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本文引用的文献

1
Using the ferret model to study morbillivirus entry, spread, transmission and cross-species infection.利用雪貂模型研究麻疹病毒的进入、传播、传播和跨物种感染。
Curr Opin Virol. 2014 Feb;4:15-23. doi: 10.1016/j.coviro.2013.11.001. Epub 2013 Dec 6.
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Paramyxovirus infections in ex vivo lung slice cultures of different host species.不同宿主物种的离体肺切片培养中的副粘病毒感染。
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Fatal combined infection with canine distemper virus and orthopoxvirus in a group of Asian marmots (Marmota caudata).一组亚洲土拨鼠(Marmota caudata)中犬瘟热病毒和正痘病毒的致命合并感染。
Vet Pathol. 2013 Sep;50(5):914-20. doi: 10.1177/0300985813476060. Epub 2013 Feb 4.
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Measles virus infection of epithelial cells in the macaque upper respiratory tract is mediated by subepithelial immune cells.猴上呼吸道上皮细胞中的麻疹病毒感染是由黏膜下免疫细胞介导的。
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Lethal canine distemper virus outbreak in cynomolgus monkeys in Japan in 2008.2008 年日本食蟹猴中发生致命犬瘟热病毒暴发。
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Measles immune suppression: lessons from the macaque model.麻疹免疫抑制:猕猴模型的经验教训。
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7
Nectin4 is an epithelial cell receptor for canine distemper virus and involved in neurovirulence.神经细胞黏附分子 4 是犬瘟热病毒的上皮细胞受体,参与病毒的神经毒力。
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Nectin 4 is the epithelial cell receptor for measles virus.Nectin 4 是麻疹病毒的上皮细胞受体。
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9
Recombinant canine distemper virus strain Snyder Hill expressing green or red fluorescent proteins causes meningoencephalitis in the ferret.表达绿色或红色荧光蛋白的重组犬瘟热病毒 Snyder Hill 株可引起雪貂的脑膜脑炎。
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10
Bats host major mammalian paramyxoviruses.蝙蝠是主要的哺乳动物副粘病毒宿主。
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给非人类灵长类动物接种麻疹疫苗可提供针对犬瘟热病毒感染的部分保护。

Measles vaccination of nonhuman primates provides partial protection against infection with canine distemper virus.

机构信息

Department of Viroscience, Erasmus MC, Rotterdam, the Netherlands.

出版信息

J Virol. 2014 Apr;88(8):4423-33. doi: 10.1128/JVI.03676-13. Epub 2014 Feb 5.

DOI:10.1128/JVI.03676-13
PMID:24501402
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3993716/
Abstract

UNLABELLED

Measles virus (MV) is being considered for global eradication, which would likely reduce compliance with MV vaccination. As a result, children will grow up without MV-specific immunity, creating a potential niche for closely related animal morbilliviruses such as canine distemper virus (CDV). Natural CDV infection causing clinical signs has never been reported in humans, but recent outbreaks in captive macaques have shown that CDV can cause disease in primates. We studied the virulence and tropism of recombinant CDV expressing enhanced green fluorescent protein in naive and measles-vaccinated cynomolgus macaques. In naive animals CDV caused viremia and fever and predominantly infected CD150(+) lymphocytes and dendritic cells. Virus was reisolated from the upper and lower respiratory tracts, but infection of epithelial or neuronal cells was not detectable at the time points examined, and the infections were self-limiting. This demonstrates that CDV readily infects nonhuman primates but suggests that additional mutations are necessary to achieve full virulence in nonnatural hosts. Partial protection against CDV was observed in measles-vaccinated macaques, as demonstrated by accelerated control of virus replication and limited shedding from the upper respiratory tract. While neither CDV infection nor MV vaccination induced detectable cross-reactive neutralizing antibodies, MV-specific neutralizing antibody levels of MV-vaccinated macaques were boosted by CDV challenge infection, suggesting that cross-reactive VN epitopes exist. Rapid increases in white blood cell counts in MV-vaccinated macaques following CDV challenge suggested that cross-reactive cellular immune responses were also present. This study demonstrates that zoonotic morbillivirus infections can be controlled by measles vaccination.

IMPORTANCE

Throughout history viral zoonoses have had a substantial impact on human health. Given the drive toward global eradication of measles, it is essential to understand the zoonotic potential of animal morbilliviruses. Morbilliviruses are thought to have evolved from a common ancestral virus that jumped species and adapted to new hosts. Recently, canine distemper virus (CDV), a morbillivirus normally restricted to carnivores, caused disease outbreaks in nonhuman primates. Here, we report that experimental CDV infection of monkeys resulted in fever and leukopenia. The virus replicated to high levels in lymphocytes but did not spread to epithelial cells or the central nervous system. Importantly, like measles virus in macaques, the infections were self-limiting. In measles-vaccinated macaques CDV was cleared more rapidly, resulting in limited virus shedding from the upper respiratory tract. These studies demonstrate that although CDV can readily infect primates, measles immunity is protective, and CDV infection is self-limiting.

摘要

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麻疹病毒 (MV) 正被考虑用于全球根除,这可能会降低对 MV 疫苗接种的依从性。因此,儿童将在没有 MV 特异性免疫的情况下成长,为密切相关的动物麻疹病毒(如犬瘟热病毒(CDV))创造潜在的利基。自然 CDV 感染引起临床症状从未在人类中报告过,但最近在圈养猕猴中的暴发表明 CDV 可导致灵长类动物患病。我们研究了在无经验和麻疹疫苗接种的食蟹猕猴中表达增强型绿色荧光蛋白的重组 CDV 的毒力和嗜性。在无经验的动物中,CDV 引起病毒血症和发热,并主要感染 CD150(+)淋巴细胞和树突状细胞。病毒从上呼吸道和下呼吸道中分离出来,但在检查的时间点未检测到上皮或神经元细胞的感染,感染是自限性的。这表明 CDV 很容易感染非人类灵长类动物,但表明需要额外的突变才能在非天然宿主中实现完全毒力。在麻疹疫苗接种的猕猴中观察到对 CDV 的部分保护,这表现为病毒复制的加速控制和上呼吸道脱落的减少。虽然 CDV 感染或麻疹疫苗接种都没有诱导出可检测的交叉反应性中和抗体,但麻疹疫苗接种猕猴的 MV 特异性中和抗体水平在 CDV 挑战感染后得到了增强,表明存在交叉反应性 VN 表位。在 CDV 挑战后,麻疹疫苗接种的猕猴白细胞计数迅速增加,表明存在交叉反应性细胞免疫反应。这项研究表明,动物麻疹病毒感染可以通过麻疹疫苗接种来控制。

重要性

纵观历史,病毒性人畜共患病对人类健康产生了重大影响。鉴于全球根除麻疹的努力,了解动物麻疹病毒的人畜共患潜力至关重要。麻疹病毒被认为是从一种共同的祖先病毒进化而来的,该病毒跨越了物种并适应了新的宿主。最近,犬瘟热病毒(CDV),一种通常局限于食肉动物的麻疹病毒,在非人类灵长类动物中引起了疾病暴发。在这里,我们报告说,实验性 CDV 感染猴子会导致发热和白细胞减少。该病毒在淋巴细胞中复制到很高的水平,但不会扩散到上皮细胞或中枢神经系统。重要的是,与麻疹病毒在猕猴中一样,感染是自限性的。在麻疹疫苗接种的猕猴中,CDV 被更迅速地清除,导致上呼吸道病毒脱落减少。这些研究表明,尽管 CDV 可以轻易感染灵长类动物,但麻疹免疫力具有保护作用,并且 CDV 感染是自限性的。