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人类朊病毒疾病中的生物体液生物标志物及生物安全注意事项

Biological Fluid Biomarkers in Human Prion Diseases with a Note on Biosafety.

作者信息

Ferrer Isidro

机构信息

Department of Pathology and Experimental Therapeutics, University of Barcelona, CIBERNED, 08907 Hospitalet de Llobregat, Barcelona, Spain.

出版信息

Subcell Biochem. 2025;112:189-217. doi: 10.1007/978-3-031-97055-9_9.

DOI:10.1007/978-3-031-97055-9_9
PMID:41004059
Abstract

The definitive diagnosis of human prion diseases can only be obtained postmortem by combining clinical symptoms, neuropathology and PrP immunohistochemistry, Western blotting of PrP types, zygosity of codon 129, and genetic study of PRNP. Premortem diagnosis is strongly sustained by one positive prion-specific assay, commonly protein misfolded cyclic amplification (PMCA) or real-time quaking-induced conversion (RT-QuIC), principally in CSF samples. Surrogate biomarkers 14-3-3, t-tau, P-tau, βA4, and total-PrP levels in the CSF help discriminate other neurodegenerative diseases, but their sensitivity and specificity are variable depending on the prion disease. Other altered proteins in the CSF, such as neurofilament light chain (NfL), calcium-binding protein S100β, neuron-specific enolase, α-synuclein and β-synuclein, neurogranin and SNAP-25, triggering receptor expressed on myeloid cells 2 (TREM2), cytokines, astroglial markers, and microRNAs, need further validation. Total-tau and NfL levels in the blood may serve to monitor disease progression, whereas the value of total-PrP, synuclein, S100β, TREM2, and peripheral inflammatory markers in the blood is limited. Since the products of positive PMCA and PrP are present in several tissues in CJD, special care and biosafety conditions must be applied in managing and processing human biological samples of suspected prion disease. Regarding RT-QuIC products, further experimental studies are needed to elucidate their seeding capacity.

摘要

人类朊病毒病的确诊只能在死后通过结合临床症状、神经病理学、朊蛋白免疫组织化学、朊蛋白类型的蛋白质免疫印迹法、密码子129的纯合性以及朊蛋白基因(PRNP)的遗传学研究来获得。生前诊断主要依靠一种阳性的朊病毒特异性检测方法,通常是蛋白质错误折叠循环扩增法(PMCA)或实时震颤诱导转化法(RT-QuIC),主要检测脑脊液样本。脑脊液中的替代生物标志物14-3-3、总tau蛋白、磷酸化tau蛋白、β淀粉样蛋白4(βA4)和总朊蛋白水平有助于鉴别其他神经退行性疾病,但其敏感性和特异性因朊病毒病而异。脑脊液中其他改变的蛋白质,如神经丝轻链(NfL)、钙结合蛋白S100β、神经元特异性烯醇化酶、α-突触核蛋白和β-突触核蛋白、神经颗粒素和突触小体相关蛋白25(SNAP-25)、髓样细胞触发受体2(TREM2)、细胞因子、星形胶质细胞标志物和微小RNA,需要进一步验证。血液中的总tau蛋白和NfL水平可用于监测疾病进展,而血液中总朊蛋白、突触核蛋白、S100β、TREM2和外周炎症标志物的价值有限。由于在克雅氏病(CJD)中,阳性PMCA和朊蛋白的产物存在于多个组织中,因此在处理和加工疑似朊病毒病的人类生物样本时必须采取特殊的护理和生物安全措施。关于RT-QuIC产物,需要进一步的实验研究来阐明其种子传播能力。

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