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非洲和亚洲的寨卡病毒分离株在体外和体内均表现出表型差异。

African and Asian Zika Virus Isolates Display Phenotypic Differences Both In Vitro and In Vivo.

机构信息

Virology Division, United States Army Medical Research Institute of Infectious Diseases, Frederick, Maryland.

Diagnostics Systems Division, United States Army Medical Research Institute of Infectious Diseases, Frederick, Maryland.

出版信息

Am J Trop Med Hyg. 2018 Feb;98(2):432-444. doi: 10.4269/ajtmh.17-0685. Epub 2017 Dec 21.

Abstract

Zika virus (ZIKV) is a mosquito-borne member of the genus that has emerged since 2007 to cause outbreaks in Africa, Asia, Oceania, and most recently, in the Americas. Here, we used an isolate history as well as genetic and phylogenetic analyses to characterize three low-passage isolates representing African (ArD 41525) and Asian (CPC-0740, SV0127-14) lineages to investigate the potential phenotypic differences in vitro and in vivo. The African isolate displayed a large plaque phenotype (∼3-4 mm) on Vero and HEK-293 cells, whereas the Asian isolates either exhibited a small plaque phenotype (∼1-2 mm) or did not produce any plaques. In multistep replication kinetics in nine different vertebrate and insect cell lines, the African isolate consistently displayed faster replication kinetics and yielded ∼10- to 10,000-fold higher peak virus titers (infectious or RNA copies) compared with the Asian isolates. Oral exposure of mosquitoes with the African isolate yielded higher infection and dissemination rates compared with the Asian isolates. Infection of mice with the African isolate produced a uniformly fatal disease, whereas infection with the Asian isolates produced either a delay in time-to-death or a significantly lower mortality rate. Last, the African isolate was > 10,000-fold more virulent than the Asian isolates in an interferon type I antibody blockade mouse model. These data demonstrate substantial phenotypic differences between low-passage African and Asian isolates both in vitro and in vivo and warrant further investigation. They also highlight the need for basic characterization of ZIKV isolates, as the utilization of the uncharacterized isolates could have consequences for animal model and therapeutic/vaccine development.

摘要

寨卡病毒(ZIKV)是一种虫媒病毒,属于黄病毒属,自 2007 年以来出现,在非洲、亚洲、大洋洲以及最近的美洲引发了疫情。在这里,我们使用分离株历史以及遗传和系统发育分析来描述三个低传代分离株,代表非洲(ArD 41525)和亚洲(CPC-0740、SV0127-14)谱系,以研究体外和体内的潜在表型差异。非洲分离株在 Vero 和 HEK-293 细胞上表现出大斑块表型(3-4mm),而亚洲分离株要么表现出小斑块表型(1-2mm),要么不产生任何斑块。在九种不同的脊椎动物和昆虫细胞系中的多步复制动力学中,非洲分离株始终表现出更快的复制动力学,并且与亚洲分离株相比,产生了~10-到 10000 倍更高的峰值病毒滴度(感染性或 RNA 拷贝)。与亚洲分离株相比,用非洲分离株对 蚊子进行口服暴露导致更高的感染和传播率。用非洲分离株感染 小鼠会导致均匀致命的疾病,而用亚洲分离株感染则会导致延迟死亡时间或死亡率显著降低。最后,在干扰素 I 型抗体阻断小鼠模型中,非洲分离株的毒力比亚洲分离株高 10000 倍以上。这些数据表明,在体外和体内,低传代的非洲和亚洲分离株之间存在显著的表型差异,需要进一步研究。它们还强调了对寨卡病毒分离株进行基本特征描述的必要性,因为使用未特征化的分离株可能会对动物模型和治疗/疫苗开发产生影响。

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