Early preclinical plasma protein biomarkers of brain trauma are influenced by early seizures and levetiracetam

Author:

Saletti Patricia G.1,Mowrey Wenzhu B.2,Liu Wei1,Li Qianyun1,McCullough Jesse3,Aniceto Roxanne3,Lin I‐Hsuan3,Eklund Michael3,Casillas‐Espinosa Pablo M.456ORCID,Ali Idrish456ORCID,Santana‐Gomez Cesar7ORCID,Coles Lisa8,Shultz Sandy R.456,Jones Nigel456ORCID,Staba Richard7,O'Brien Terence J.456,Moshé Solomon L.191011ORCID,Agoston Denes V.3,Galanopoulou Aristea S.1910ORCID,

Affiliation:

1. Saul R. Korey Department of Neurology, Laboratory of Developmental Epilepsy Albert Einstein College of Medicine Bronx New York USA

2. Department of Epidemiology & Population Health Albert Einstein College of Medicine Bronx New York USA

3. Department of Anatomy, Physiology and Genetics Uniformed Services University Bethesda Maryland USA

4. Department of Neuroscience Monash University Melbourne Victoria Australia

5. Department of Medicine The University of Melbourne Parkville Victoria Australia

6. Department of Neurology Alfred Health Melbourne Victoria Australia

7. Department of Neurology UCLA Los Angeles California USA

8. University of Minnesota Twin Cities Minneapolis Minnesota USA

9. Isabelle Rapin Division of Child Neurology Albert Einstein College of Medicine Bronx New York USA

10. Dominick P Purpura Department of Neuroscience Albert Einstein College of Medicine Bronx New York USA

11. Department of Pediatrics Albert Einstein College of Medicine Bronx New York USA

Abstract

AbstractObjectiveWe used the lateral fluid percussion injury (LFPI) model of moderate‐to‐severe traumatic brain injury (TBI) to identify early plasma biomarkers predicting injury, early post‐traumatic seizures or neuromotor functional recovery (neuroscores), considering the effect of levetiracetam, which is commonly given after severe TBI.MethodsAdult male Sprague–Dawley rats underwent left parietal LFPI, received levetiracetam (200 mg/kg bolus, 200 mg/kg/day subcutaneously for 7 days [7d]) or vehicle post‐LFPI, and were continuously video‐EEG recorded (n = 14/group). Sham (craniotomy only, n = 6), and naïve controls (n = 10) were also used. Neuroscores and plasma collection were done at 2d or 7d post‐LFPI or equivalent timepoints in sham/naïve. Plasma protein biomarker levels were determined by reverse phase protein microarray and classified according to injury severity (LFPI vs. sham/control), levetiracetam treatment, early seizures, and 2d‐to‐7d neuroscore recovery, using machine learning.ResultsLow 2d plasma levels of Thr231‐phosphorylated tau protein (pTAU‐Thr231) and S100B combined (ROC AUC = 0.7790) predicted prior craniotomy surgery (diagnostic biomarker). Levetiracetam‐treated LFPI rats were differentiated from vehicle treated by the 2d‐HMGB1, 2d‐pTAU‐Thr231, and 2d‐UCHL1 plasma levels combined (ROC AUC = 0.9394) (pharmacodynamic biomarker). Levetiracetam prevented the seizure effects on two biomarkers that predicted early seizures only among vehicle‐treated LFPI rats: pTAU‐Thr231 (ROC AUC = 1) and UCHL1 (ROC AUC = 0.8333) (prognostic biomarker of early seizures among vehicle‐treated LFPI rats). Levetiracetam‐resistant early seizures were predicted by high 2d‐IFNγ plasma levels (ROC AUC = 0.8750) (response biomarker). 2d‐to‐7d neuroscore recovery was best predicted by higher 2d‐S100B, lower 2d‐HMGB1, and 2d‐to‐7d increase in HMGB1 or decrease in TNF (P < 0.05) (prognostic biomarkers).SignificanceAntiseizure medications and early seizures need to be considered in the interpretation of early post‐traumatic biomarkers.

Funder

Eunice Kennedy Shriver National Institute of Child Health and Human Development

National Institute of Mental Health

National Institute of Neurological Disorders and Stroke

National Health and Medical Research Council

U.S. Department of Defense

Publisher

Wiley

Subject

Neurology (clinical),Neurology

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