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中澳蝙蝠相关狂犬病毒比从野生犬科动物中分离出的病毒具有更短的临床潜伏期和更低的致病潜力。

Nyctinomops laticaudatus bat-associated Rabies virus causes disease with a shorter clinical period and has lower pathogenic potential than strains isolated from wild canids.

机构信息

Pasteur Institute, Av. Paulista 393, São Paulo, SP, CEP 01311-000, Brazil.

Laboratory of Immunogenetics, Butantan Institute, Av. Vital Brasil 1500, São Paulo, SP, CEP 05503-900, Brazil.

出版信息

Arch Virol. 2019 Oct;164(10):2469-2477. doi: 10.1007/s00705-019-04335-5. Epub 2019 Jul 10.

Abstract

Rabies is a lethal viral disease that can affect a wide range of mammals. Currently, Rabies virus (RABV) in some European and American countries is maintained primarily in wild species. The regulation of viral replication is one of the critical mechanisms involved in RABV pathogenesis. However, the relationship between replication and the pathogenesis of RABV isolated from wild animals remains poorly understood. In the present study, we evaluated the pathogenicity of the street viruses Nyctinomops laticaudatus bat-associated RABV (NYBRV) and Cerdocyon thous canid-associated RABV (CECRV). Infection of mice with NYBRV led to 33% mortality with rapid disease evolution and marked histopathological changes in the CNS. In contrast, infection with CECRV led to 67% mortality and caused mild neuropathological lesions. The proportion of RABV antigen was significantly higher in the cytoplasm of neuronal cells of the cerebral cortex and in the meninges of mice infected with CECRV and NYBRV, respectively. Moreover, the replication rate of NYBRV was significantly higher (p < 0.001) than that of CECRV in neuroblastoma cells. However, CECRV replicated to a significantly higher titer in epithelial cells. Our results indicate that NYBRV infection results in rapid disease progression accompanied by frequent and intense histopathological alterations in the CNS in mice, and in a high replication rate in neuroblastoma cells. Although, CECRV is more pathogenic in mice, it caused milder histopathological changes in the CNS and replicated more efficiently in epithelial cells. Our data point to a correlation between clinical aspects of disease and the replication of RABV in different cell lines.

摘要

狂犬病是一种致命的病毒性疾病,可影响多种哺乳动物。目前,一些欧美国家的狂犬病病毒(RABV)主要存在于野生动物中。病毒复制的调控是 RABV 发病机制中的关键机制之一。然而,从野生动物中分离出的 RABV 的复制与发病机制之间的关系仍知之甚少。在本研究中,我们评估了 Nyctinomops laticaudatus 蝙蝠相关狂犬病病毒(NYBRV)和 Cerdocyon thous 犬相关狂犬病病毒(CECRV)的致病性。用 NYBRV 感染小鼠导致 33%的死亡率,疾病迅速发展,并导致中枢神经系统明显的组织病理学变化。相比之下,用 CECRV 感染导致 67%的死亡率,并引起轻度神经病理学病变。感染 CECRV 和 NYBRV 的小鼠大脑皮层神经元细胞的细胞质和脑膜中,RABV 抗原的比例明显更高。此外,NYBRV 在神经母细胞瘤细胞中的复制率明显高于 CECRV(p<0.001)。然而,CECRV 在上皮细胞中的复制率明显更高。我们的结果表明,NYBRV 感染导致疾病迅速进展,同时伴有小鼠中枢神经系统频繁和强烈的组织病理学改变,以及在神经母细胞瘤细胞中高复制率。尽管 CECRV 在小鼠中更具致病性,但它在中枢神经系统中引起的组织病理学变化较轻,在上皮细胞中复制效率更高。我们的数据表明,疾病的临床方面与 RABV 在不同细胞系中的复制之间存在相关性。

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