The longitudinal biochemical profiling of TBI in a drop weight model of TBI

Ali Yilmaz; Sigal Liraz-Zaltsman; Esther Shohami; Juozas Gordevičius; Ieva Kerševičiūtė; Eric Sherman; Ray O Bahado-Singh; Stewart F Graham

doi:10.1038/s41598-023-48539-x

The longitudinal biochemical profiling of TBI in a drop weight model of TBI

Sci Rep. 2023 Dec 14;13(1):22260. doi: 10.1038/s41598-023-48539-x.

Authors

Ali Yilmaz^{1

2}, Sigal Liraz-Zaltsman^{3

4

5}, Esther Shohami³, Juozas Gordevičius⁶, Ieva Kerševičiūtė⁶, Eric Sherman⁷, Ray O Bahado-Singh², Stewart F Graham^{8

9}

Affiliations

¹ Metabolomics Department, Beaumont Research Institute, Beaumont Health, Royal Oak, MI, 48073, USA.
² Oakland University-William Beaumont School of Medicine, Rochester, MI, 48073, USA.
³ Department of Pharmacology, The Institute for Drug Research, The Hebrew University of Jerusalem, Jerusalem, Israel.
⁴ The Joseph Sagol Neuroscience Center, Sheba Medical Center, Ramat-Gan, Israel.
⁵ Department of Sports Therapy, Institute for Health and Medical Professions, Ono Academic College, Qiryat Ono, Israel.
⁶ VUGENE LLC, 625 EKenmoor Avenue Southeast, Suite 301, PMB 96578, Grand Rapids, MI, 49546, USA.
⁷ Wayne State University School of Medicine, Detroit, MI, 48202, USA.
⁸ Metabolomics Department, Beaumont Research Institute, Beaumont Health, Royal Oak, MI, 48073, USA. stewart.graham@beaumont.edu.
⁹ Oakland University-William Beaumont School of Medicine, Rochester, MI, 48073, USA. stewart.graham@beaumont.edu.

Abstract

Traumatic brain injury (TBI) is a major cause of mortality and disability worldwide, particularly among individuals under the age of 45. It is a complex, and heterogeneous disease with a multifaceted pathophysiology that remains to be elucidated. Metabolomics has the potential to identify metabolic pathways and unique biochemical profiles associated with TBI. Herein, we employed a longitudinal metabolomics approach to study TBI in a weight drop mouse model to reveal metabolic changes associated with TBI pathogenesis, severity, and secondary injury. Using proton nuclear magnetic resonance (¹H NMR) spectroscopy, we biochemically profiled post-mortem brain from mice that suffered mild TBI (N = 25; 13 male and 12 female), severe TBI (N = 24; 11 male and 13 female) and sham controls (N = 16; 11 male and 5 female) at baseline, day 1 and day 7 following the injury. ¹H NMR-based metabolomics, in combination with bioinformatic analyses, highlights a few significant metabolites associated with TBI severity and perturbed metabolism related to the injury. We report that the concentrations of taurine, creatinine, adenine, dimethylamine, histidine, N-Acetyl aspartate, and glucose 1-phosphate are all associated with TBI severity. Longitudinal metabolic observation of brain tissue revealed that mild TBI and severe TBI lead distinct metabolic profile changes. A multi-class model was able to classify the severity of injury as well as time after TBI with estimated 86% accuracy. Further, we identified a high degree of correlation between respective hemisphere metabolic profiles (r > 0.84, p < 0.05, Pearson correlation). This study highlights the metabolic changes associated with underlying TBI severity and secondary injury. While comprehensive, future studies should investigate whether: (a) the biochemical pathways highlighted here are recapitulated in the brain of TBI sufferers and (b) if the panel of biomarkers are also as effective in less invasively harvested biomatrices, for objective and rapid identification of TBI severity and prognosis.

MeSH terms

Animals
Brain / metabolism
Brain Concussion* / complications
Brain Injuries, Traumatic* / metabolism
Female
Male
Metabolome
Metabolomics / methods
Mice
Prognosis