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代谢组学生物标志物可能是中风发病时间的分子时钟。

Metabolomic biomarkers could be molecular clocks in timing stroke onset.

作者信息

Li Qianyun, Zhang Xiaodan, Zhang Yilin, Lam Rex Pui Kin, Jin Yulan, Ji Chengcheng, Fan Weinv, Rainer Timothy Hudson

机构信息

Department of Emergency Medicine, School of Clinical Medicine, LKS Faculty of Medicine, The University of Hong Kong. G06, G/F, University of Hong Kong the Hong Kong Jockey Club Building for Interdisciplinary Research, University of Hong Kong, 5 Sassoon Road, Pokfulam, Hong Kong SAR, China.

Department of Clinical Laboratory, Ningbo NO.2 Hospital, Ningbo, Zhejiang Province, China.

出版信息

Sci Rep. 2025 Jul 1;15(1):21645. doi: 10.1038/s41598-025-05334-0.

Abstract

The preferred treatment for acute ischaemic stroke (AIS) is intravenous thrombolysis (IVT) administered within 4.5 hours (h) of symptom onset. This study aimed to identify metabolomic biomarkers for distinguishing AIS patients within 4.5 h of symptom onset, addressing the often exclusion of those with unknown onset times from IVT. In this retrospective case-control study with 30 AIS patients, early AIS with onset time within 0-4.5 h (ES, n = 16) and late AIS within 4.5-24 h (LS, n = 14) groups were differentiated. Their complete sets of plasma metabolites were examined. A stepwise analysis was performed to identify potential biomarkers. Biliverdin and Nicotinamide N-oxide (NAMO) emerged as potential biomarkers, combined to achieve a high AUC of 0.964 (95% Confidential interval 0.900-1), a specificity of 100% (78.47-100%), and a sensitivity of 93.75% (71.67-98.89%) for AIS onset time determination. These metabolites show promise as molecular clocks for determining the onset time of AIS, potentially extending IVT access to patients with unknown onset times. However, their clinical applicability necessitates rigorous validation in larger and independent cohorts to establish their role in improving AIS management through extended IVT accessibility.

摘要

急性缺血性卒中(AIS)的首选治疗方法是在症状发作后4.5小时内进行静脉溶栓(IVT)。本研究旨在识别用于区分症状发作后4.5小时内AIS患者的代谢组学生物标志物,以解决IVT通常会排除发病时间不明患者的问题。在这项回顾性病例对照研究中,纳入了30例AIS患者,区分出了发病时间在0 - 4.5小时内的早期AIS组(ES,n = 16)和发病时间在4.5 - 24小时内的晚期AIS组(LS,n = 14)。检测了他们的全套血浆代谢物。进行了逐步分析以识别潜在的生物标志物。胆红素和烟酰胺N - 氧化物(NAMO)成为潜在的生物标志物,两者结合对AIS发病时间的测定具有较高的曲线下面积(AUC),为0.964(95%置信区间0.900 - 1),特异性为100%(78.47 - 100%),敏感性为93.75%(71.67 - 98.89%)。这些代谢物有望作为确定AIS发病时间的分子时钟,有可能将IVT治疗扩展到发病时间不明的患者。然而,它们的临床适用性需要在更大规模的独立队列中进行严格验证,以确定它们在通过扩大IVT可及性来改善AIS管理方面的作用。

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