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一种用于补充神经病理学朊病毒病诊断的固定脑种子扩增检测方法。

A fixed brain seeded amplification assay to complement neuropathological prion disease diagnosis.

作者信息

Lewis Victoria, Ellett Laura, Lei Enie, Stehmann Christiane, Birchall Ian, Senesi Matteo, McLean Catriona, Collins Steven J

机构信息

Department of Medicine (RMH), The University of Melbourne, Parkville, VIC, Australia.

Australian National Creutzfeldt-Jakob Disease Registry (ANCJDR), The Florey Institute of Neuroscience and Mental Health, Parkville, VIC, Australia.

出版信息

J Neuropathol Exp Neurol. 2025 Sep 3. doi: 10.1093/jnen/nlaf105.

Abstract

Prion diseases are rare neurodegenerative disorders that share misfolding of the normal cellular prion protein into disease-causing isoforms known as "prions" as the critical pathophysiological event. Definite diagnosis can only be achieved through neuropathological confirmation. The neuropathological features of prion disease are well described; however, some molecular subtypes are typified by characteristic neuropathological features that are subtle or absent. Prion seeding assays have excellent specificity and have considerably improved premortem diagnostic accuracy but they have reduced sensitivity for some uncommon prion disease molecular subtypes. We developed a formalin-fixed, paraffin-embedded tissue-based prion seeding assay to serve as a complementary diagnostic tool for prion diseases. Fixed brain tissue was prepared through an optimized process involving careful defacing of tissue blocks prior to sampling and then stepwise deparaffinization and homogenization. Fixed tissue homogenates are then tested in an adapted version of a diagnostic cerebrospinal fluid (CSF) prion seeding assay, which utilizes full-length recombinant hamster prion protein as substrate. Two examples illustrate the utility of the assay by confirming prion seeding in fixed brain tissue from previously neuropathologically misdiagnosed obligate carriers of 2 different prion protein gene mutations. The importance of careful tissue sampling to rigorously maintain the diagnostic specificity of this assay is also highlighted.

摘要

朊病毒病是罕见的神经退行性疾病,其关键病理生理事件是正常细胞朊病毒蛋白错误折叠为致病异构体,即“朊病毒”。只有通过神经病理学确认才能做出明确诊断。朊病毒病的神经病理学特征已有详细描述;然而,一些分子亚型以细微或不存在的特征性神经病理学特征为典型。朊病毒种子检测具有出色的特异性,大大提高了生前诊断准确性,但对一些罕见的朊病毒病分子亚型的敏感性有所降低。我们开发了一种基于福尔马林固定、石蜡包埋组织的朊病毒种子检测方法,作为朊病毒病的补充诊断工具。通过优化流程制备固定脑组织,该流程包括在取样前仔细去除组织块表面,然后逐步脱石蜡和匀浆。然后,将固定组织匀浆在一种改良的诊断性脑脊液(CSF)朊病毒种子检测方法中进行检测,该方法利用全长重组仓鼠朊病毒蛋白作为底物。两个例子说明了该检测方法的实用性,通过在先前经神经病理学误诊的两种不同朊病毒蛋白基因突变的 obligate 携带者的固定脑组织中确认朊病毒种子。还强调了仔细组织取样以严格保持该检测方法诊断特异性的重要性。

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