Memory and Aging Center, Department of Neurology, University of California, San Francisco, San Francisco, California 94158.
Cognitive and Behavioral Neurology Unit, Department of Neurology, University of São Paulo, São Paulo, 05403-900, Brazil.
Cold Spring Harb Perspect Biol. 2018 May 1;10(5):a033134. doi: 10.1101/cshperspect.a033134.
Genetic prion diseases (gPrDs) caused by mutations in the prion protein gene () have been classified as genetic Creutzfeldt-Jakob disease, Gerstmann-Sträussler-Scheinker disease, or fatal familial insomnia. Mutations in can be missense, nonsense, and/or octapeptide repeat insertions or, possibly, deletions. These mutations can produce diverse clinical features. They may also show varying ancillary testing results and neuropathological findings. Although the majority of gPrDs have a rapid progression with a short survival time of a few months, many also present as ataxic or parkinsonian disorders, which have a slower decline over a few to several years. A few very rare mutations manifest as neuropsychiatric disorders, with systemic symptoms that include gastrointestinal disorders and neuropathy; these forms can progress over years to decades. In this review, we classify gPrDs as rapid, slow, or mixed types based on their typical rate of progression and duration, and we review the broad spectrum of phenotypes manifested by these diseases.
遗传性朊病毒病(gPrD)是由朊蛋白基因突变引起的,可分为遗传性克雅氏病、格斯特曼-斯特鲁塞尔综合征或致死性家族性失眠症。 基因中的突变可以是错义、无义和/或八肽重复插入或可能缺失。 这些突变可以产生不同的临床特征。 它们也可能显示不同的辅助检测结果和神经病理学发现。 虽然大多数 gPrD 具有快速进展和数月的短生存期,但许多也表现为共济失调或帕金森病,其在数年内逐渐下降。 一些非常罕见的突变表现为神经精神障碍,伴有包括胃肠道疾病和神经病在内的全身症状;这些形式可以在数年内进展到数十年。 在这篇综述中,我们根据其典型进展速度和持续时间将 gPrD 分为快速、缓慢或混合类型,并综述了这些疾病表现出的广泛表型。
