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C9orf7-ALS 生物标志物在有症状和无症状患者中的研究进展:临床试验新时代的现状。

Biomarkers for C9orf7-ALS in Symptomatic and Pre-symptomatic Patients: State-of-the-art in the New Era of Clinical Trials.

机构信息

Institut de Myologie, I-Motion Adult ClinicalTrials Platform, Hôpital Pitié-Salpêtrière, Paris, France.

APHP, Centre de référence desmaladies neuromusculaires Nord/Est/Ile de France, Hôpital Pitié-Salpêtrière, Paris, France.

出版信息

J Neuromuscul Dis. 2022;9(1):25-37. doi: 10.3233/JND-210754.

Abstract

The development of new possible treatments for C9orf72-related ALS and the possibility of early identification of subjects genetically at risk of developing the disease is creating a critical need for biomarkers to track neurodegeneration that could be used as outcome measures in clinical trials. Current candidate biomarkers in C9orf72-ALS include neuropsychology tests, imaging, electrophysiology as well as different circulating biomarkers. Neuropsychology tests show early executive and verbal function involvement both in symptomatic and asymptomatic mutation carriers. At brain MRI, C9orf72-ALS patients present diffuse white and grey matter degeneration, which are already identified up to 20 years before symptom onset and that seem to be slowly progressive over time, while regions of altered connectivity at fMRI and of hypometabolism at [18F]FDG PET have been described as well. At the same time, spinal cord MRI has also shown progressive decrease of FA in the cortico-spinal tract over time. On the side of wet biomarkers, neurofilament proteins are increased both in the CSF and serum just before symptom onset and tend to slowly increase over time, while poly(GP) protein can be detected in the CSF and probably used as target engagement marker in clinical trials.

摘要

针对 C9orf72 相关肌萎缩侧索硬化症(ALS)的新治疗方法不断涌现,并且有可能早期识别出具有遗传风险的患者,因此,寻找可用于临床试验中跟踪神经退行性变的生物标志物成为当务之急。目前 C9orf72-ALS 的候选生物标志物包括神经心理学测试、影像学、电生理学以及各种循环生物标志物。神经心理学测试显示,在有症状和无症状的突变携带者中,早期就会出现执行功能和语言功能的障碍。在脑 MRI 上,C9orf72-ALS 患者表现为弥漫性白质和灰质变性,这些变化在症状出现前 20 年就已被识别出来,并且似乎随着时间的推移而逐渐进展,同时功能磁共振成像(fMRI)显示的连接改变区域和 [18F]FDG PET 显示的代谢降低区域也已被描述。与此同时,脊髓 MRI 也显示出皮质脊髓束的 FA 值随时间逐渐降低。在湿生物标志物方面,神经丝蛋白在 CSF 和血清中均在症状出现前升高,并随着时间的推移而逐渐升高,而多聚(GP)蛋白可在 CSF 中检测到,并可能作为临床试验中的靶点结合标志物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/896b/8842771/8f55a60bf304/jnd-9-jnd210754-g001.jpg

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