4.6 Article

Monitoring of brain interstitial total tau and beta amyloid proteins by microdialysis in patients with traumatic brain injury Clinical article

Journal

JOURNAL OF NEUROSURGERY
Volume 110, Issue 6, Pages 1227-1237

Publisher

AMER ASSOC NEUROLOGICAL SURGEONS
DOI: 10.3171/2008.9.JNS08584

Keywords

amyloid beta; diffuse axonal injury; microdialysis; tau protein; traumatic brain injury

Funding

  1. Swedish Research Council
  2. Uppsala University Hospital
  3. Swedish Brain Foundation
  4. Laerdahl Foundation for Acute Medicine

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Object. Damage to axons contributes to postinjury disabilities and is commonly observed following traumatic brain injury (TBI). Traumatic brain injury is ail important environmental risk factor for the development of Alzheimer disease (AD). In the present feasibility study, the aim was to use intracerebral rnicrodialysis catheters with a high molecular Cutoff membrane (100 kD) to harvest interstitial total tau (T-tau) and amyloid beta 1-42 (A beta 42) proteins, which are important biomarkers for axonal injury and for AD, following moderate-to-severe TBI. Methods. Eight patients (5 men and 3 women) were included in the Study; 5 of the patients had a focal/mixed TBI and 3 had a diffuse axonal injury (DAI). Following the bedside analysis of the routinely measured energy metabolic markers (that is, glucose, lactate/pyrilvate ratio, glycerol, and glutaniate), the remaining dialysate was pooled and two 12-hour samples per day were used to analyze T-tau and A beta 42 by enzyme-linked immunosorbent assay from Day 1 up to 8 days postinjury. Results. The results show high levels of interstitial T-tau and A beta 42 postinjury. Patients with a predominantly focal lesion had higher interstitial T-tau levels than in the DAI group from Days 1 to 3 postinjury (p < 0.05). In contrast, patients with DAI had consistently higher A beta 42 levels when compared with patients with focal injury, Conclusions. These results suggest that monitoring of interstitial T-tau and A beta 42 by using microdialysis may be an important tool when evaluating the presence and role of axonal injury following TBI (DOI: 10.3171/2008.9.JNS08584)

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