Respond to Neuropsychological Outcome in Chronic Tbi Participants

نویسندگان

  • Ava Puccio
  • Milos Ikonomovic
  • Sue Beers
  • Kathryn Edelman
  • Steven Benso
  • Yuefang Chang
  • Walter Schneider
  • James Mountz
  • David Okonkwo
  • Prerna Ranganathan
  • Raj Kumar
  • Amy Wagner
چکیده

Objectives: Traumatic brain injury (TBI) involves axonal injury and accumulation of pathological protein aggregates including amyloid-b (Ab) and hyperphosphorylated tau (p-tau). Biomarker analysis of tau and Ab concentrations in cerebrospinal fluid (CSF) may be an objective marker of cognitive status after TBI. The goal of the current study was to analyze tau and Ab 40–42 in a cohort of military and civilian participants with chronic deficits secondary to TBI, and correlate neuropsychological outcome data with concentrations of tau and Ab42 measured in CSF from the same subjects. Methods: 19 chronic TBI participants ( > 6 months from injury; 16 males, mean age 41yrs, 8 military veterans and 11 civilians) underwent lumbar puncture as well as neuropsychological testing. CSF was analyzed for concentrations of total tau, Ab1-42 (Ab42) and Ab1-40 (Ab40) by ELISA, and tau/Ab42 ratio was calculated. The neuropsychological test battery included measures of memory, processing speed and executive function: California Verbal Learning Test-II (CVLT) Short and Long Delay Free Recall (SDFR, LDFR), Wechsler Adult Intelligence Scale Working Memory Index (WAIS IV) and Trail Making Test Part A/B. Nonparametric correlation (Spearman rho, q) was used to relate CSF levels to neuropsychological data, controlling for age. Results: CSF tau/Ab42 ratio was inversely associated with Trails B (Spearman p > -0.49, p< 0.047). CSF Ab40 concentration was inversely correlated with CVLT SDFR and LDFR (Spearman p > -0.51, p < 0.032; p > -0.50, p< 0.034, respectively). There were no significant correlations between CSF biomarker levels and WAIS neuropsychological measures. Conclusions: In chronic TBI, neuropsychological outcome on measures of memory and executive function (CVLT and Trails B) corresponded to CSF biomarkers of tau and Ab concentrations. Additional studies with a larger cohort of TBI participants are needed to draw meaningful conclusions. The use of CSF biomarkers in ongoing studies will allow us to test more specific hypotheses regarding the link between TBI and chronic neurodegenerative conditions such as chronic traumatic encephalopathy.

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تاریخ انتشار 2017