医学
心脏病学
生物标志物
前瞻性队列研究
内科学
磁共振成像
队列
冲程(发动机)
缺血
血液取样
代理终结点
脑缺血
缺血性中风
梗塞
临床终点
缺血性损伤
脑梗塞
创伤性脑损伤
试验预测值
脑血流
队列研究
神经影像学
多中心试验
中枢神经系统疾病
病理生理学
急性中风
成像生物标志物
冲程容积
疾病严重程度
中风恢复
作者
Naomi Vlegels,Nicoló Luca Knuth,Konstantin A. Steiner,Linjie Zhang,Apolline L. Vix,Dilara Moumin,Irem Mirzen,Nada Khalifeh,Charlotte Forster,Benno Gesierich,Franziska Müller,P Lohse,Jule Filler,Rong Fang,Matthias S. Klein,Konstantinos Dimitriadis,Nicolai Franzmeier,Thomas Liebig,Endres Matthias,Michael Goertler
标识
DOI:10.1126/scitranslmed.adz1280
摘要
A specific and accurate blood test for acute brain injury could help monitor infarct growth in ischemic stroke and serve as a surrogate end point in clinical trials. Using a single-molecule detection assay, we assessed plasma brain-derived tau (BD-tau), a marker selectively quantifying tau protein from the central nervous system, in a prospective cohort of 502 patients with acute ischemic stroke with serial blood sampling from admission to day 7. Higher BD-tau concentrations at admission were associated with more extensive early brain injury on computed tomography and predicted larger final infarct volumes. BD-tau increases from admission to day 2 were related to infarct growth. BD-tau concentrations rose until day 7 and were higher in patients with secondary events, including recurrent stroke. After thrombectomy, the rise of BD-tau was smaller in patients with complete versus incomplete recanalization. BD-tau outperformed other blood markers and imaging metrics in predicting 90-day functional outcome across infarct size strata and time points. In an independent multicenter prospective cohort ( N = 519), BD-tau showed higher performance than magnetic resonance imaging–derived final infarct volume in predicting functional outcomes at 3, 12, and 36 months. In the biomarker substudy of a phase 3 trial assessing nerinetide in patients with ischemic stroke ( N = 193), BD-tau showed predictive performance comparable to the other cohorts, mediated the relationship between recanalization and functional outcome, and showed a 49% smaller increase in the nerinetide group versus placebo. Overall, plasma BD-tau tracked ischemic brain injury over time, outperformed other biomarkers in predicting functional outcomes, and identified possible treatment responses.
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