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循环代谢物可区分急性缺血性卒中和卒中介体。

Circulating Metabolites Differentiate Acute Ischemic Stroke from Stroke Mimics.

机构信息

Institute for Stroke and Dementia Research, University Hospital, LMU Munich, Munich, Germany.

Munich Cluster for Systems Neurology (SyNergy), Munich, Germany.

出版信息

Ann Neurol. 2020 Oct;88(4):736-746. doi: 10.1002/ana.25859. Epub 2020 Aug 29.

Abstract

OBJECTIVE

Early discrimination of patients with ischemic stroke (IS) from stroke mimics (SMs) poses a diagnostic challenge. The circulating metabolome might reflect pathophysiological events related to acute IS. Here, we investigated the utility of early metabolic changes for differentiating IS from SM.

METHODS

We performed untargeted metabolomics on serum samples obtained from patients with IS (N = 508) and SM (N = 349; defined by absence of a diffusion weighted imaging [DWI] positive lesion on magnetic resonance imaging [MRI]) who presented to the hospital within 24 hours after symptom onset (median time from symptom onset to blood sampling = 3.3 hours; interquartile range [IQR] = 1.6-6.7 hours) and from neurologically normal controls (NCs; N = 112). We compared diagnostic groups in a discovery-validation approach by applying multivariable linear regression models, machine learning techniques, and propensity score matching. We further performed a targeted look-up of published metabolite sets.

RESULTS

Levels of 41 metabolites were significantly associated with IS compared to NCs. The top metabolites showing the highest value in separating IS from SMs were asymmetrical and symmetrical dimethylarginine, pregnenolone sulfate, and adenosine. Together, these 4 metabolites differentiated patients with IS from SMs with an area under the curve (AUC) of 0.90 in the replication sample, which was superior to multimodal cranial computed tomography (CT; AUC = 0.80) obtained for routine diagnostics. They were further superior to previously published metabolite sets detected in our samples. All 4 metabolites returned to control levels by day 90.

INTERPRETATION

A set of 4 metabolites with known biological effects relevant to stroke pathophysiology shows unprecedented utility to identify patients with IS upon hospital arrival, thus encouraging further investigation, including multicenter studies. ANN NEUROL 2020;88:736-746.

摘要

目的

早期区分缺血性脑卒中(IS)患者与脑卒中类似症(SM)具有诊断挑战性。循环代谢组可能反映与急性 IS 相关的病理生理事件。在此,我们研究了早期代谢变化在区分 IS 与 SM 中的作用。

方法

我们对发病 24 小时内入院的 IS 患者(N=508)和 SM 患者(无磁共振成像 [MRI] 弥散加权成像 [DWI] 阳性病灶,N=349)以及神经正常对照者(NC;N=112)的血清样本进行非靶向代谢组学分析。我们通过多变量线性回归模型、机器学习技术和倾向评分匹配在发现-验证方法中比较诊断组。我们还对已发表的代谢物集进行了靶向查找。

结果

与 NC 相比,41 种代谢物的水平与 IS 显著相关。区分 IS 与 SM 中最高效的前 4 种代谢物是不对称和对称二甲基精氨酸、孕烯醇酮硫酸盐和腺苷。这 4 种代谢物联合使用可在验证样本中区分 IS 与 SM,曲线下面积(AUC)为 0.90,优于常规诊断中获得的多模态头颅计算机断层扫描(CT;AUC=0.80)。它们还优于我们样本中检测到的先前发表的代谢物集。所有 4 种代谢物在第 90 天均恢复到对照水平。

结论

一组与卒中病理生理学相关的 4 种具有已知生物学效应的代谢物具有前所未有的效用,可在入院时识别 IS 患者,因此鼓励进一步研究,包括多中心研究。

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