Biomarkers: Our Path Towards a Cure for Alzheimer Disease.

IF 3.4 Q2 MEDICINE, RESEARCH & EXPERIMENTAL
Biomarker Insights Pub Date : 2020-11-25 eCollection Date: 2020-01-01 DOI:10.1177/1177271920976367
Rawan Tarawneh
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引用次数: 17

Abstract

Over the last decade, biomarkers have significantly improved our understanding of the pathophysiology of Alzheimer disease (AD) and provided valuable tools to examine different disease mechanisms and their progression over time. While several markers of amyloid, tau, neuronal, synaptic, and axonal injury, inflammation, and immune dysregulation in AD have been identified, there is a relative paucity of biomarkers which reflect other disease mechanisms such as oxidative stress, mitochondrial injury, vascular or endothelial injury, and calcium-mediated excitotoxicity. Importantly, there is an urgent need to standardize methods for biomarker assessments across different centers, and to identify dynamic biomarkers which can monitor disease progression over time and/or response to potential disease-modifying treatments. The updated research framework for AD, proposed by the National Institute of Aging- Alzheimer's Association (NIA-AA) Work Group, emphasizes the importance of incorporating biomarkers in AD research and defines AD as a biological construct consisting of amyloid, tau, and neurodegeneration which spans pre-symptomatic and symptomatic stages. As results of clinical trials of AD therapeutics have been disappointing, it has become increasingly clear that the success of future AD trials will require the incorporation of biomarkers in participant selection, prognostication, monitoring disease progression, and assessing response to treatments. We here review the current state of fluid AD biomarkers, and discuss the advantages and limitations of the updated NIA-AA research framework. Importantly, the integration of biomarker data with clinical, cognitive, and imaging domains through a systems biology approach will be essential to adequately capture the molecular, genetic, and pathological heterogeneity of AD and its spatiotemporal evolution over time.

Abstract Image

Abstract Image

生物标志物:我们治疗阿尔茨海默病的途径。
在过去的十年中,生物标志物显著提高了我们对阿尔茨海默病(AD)病理生理学的理解,并为研究不同的疾病机制及其随时间的进展提供了有价值的工具。虽然已经确定了AD中淀粉样蛋白、tau蛋白、神经元、突触和轴突损伤、炎症和免疫失调的几种标志物,但反映其他疾病机制(如氧化应激、线粒体损伤、血管或内皮损伤和钙介导的兴奋性毒性)的生物标志物相对缺乏。重要的是,迫切需要标准化不同中心的生物标志物评估方法,并确定动态生物标志物,以监测疾病随时间的进展和/或对潜在疾病改善治疗的反应。由美国国家衰老研究所-阿尔茨海默病协会(NIA-AA)工作组提出的阿尔茨海默病最新研究框架强调了在阿尔茨海默病研究中纳入生物标志物的重要性,并将阿尔茨海默病定义为一种由淀粉样蛋白、tau蛋白和神经变性组成的生物结构,跨越症状前和症状期。由于阿尔茨海默病治疗药物的临床试验结果令人失望,越来越清楚的是,未来阿尔茨海默病试验的成功将需要在参与者选择、预测、监测疾病进展和评估对治疗的反应方面纳入生物标志物。我们在此回顾了流体AD生物标志物的现状,并讨论了更新的NIA-AA研究框架的优点和局限性。重要的是,通过系统生物学方法将生物标志物数据与临床、认知和成像领域相结合,对于充分捕捉阿尔茨海默病的分子、遗传和病理异质性及其时空演变至关重要。
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来源期刊
Biomarker Insights
Biomarker Insights MEDICINE, RESEARCH & EXPERIMENTAL-
CiteScore
6.00
自引率
0.00%
发文量
26
审稿时长
8 weeks
期刊介绍: An open access, peer reviewed electronic journal that covers all aspects of biomarker research and clinical applications.
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