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朊病毒株:为旧概念带来新曙光。

Prion strains: shining new light on old concepts.

机构信息

Department of Medical Microbiology and Immunology, Creighton University, 2500 California Plaza, Omaha, NE, 68178, USA.

出版信息

Cell Tissue Res. 2023 Apr;392(1):113-133. doi: 10.1007/s00441-022-03665-2. Epub 2022 Jul 7.

Abstract

Prion diseases are a group of inevitably fatal neurodegenerative disorders affecting numerous mammalian species, including humans. The existence of heritable phenotypes of disease in the natural host suggested that prions exist as distinct strains. Transmission of sheep scrapie to rodent models accelerated prion research, resulting in the isolation and characterization of numerous strains with distinct characteristics. These strains are grouped into categories based on the incubation period of disease in different strains of mice and also by how stable the strain properties were upon serial passage. These classical studies defined the host and agent parameters that affected strain properties, and, prior to the advent of the prion hypothesis, strain properties were hypothesized to be the result of mutations in a nucleic acid genome of a conventional pathogen. The development of the prion hypothesis challenged the paradigm of infectious agents, and, initially, the existence of strains was difficult to reconcile with a protein-only agent. In the decades since, much evidence has revealed how a protein-only infectious agent can perform complex biological functions. The prevailing hypothesis is that strain-specific conformations of PrP encode prion strain diversity. This hypothesis can provide a mechanism to explain the observed strain-specific differences in incubation period of disease, biochemical properties of PrP, tissue tropism, and subcellular patterns of pathology. This hypothesis also explains how prion strains mutate, evolve, and adapt to new species. These concepts are applicable to prion-like diseases such as Parkinson's and Alzheimer's disease, where evidence of strain diversity is beginning to emerge.

摘要

朊病毒病是一组不可避免的致命神经退行性疾病,影响包括人类在内的许多哺乳动物物种。天然宿主中存在疾病遗传表型表明,朊病毒存在不同的株系。绵羊瘙痒病向啮齿动物模型的传播加速了朊病毒研究,导致了许多具有不同特征的株系的分离和特征描述。这些株系根据不同品系小鼠中疾病的潜伏期以及株系特性在连续传代过程中的稳定性进行分类。这些经典研究定义了影响株系特性的宿主和因子参数,并且在朊病毒假说出现之前,人们假设株系特性是传统病原体核酸基因组突变的结果。朊病毒假说的提出挑战了传染性病原体的范式,最初,株系的存在很难与仅由蛋白质组成的病原体相一致。在随后的几十年中,大量证据揭示了仅由蛋白质组成的传染性病原体如何执行复杂的生物学功能。目前的主流假说认为,PrP 的株系特异性构象编码了朊病毒株系的多样性。该假说可以提供一种机制来解释观察到的疾病潜伏期、PrP 的生化特性、组织嗜性和病理的亚细胞模式的株系特异性差异。该假说还解释了朊病毒株系如何突变、进化和适应新物种。这些概念适用于朊病毒样疾病,如帕金森病和阿尔茨海默病,其中开始出现株系多样性的证据。

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