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利用血清氨基酸预测创伤性脑损伤:一种利用多种生物标志物的系统方法。

Using Serum Amino Acids to Predict Traumatic Brain Injury: A Systematic Approach to Utilize Multiple Biomarkers.

机构信息

Wallace H. Coulter Department of Biomedical Engineering, Georgia Institute of Technology and Emory University, Atlanta, GA 30322, USA.

Perelman School of Medicine, University of Pennsylvania, Philadelphia, PA 19104, USA.

出版信息

Int J Mol Sci. 2020 Mar 5;21(5):1786. doi: 10.3390/ijms21051786.

Abstract

Traumatic brain injury (TBI) can cause biochemical and metabolomic alterations in the brain tissue and serum. These alterations can be used for diagnosis and prognosis of TBI. Here, the serum concentrations of seventeen amino acids (AA) were studied for their potential utility as biomarkers of TBI. Twenty-five female, 4-week-old piglets received diffuse ( = 13) or focal ( = 12) TBI. Blood samples were obtained both pre-injury and at either 24-h or 4-days post-TBI. To find a robust panel of biomarkers, the results of focal and diffuse TBIs were combined and multivariate logistic regression analysis, coupled with the best subset selection technique and repeated k-fold cross-validation method, was used to perform a thorough search of all possible subsets of AAs. The combination of serum glycine, taurine, and ornithine was optimal for TBI diagnosis, with 80% sensitivity and 86% overall prediction rate, and showed excellent TBI diagnostic performance, with 100% sensitivity and 78% overall prediction rate, on a separate validation dataset including four uninjured and five injured animals. We found that combinations of biomarkers outperformed any single biomarker. We propose this 3-AA serum biomarker panel to diagnose mild-to-moderate focal/diffuse TBI. The systematic approaches implemented herein can be used for combining parameters from various TBI assessments to develop/evaluate optimal multi-factorial diagnostic/prognostic TBI metrics.

摘要

创伤性脑损伤(TBI)可导致脑组织和血清中的生化和代谢组学改变。这些改变可用于 TBI 的诊断和预后。本研究旨在探讨 17 种氨基酸(AA)在血清中的浓度变化,评估其作为 TBI 生物标志物的潜在应用价值。25 只 4 周龄雌性小猪接受弥漫性(n=13)或局灶性(n=12)TBI。在损伤前以及损伤后 24 小时或 4 天采集血样。为了寻找稳健的生物标志物组合,将局灶性和弥漫性 TBI 的结果进行合并,采用多元逻辑回归分析,结合最佳子集选择技术和重复 k 折交叉验证方法,对所有可能的 AA 子集进行全面搜索。血清甘氨酸、牛磺酸和鸟氨酸的组合对 TBI 诊断最佳,敏感性为 80%,总体预测率为 86%,在包括 4 只未受伤和 5 只受伤动物的单独验证数据集中,诊断性能优异,敏感性为 100%,总体预测率为 78%。我们发现,生物标志物组合的表现优于任何单一生物标志物。我们提出了这个 3-AA 血清生物标志物组合来诊断轻度至中度局灶性/弥漫性 TBI。本研究中实施的系统方法可用于整合各种 TBI 评估的参数,以开发/评估最佳的多因素诊断/预后 TBI 指标。

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