 028741]
  8. National Institute of Mental Health [R01 MH 074794, R01 MH 125860, R01 MH 119222]
  9. National Institutes of Health

Ask authors/readers for more resources

Age is linearly associated with white matter degradation, likely not only due to injury but also to cumulative effects of other pathologies and their interactions with injury. As time passes, the degradation of brain white matter will result in age-dependent deficits in information processing speed, interhemispheric communication, motor coordination, visual acuity, sensory integration, reading speed/comprehension, executive function, personality, and memory.
Little is known on how mild traumatic brain injury affects white matter based on age at injury, sex, cerebral microbleeds, and time since injury. Here, we study the fractional anisotropy of white matter to study these effects in 109 participants aged 18-77 (46 females, age mu +/- sigma = 40 +/- 17 years) imaged within similar to 1 week and similar to 6 months post-injury. Age is found to be linearly associated with white matter degradation, likely due not only to injury but also to cumulative effects of other pathologies and to their interactions with injury. Age is associated with mean anisotropy decreases in the corpus callosum, middle longitudinal fasciculi, inferior longitudinal and occipitofrontal fasciculi, and superficial frontal and temporal fasciculi. Over similar to 6 months, the mean anisotropies of the corpus callosum, left superficial frontal fasciculi, and left corticospinal tract decrease significantly. Independently of other predictors, age and cerebral microbleeds contribute to anisotropy decrease in the callosal genu. Chronically, the white matter of commissural tracts, left superficial frontal fasciculi, and left corticospinal tract degrade appreciably, independently of other predictors. Our findings suggest that large commissural and intra-hemispheric structures are at high risk for post-traumatic degradation. This study identifies detailed neuroanatomic substrates consistent with brain injury patients' age-dependent deficits in information processing speed, interhemispheric communication, motor coordination, visual acuity, sensory integration, reading speed/comprehension, executive function, personality, and memory. We also identify neuroanatomic features underlying white matter degradation whose severity is associated with the male sex. Future studies should compare our findings to functional measures and other neurodegenerative processes.

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