Literature DB >> 21937927

Clinical utility of serum levels of ubiquitin C-terminal hydrolase as a biomarker for severe traumatic brain injury.

Stefania Mondello1, Akinyi Linnet, Andras Buki, Steven Robicsek, Andrea Gabrielli, Joseph Tepas, Linda Papa, Gretchen M Brophy, Frank Tortella, Ronald L Hayes, Kevin K Wang.   

Abstract

BACKGROUND: Brain damage markers released in cerebrospinal fluid (CSF) and blood may provide valuable information about diagnosis and outcome prediction after traumatic brain injury (TBI).
OBJECTIVE: To examine the concentrations of ubiquitin C-terminal hydrolase-L1 (UCH-L1), a novel brain injury biomarker, in CSF and serum of severe TBI patients and their association with clinical characteristics and outcome.
METHODS: This case-control study enrolled 95 severe TBI subjects (Glasgow Coma Scale [GCS] score, 8). Using sensitive UCH-L1 sandwich ELISA, we studied the temporal profile of CSF and serum UCH-L1 levels over 7 days for severe TBI patients.
RESULTS: Comparison of serum and CSF levels of UCH-L1 in TBI patients and control subjects shows a robust and significant elevation of UCH-L1 in the acute phase and over the 7-day study period. Serum and CSF UCH-L1 receiver-operating characteristic curves further confirm strong specificity and selectivity for diagnosing severe TBI vs controls, with area under the curve values in serum and CSF statistically significant at all time points up to 24 hours (P < .001). The first 12-hour levels of both serum and CSF UCH-L1 in patients with GCS score of 3 to 5 were also significantly higher than those with GCS score of 6 to 8. Furthermore, UCH-L1 levels in CSF and serum appear to distinguish severe TBI survivors from nonsurvivors within the study, with nonsurvivors having significantly higher and more persistent levels of serum and CSF UCH-L1. Cumulative serum UCH-L1 levels > 5.22 ng/mL predicted death (odds ratio, 4.8).
CONCLUSION: Serum levels of UCH-L1 appear to have potential clinical utility in diagnosing TBI, including correlating to injury severity and survival outcome.

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Year:  2012        PMID: 21937927      PMCID: PMC3288385          DOI: 10.1227/NEU.0b013e318236a809

Source DB:  PubMed          Journal:  Neurosurgery        ISSN: 0148-396X            Impact factor:   4.654


  42 in total

1.  GFAP and S100B are biomarkers of traumatic brain injury: an observational cohort study.

Authors:  P E Vos; B Jacobs; T M J C Andriessen; K J B Lamers; G F Borm; T Beems; M Edwards; C F Rosmalen; J L M Vissers
Journal:  Neurology       Date:  2010-11-16       Impact factor: 9.910

2.  Ubiquitin C-terminal hydrolase is a novel biomarker in humans for severe traumatic brain injury.

Authors:  Linda Papa; Linnet Akinyi; Ming Cheng Liu; Jose A Pineda; Joseph J Tepas; Monika W Oli; Wenrong Zheng; Gillian Robinson; Steven A Robicsek; Andrea Gabrielli; Shelley C Heaton; H Julia Hannay; Jason A Demery; Gretchen M Brophy; Joe Layon; Claudia S Robertson; Ronald L Hayes; Kevin K W Wang
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3.  Novel differential neuroproteomics analysis of traumatic brain injury in rats.

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4.  Ubiquitin immunoreactivity in cerebrospinal fluid after traumatic brain injury: clinical and experimental findings.

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6.  GFAP versus S100B in serum after traumatic brain injury: relationship to brain damage and outcome.

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7.  Biokinetic analysis of ubiquitin C-terminal hydrolase-L1 (UCH-L1) in severe traumatic brain injury patient biofluids.

Authors:  Gretchen M Brophy; Stefania Mondello; Linda Papa; Steven A Robicsek; Andrea Gabrielli; Joseph Tepas; Andras Buki; Claudia Robertson; Frank C Tortella; Ronald L Hayes; Kevin K W Wang
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10.  Novel Metabolomic Comparison of Arterial and Jugular Venous Blood in Severe Adult Traumatic Brain Injury Patients and the Impact of Pentobarbital Infusion.

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