Blood biomarkers in ALS: challenges, applications and novel frontiers

IF 2.9 3区 医学 Q2 CLINICAL NEUROLOGY
Ellie Sturmey, Andrea Malaspina
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引用次数: 13

Abstract

Amyotrophic lateral sclerosis (ALS) is the most common motor neuron disease among adults. With diagnosis reached relatively late into the disease process, extensive motor cell loss narrows the window for therapeutic opportunities. Clinical heterogeneity in ALS and the lack of disease-specific biomarkers have so far led to large-sized clinical trials with long follow-up needed to define clinical outcomes. In advanced ALS patients, there is presently limited scope to use imaging or invasive cerebrospinal fluid (CSF) collection as a source of disease biomarkers. The development of more patient-friendly and accessible blood biomarker assays is hampered by analytical hurdles like the matrix effect of blood components. However, blood also provides the opportunity to identify disease-specific adaptive changes of the stoichiometry and conformation of target proteins and the endogenous immunological response to low-abundance brain peptides, such as neurofilaments (Nf). Among those biomarkers under investigation in ALS, the change in concentration before or after diagnosis of Nf has been shown to aid prognostication and to allow the a priori stratification of ALS patients into smaller sized and clinically more homogeneous cohorts, supporting more affordable clinical trials. Here, we discuss the technical hurdles affecting reproducible and sensitive biomarker measurement in blood. We also summarize the state of the art of non-CSF biomarkers in the study of prognosis, disease progression, and treatment response. We will then address the potential as disease-specific biomarkers of the newly discovered cryptic peptides which are formed down-stream of TDP-43 loss of function, the hallmark of ALS pathobiology.

Abstract Image

Abstract Image

ALS中的血液生物标志物:挑战、应用和新领域
肌萎缩性侧索硬化症(ALS)是成人中最常见的运动神经元疾病。由于诊断相对较晚,广泛的运动细胞损失缩小了治疗机会的窗口。到目前为止,ALS的临床异质性和缺乏疾病特异性生物标志物导致需要长时间随访的大规模临床试验来确定临床结果。在晚期ALS患者中,目前使用成像或侵入性脑脊液(CSF)收集作为疾病生物标志物来源的范围有限。由于血液成分的基质效应等分析障碍,对患者更友好和更容易获得的血液生物标志物检测的发展受到了阻碍。然而,血液也提供了机会来确定目标蛋白的化学计量学和构象的疾病特异性适应性变化以及对低丰度脑肽(如神经丝(Nf))的内源性免疫反应。在正在研究的ALS生物标志物中,Nf诊断前后的浓度变化已被证明有助于预测,并允许将ALS患者先验分层为较小规模和临床更均匀的队列,支持更负担得起的临床试验。在这里,我们讨论了影响血液中可重复和敏感的生物标志物测量的技术障碍。我们还总结了非脑脊液生物标志物在预后、疾病进展和治疗反应研究中的最新进展。然后,我们将讨论新发现的隐肽作为疾病特异性生物标志物的潜力,这些隐肽是在TDP-43功能丧失的下游形成的,这是ALS病理生物学的标志。
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来源期刊
Acta Neurologica Scandinavica
Acta Neurologica Scandinavica 医学-临床神经学
CiteScore
6.70
自引率
2.90%
发文量
161
审稿时长
4-8 weeks
期刊介绍: Acta Neurologica Scandinavica aims to publish manuscripts of a high scientific quality representing original clinical, diagnostic or experimental work in neuroscience. The journal''s scope is to act as an international forum for the dissemination of information advancing the science or practice of this subject area. Papers in English will be welcomed, especially those which bring new knowledge and observations from the application of therapies or techniques in the combating of a broad spectrum of neurological disease and neurodegenerative disorders. Relevant articles on the basic neurosciences will be published where they extend present understanding of such disorders. Priority will be given to review of topical subjects. Papers requiring rapid publication because of their significance and timeliness will be included as ''Clinical commentaries'' not exceeding two printed pages, as will ''Clinical commentaries'' of sufficient general interest. Debate within the speciality is encouraged in the form of ''Letters to the editor''. All submitted manuscripts falling within the overall scope of the journal will be assessed by suitably qualified referees.
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