Protective role of cytosolic prion protein against virus infection in prion-infected cells.

IF 4 2区医学 Q2 VIROLOGY

Journal of Virology Pub Date : 2024-09-17 Epub Date: 2024-08-28 DOI:10.1128/jvi.01262-24

Hideyuki Hara, Junji Chida, Batzaya Batchuluun, Etsuhisa Takahashi, Hiroshi Kido, Suehiro Sakaguchi

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引用次数: 0

Abstract

Production of the amyloidogenic prion protein, PrP^Sc, which forms infectious protein aggregates, or prions, is a key pathogenic event in prion diseases. Functional prion-like protein aggregations, such as the mitochondrial adaptor protein MAVS and the inflammasome component protein ASC, have been identified to play a protective role in viral infections in mammalian cells. In this study, to investigate if PrP^Sc could play a functional role against external stimuli, we infected prion-infected cells with a neurotropic influenza A virus strain, IAV/WSN. We found that prion-infected cells were highly resistant to IAV/WSN infection. In these cells, NF-κB nuclear translocation was disturbed; therefore, mitochondrial superoxide dismutase (mtSOD) expression was suppressed, and mitochondrial reactive oxygen species (mtROS) was increased. The elevated mtROS subsequently activated NLRP3 inflammasomes, leading to the suppression of IAV/WSN-induced necroptosis. We also found that prion-infected cells accumulated a portion of PrP molecules in the cytosol, and that the N-terminal potential nuclear translocation signal of PrP impeded NF-κB nuclear translocation. These results suggest that PrP^Sc might play a functional role in protection against viral infections by stimulating the NLRP3 inflammasome-dependent antivirus mechanism through the cytosolic PrP-mediated disturbance of NF-κB nuclear translocation, which leads to suppression of mtSOD expression and consequently upregulation of the NLRP3 inflammasome activator mtROS.

Importance: Cytosolic PrP has been detected in prion-infected cells and suggested to be involved in the neurotoxicity of prions. Here, we also detected cytosolic PrP in prion-infected cells. We further found that the nuclear translocation of NF-κB was disturbed in prion-infected cells and that the N-terminal potential nuclear translocation signal of PrP expressed in the cytosol disturbed the nuclear translocation of NF-κB. Thus, the N-terminal nuclear translocation signal of cytosolic PrP might play a role in prion neurotoxicity. Prion-like protein aggregates in other protein misfolding disorders, including Alzheimer's disease were reported to play a protective role against various environmental stimuli. We here showed that prion-infected cells were partially resistant to IAV/WSN infection due to the cytosolic PrP-mediated disturbance of the nuclear translocation of NF-κB, which consequently activated NLRP3 inflammasomes after IAV/WSN infection. It is thus possible that prions could also play a protective role in viral infections.

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朊病毒感染细胞中细胞膜朊病毒蛋白对病毒感染的保护作用。

产生淀粉样蛋白朊病毒蛋白 PrPSc，形成感染性蛋白聚集体或朊病毒，是朊病毒疾病的关键致病事件。已发现线粒体适配蛋白 MAVS 和炎性体组成蛋白 ASC 等功能性朊病毒样蛋白聚集体在哺乳动物细胞的病毒感染中发挥保护作用。在本研究中，为了研究PrPSc是否能在抵御外部刺激时发挥功能性作用，我们用一种神经性甲型流感病毒株IAV/WSN感染了朊病毒感染细胞。我们发现，朊病毒感染细胞对 IAV/WSN 感染具有很强的抵抗力。在这些细胞中，NF-κB 的核转位受到干扰，因此线粒体超氧化物歧化酶（mtSOD）的表达受到抑制，线粒体活性氧（mtROS）增加。升高的 mtROS 随后激活了 NLRP3 炎症小体，从而抑制了 IAV/WSN 诱导的坏死。我们还发现，受朊病毒感染的细胞在细胞质中积累了一部分 PrP 分子，而 PrP 的 N 端潜在核转位信号阻碍了 NF-κB 的核转位。这些结果表明，PrPSc可能通过细胞膜PrP介导的NF-κB核转位干扰，刺激NLRP3炎性体依赖的抗病毒机制，从而抑制mtSOD的表达，进而上调NLRP3炎性体激活剂mtROS，在抵御病毒感染方面发挥功能性作用：在朊病毒感染的细胞中检测到了细胞膜 PrP，并认为它与朊病毒的神经毒性有关。在这里，我们也在朊病毒感染的细胞中检测到了细胞质 PrP。我们进一步发现，在朊病毒感染的细胞中，NF-κB 的核转位受到干扰，在细胞质中表达的 PrP 的 N 端潜在核转位信号干扰了 NF-κB 的核转位。因此，胞浆 PrP 的 N 端核转位信号可能在朊病毒神经毒性中发挥作用。据报道，在包括阿尔茨海默病在内的其他蛋白质错误折叠疾病中，朊病毒样蛋白聚集体对各种环境刺激起到保护作用。我们在这里发现，朊病毒感染细胞对 IAV/WSN 感染具有部分抵抗力，这是由于细胞膜 PrP 介导的 NF-κB 核转位紊乱，从而在 IAV/WSN 感染后激活了 NLRP3 炎症体。因此，朊病毒也可能在病毒感染中发挥保护作用。

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来源期刊

Journal of Virology 医学-病毒学

CiteScore

10.10

自引率

7.40%

发文量

906

审稿时长

1 months

期刊介绍： Journal of Virology (JVI) explores the nature of the viruses of animals, archaea, bacteria, fungi, plants, and protozoa. We welcome papers on virion structure and assembly, viral genome replication and regulation of gene expression, genetic diversity and evolution, virus-cell interactions, cellular responses to infection, transformation and oncogenesis, gene delivery, viral pathogenesis and immunity, and vaccines and antiviral agents.