Blood biomarkers for mild traumatic brain injury: a selective review of unresolved issues
Abstract Background The use of blood biomarkers after mild traumatic brain injury (mTBI) has been widely studied. We have identified eight unresolved issues related to the use of five commonly investigated blood biomarkers: neurofilament light chain, ubiquitin carboxy-terminal hydrolase-L1, tau, S10...
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2021-09-01
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| Series: | Biomarker Research |
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| Online Access: | https://doi.org/10.1186/s40364-021-00325-5 |
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doaj-c5c8659cb7d449df818596860ad3dae72021-09-19T11:11:44ZengBMCBiomarker Research2050-77712021-09-019111710.1186/s40364-021-00325-5Blood biomarkers for mild traumatic brain injury: a selective review of unresolved issuesDaniel B. Hier0Tayo Obafemi-Ajayi1Matthew S. Thimgan2Gayla R. Olbricht3Sima Azizi4Blaine Allen5Bassam A. Hadi6Donald C. Wunsch7Department of Electrical and Computer Engineering, Missouri University of Science and TechnologyCooperative Engineering Program, Missouri State UniversityDepartment of Biological Sciences, Missouri University of Science and TechnologyDepartment of Mathematics and Statistics, Missouri University of Science and TechnologyDepartment of Electrical and Computer Engineering, Missouri University of Science and TechnologyDepartment of Electrical and Computer Engineering, Missouri University of Science and TechnologyDepartment of Surgery, Mercy Hospital, St. Louis MODepartment of Electrical and Computer Engineering, Missouri University of Science and TechnologyAbstract Background The use of blood biomarkers after mild traumatic brain injury (mTBI) has been widely studied. We have identified eight unresolved issues related to the use of five commonly investigated blood biomarkers: neurofilament light chain, ubiquitin carboxy-terminal hydrolase-L1, tau, S100B, and glial acidic fibrillary protein. We conducted a focused literature review of unresolved issues in three areas: mode of entry into and exit from the blood, kinetics of blood biomarkers in the blood, and predictive capacity of the blood biomarkers after mTBI. Findings Although a disruption of the blood brain barrier has been demonstrated in mild and severe traumatic brain injury, biomarkers can enter the blood through pathways that do not require a breach in this barrier. A definitive accounting for the pathways that biomarkers follow from the brain to the blood after mTBI has not been performed. Although preliminary investigations of blood biomarkers kinetics after TBI are available, our current knowledge is incomplete and definitive studies are needed. Optimal sampling times for biomarkers after mTBI have not been established. Kinetic models of blood biomarkers can be informative, but more precise estimates of kinetic parameters are needed. Confounding factors for blood biomarker levels have been identified, but corrections for these factors are not routinely made. Little evidence has emerged to date to suggest that blood biomarker levels correlate with clinical measures of mTBI severity. The significance of elevated biomarker levels thirty or more days following mTBI is uncertain. Blood biomarkers have shown a modest but not definitive ability to distinguish concussed from non-concussed subjects, to detect sub-concussive hits to the head, and to predict recovery from mTBI. Blood biomarkers have performed best at distinguishing CT scan positive from CT scan negative subjects after mTBI.https://doi.org/10.1186/s40364-021-00325-5NF-LUCH-L1GFAPMild traumatic brain injuryKineticsS100B |
| collection |
DOAJ |
| language |
English |
| format |
Article |
| sources |
DOAJ |
| author |
Daniel B. Hier Tayo Obafemi-Ajayi Matthew S. Thimgan Gayla R. Olbricht Sima Azizi Blaine Allen Bassam A. Hadi Donald C. Wunsch |
| spellingShingle |
Daniel B. Hier Tayo Obafemi-Ajayi Matthew S. Thimgan Gayla R. Olbricht Sima Azizi Blaine Allen Bassam A. Hadi Donald C. Wunsch Blood biomarkers for mild traumatic brain injury: a selective review of unresolved issues Biomarker Research NF-L UCH-L1 GFAP Mild traumatic brain injury Kinetics S100B |
| author_facet |
Daniel B. Hier Tayo Obafemi-Ajayi Matthew S. Thimgan Gayla R. Olbricht Sima Azizi Blaine Allen Bassam A. Hadi Donald C. Wunsch |
| author_sort |
Daniel B. Hier |
| title |
Blood biomarkers for mild traumatic brain injury: a selective review of unresolved issues |
| title_short |
Blood biomarkers for mild traumatic brain injury: a selective review of unresolved issues |
| title_full |
Blood biomarkers for mild traumatic brain injury: a selective review of unresolved issues |
| title_fullStr |
Blood biomarkers for mild traumatic brain injury: a selective review of unresolved issues |
| title_full_unstemmed |
Blood biomarkers for mild traumatic brain injury: a selective review of unresolved issues |
| title_sort |
blood biomarkers for mild traumatic brain injury: a selective review of unresolved issues |
| publisher |
BMC |
| series |
Biomarker Research |
| issn |
2050-7771 |
| publishDate |
2021-09-01 |
| description |
Abstract Background The use of blood biomarkers after mild traumatic brain injury (mTBI) has been widely studied. We have identified eight unresolved issues related to the use of five commonly investigated blood biomarkers: neurofilament light chain, ubiquitin carboxy-terminal hydrolase-L1, tau, S100B, and glial acidic fibrillary protein. We conducted a focused literature review of unresolved issues in three areas: mode of entry into and exit from the blood, kinetics of blood biomarkers in the blood, and predictive capacity of the blood biomarkers after mTBI. Findings Although a disruption of the blood brain barrier has been demonstrated in mild and severe traumatic brain injury, biomarkers can enter the blood through pathways that do not require a breach in this barrier. A definitive accounting for the pathways that biomarkers follow from the brain to the blood after mTBI has not been performed. Although preliminary investigations of blood biomarkers kinetics after TBI are available, our current knowledge is incomplete and definitive studies are needed. Optimal sampling times for biomarkers after mTBI have not been established. Kinetic models of blood biomarkers can be informative, but more precise estimates of kinetic parameters are needed. Confounding factors for blood biomarker levels have been identified, but corrections for these factors are not routinely made. Little evidence has emerged to date to suggest that blood biomarker levels correlate with clinical measures of mTBI severity. The significance of elevated biomarker levels thirty or more days following mTBI is uncertain. Blood biomarkers have shown a modest but not definitive ability to distinguish concussed from non-concussed subjects, to detect sub-concussive hits to the head, and to predict recovery from mTBI. Blood biomarkers have performed best at distinguishing CT scan positive from CT scan negative subjects after mTBI. |
| topic |
NF-L UCH-L1 GFAP Mild traumatic brain injury Kinetics S100B |
| url |
https://doi.org/10.1186/s40364-021-00325-5 |
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