Potential blood biomarkers for chronic traumatic encephalopathy: The multi-omics landscape of an observational cohort

慢性创伤性脑病 医学 队列 观察研究 组学 创伤性脑损伤 疾病 队列研究 内科学 生物信息学 急诊医学 毒物控制 伤害预防 精神科 脑震荡 生物
作者
Xintong Ge,Mengtian Guo,Meimei Li,Shishuang Zhang,Junlian Qiang,Luoyun Zhu,Lu Cheng,Wenzhu Li,Yan Wang,Jinwen Yu,Zhenyu Yin,Fanglian Chen,Wen Tong,Ping Lei
出处
期刊:Frontiers in Aging Neuroscience [Frontiers Media SA]
卷期号:14 被引量:6
标识
DOI:10.3389/fnagi.2022.1052765
摘要

Chronic traumatic encephalopathy (CTE) is a neurodegenerative disease associated with exposure to repetitive head impacts, which is susceptible in elderly people with declined mobility, athletes of full contact sports, military personnel and victims of domestic violence. It has been pathologically diagnosed in brain donors with a history of repetitive mild traumatic brain injury (rmTBI), but cannot be clinically diagnosed for a long time. By the continuous efforts by neuropathologists, neurologists and neuroscientists in recent 10 years, an expert consensus for the diagnostic framework of CTE was proposed in 2021 funded by the National Institute of Neurological Disorders and Stroke. The new consensus contributes to facilitating research in the field. However, it still needs to incorporate in vivo biomarkers to further refine and validate the clinical diagnostic criteria. From this, a single-center, observational cohort study has been being conducted by Tianjin Medical University General Hospital since 2021. As a pilot study of this clinical trial, the present research recruited 12 pairs of gender- and age-matched rmTBI patients with healthy subjects. Their blood samples were collected for exosome isolation, and multi-omics screening to explore potential diagnostic biomarkers in blood and its exosomes. The expression level of CHL1 protein, KIF2A mRNA, LIN7C mRNA, miR-297, and miR-1183 in serum and exosomes were found to be differentially expressed between groups. Besides, serum and exosomal CHL1, KIF2A, and miR-1183, as well as exosomal miR-297 were further verified as potential biomarkers for CTE by low-throughput assays. They are expected to contribute to establishing a novel set of CTE diagnostic signatures with classic neurodegenerative indicators in our future study, thereby updating the consensus diagnostic criteria for CTE by incorporating new evidence of the in vivo biomarkers.

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