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      Diffusion tensor imaging at 3 hours after traumatic spinal cord injury predicts long-term locomotor recovery.

      Journal of Neurotrauma
      Animals, Diffusion Magnetic Resonance Imaging, methods, Disability Evaluation, Disease Models, Animal, Female, Gait Disorders, Neurologic, etiology, pathology, physiopathology, Hindlimb, innervation, Mice, Mice, Inbred C57BL, Motor Activity, physiology, Nerve Regeneration, Neuronal Plasticity, Paralysis, Predictive Value of Tests, Prognosis, Recovery of Function, Severity of Illness Index, Spinal Cord, Spinal Cord Injuries, Time, Time Factors, Wallerian Degeneration

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          Abstract

          Accurate diagnosis of spinal cord injury (SCI) severity must be achieved before highly aggressive experimental therapies can be tested responsibly in the early phases after trauma. These studies demonstrate for the first time that axial diffusivity (lambda||), derived from diffusion tensor imaging (DTI) within 3 h after SCI, accurately predicts long-term locomotor behavioral recovery in mice. Female C57BL/6 mice underwent sham laminectomy or graded contusive spinal cord injuries at the T9 vertebral level (5 groups, n = 8 for each group). In-vivo DTI examinations were performed immediately after SCI. Longitudinal measurements of hindlimb locomotor recovery were obtained using the Basso mouse scale (BMS). Injured and spared regions of ventrolateral white matter (VLWM) were reliably separated in the hyperacute phase by threshold segmentation. Measurements of lambda|| were compared with histology in the hyperacute phase and 14 days after injury. The spared normal VLWM determined by hyperacute lambda|| and 14-day histology correlated well (r = 0.95). A strong correlation between hindlimb locomotor function recovery and lambda||-determined spared normal VLWM was also observed. The odds of significant locomotor recovery increased by 18% with each 1% increase in normal VLWM measured in the hyperacute phase (odds ratio = 1.18, p = 0.037). The capability of measuring subclinical changes in spinal cord physiology and murine genetic advantages offer an early window into the basic mechanisms of SCI that was not previously possible. Although significant obstacles must still be overcome to derive similar data in human patients, the path to clinical translation is foreseeable and achievable.

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