Incremental prognostic value of acute serum biomarkers for functional outcome after traumatic brain injury (CENTER-TBI): an observational cohort study

Helmrich I.R.A.R.; Czeiter E.; Amrein K.Buki A.Lingsma H.F.Menon D.K.Mondello S.Steyerberg E.W.von Steinbuchel N.Wang K.K.W.Wilson L.Xu H.Yang Z.van Klaveren D.Maas A.I.R.

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? 2022 Elsevier LtdBackground: Several studies have reported an association between serum biomarker values and functional outcome following traumatic brain injury. We aimed to examine the incremental (added) prognostic value of serum biomarkers over demographic, clinical, and radiological characteristics and over established prognostic models, such as IMPACT and CRASH, for prediction of functional outcome. Methods: We used data from the Collaborative European NeuroTrauma Effectiveness Research in Traumatic Brain Injury (CENTER-TBI) core study. We included patients aged 14 years or older who had blood sampling within 24 h of injury, results from a CT scan, and outcome assessment according to the Glasgow Outcome Scale-Extended (GOSE) at 6 months. Amounts in serum of six biomarkers (S100 calcium-binding protein B, neuron-specific enolase, glial fibrillary acidic protein, ubiquitin C-terminal hydrolase L1 UCH-L1, neurofilament protein-light, and total tau) were measured. The incremental prognostic value of these biomarkers was determined separately and in combination. The primary outcome was the GOSE 6 months after injury. Incremental prognostic value, using proportional odds and a dichotomised analysis, was assessed by delta C-statistic and delta R2 between models with and without serum biomarkers, corrected for optimism with a bootstrapping procedure. Findings: Serum biomarker values and 6-month GOSE were available for 2283 of 4509 patients. Higher biomarker levels were associated with worse outcome. Adding biomarkers improved the C-statistic by 0·014 (95 CI 0·009–0·020) and R2 by 4·9 (3·6–6·5) for predicting GOSE compared with demographic, clinical, and radiological characteristics. UCH-L1 had the greatest incremental prognostic value. Adding biomarkers to established prognostic models resulted in a relative increase in R2 of 48–65 for IMPACT and 30–34 for CRASH prognostic models. Interpretation: Serum biomarkers have incremental prognostic value for functional outcome after traumatic brain injury. Our findings support integration of biomarkers—particularly UCH-L1—in established prognostic models. Funding: European Union's Seventh Framework Programme, Hannelore Kohl Stiftung, OneMind, Integra LifeSciences, and NeuroTrauma Sciences

机译：?2022 Elsevier Ltd背景：多项研究报告了创伤性脑损伤后血清生物标志物值与功能结果之间的关联。我们旨在研究血清生物标志物在人口统计学、临床和放射学特征以及已建立的预后模型（如IMPACT和CRASH）上对功能结局预测的增量（增加）预后价值。方法：我们使用了来自创伤性脑损伤协作欧洲神经创伤有效性研究（CENTER-TBI）核心研究的数据。我们纳入了14岁或以上的患者，这些患者在受伤后24小时内进行了血液采样，CT扫描结果，以及根据格拉斯哥结果扩展量表（GOSE）在6个月时进行结局评估。测定血清中六种生物标志物（S100 钙结合蛋白 B、神经元特异性烯醇化酶、神经胶质纤维酸性蛋白、泛素 C 末端水解酶 L1 [UCH-L1]、光神经丝蛋白和总 tau）的含量。这些生物标志物的增量预后价值是单独和组合确定的。主要结局是受伤后 6 个月的 GOSE。使用比例比值和二分类分析，通过有和没有血清生物标志物的模型之间的 delta C 统计量和 delta R2 评估增量预后值，并通过自举程序校正乐观情绪。结果：4509 例患者中有 2283 例的血清生物标志物值和 6 个月 GOSE 可用。较高的生物标志物水平与较差的结局相关。与人口统计学、临床和放射学特征相比，添加生物标志物将预测GOSE的C统计量提高了0.014（95%CI 0.009-0.020），R2提高了4.9%（3.6-6.5）。UCH-L1的增量预后价值最大。在已建立的预后模型中添加生物标志物导致 IMPACT 的 R2 相对增加 48-65%，CRASH 预后模型的 R2 相对增加 30-34%。解读：血清生物标志物对创伤性脑损伤后功能结局具有增量预后价值。我们的研究结果支持将生物标志物（尤其是UCH-L1）整合到已建立的预后模型中。资金来源：欧盟第七框架计划、Hannelore Kohl Stiftung、OneMind、Integra LifeSciences 和 NeuroTrauma Sciences

Incremental prognostic value of acute serum biomarkers for functional outcome after traumatic brain injury (CENTER-TBI): an observational cohort study

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