Abstracts

Two distinct cohorts of mice were used. In the first cohort, adult CD1 male mice underwent sham surgery (n=15) or TBI (n=30) by controlled cortical impact (CCI). Longitudinal in vivo proton magnetic resonance spectroscopy (¹H-MRS) was performed in the thalamus ipsilateral to the injured cortex before (3 weeks, w) and after (3 months, m) PTE onset. At 5 m, diffusion tensor imaging (DTI) and 3D structural MRI was done. Then, mice were ECoG-monitored to assess PTE development, and sacrificed for astrocyte-based histopathology. In the second cohort, TBI mice (n=21) were ECoG-monitored during the first week after CCI and stratified as high- or low-risk to develop PTE based on a previously validated ECoG signature (i.e., daily number of spikes/sharp waves in the contralateral hemisphere). TBI and sham mice (n=5) were then sacrificed at 3w for GFAP expression analysis.