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Characterizing the Different Effects of Zika Virus Infection in Placenta and Microglia Cells

机译:表征寨卡病毒感染在胎盘和小胶质细胞中的不同作用

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摘要

Zika virus (ZIKV) is a neuropathic virus that causes serious neurological abnormalities such as Guillain-Barre syndrome in adults and congenital Zika syndrome (CZS) in fetuses, which makes it an important concern for global human health. A catalogue of cells that support ZIKV replication, pathogenesis, and/or the persistence of the virus still remains unknown. Here, we studied the behavior of the virus in human placenta (JEG-3) and human microglia (HMC3) cell lines in order to better understand how different host tissues respond during infection. We quantified the host transcriptional response to ZIKV infection in both types of cells at 24 and 72 h post-infection. A panel of 84 genes that are involved in the innate or adaptive immune responses was used to quantify differential expression in both cell lines. HMC3 cells showed a unique set of significant differentially expressed genes (DEGs) compared with JEG-3 cells at both time points. Subsequent analysis of these data using modern pathway analysis methods revealed that the TLR7/8 pathway was strongly inhibited in HMC3 cells, while it was activated in JEG-3 cells during virus infection. The disruption of these pathways was subsequently confirmed with specific small interfering RNA (siRNA) experiments that characterize their role in the viral life cycle, and may partially explain why ZIKV infection in placental tissue contributes to extreme neurological problems in a developing fetus.
机译:寨卡病毒(ZIKV)是一种神经病性病毒,会引起严重的神经系统异常,例如成人的Guillain-Barre综合征和胎儿的先天性Zika综合征(CZS),这使其成为全球人类健康的重要关注点。支持ZIKV复制,发病机制和/或病毒持久性的细胞目录仍然未知。在这里,我们研究了病毒在人胎盘(JEG-3)和人小胶质细胞(HMC3)细胞系中的行为,以便更好地了解感染过程中不同宿主组织的反应。我们在感染后24小时和72小时对两种细胞中ZIKV感染的宿主转录反应进行了定量。与先天或适应性免疫应答有关的一组84个基因被用来量化两种细胞系中的差异表达。与两个时间点的JEG-3细胞相比,HMC3细胞显示出一组独特的显着差异表达基因(DEG)。使用现代途径分析方法对这些数据进行的后续分析表明,TLR7 / 8途径在HMC3细胞中受到强烈抑制,而在病毒感染期间在JEG-3细胞中被激活。随后,通过特定的小干扰RNA(siRNA)实验证实了这些途径的破坏,这些实验表征了它们在病毒生命周期中的作用,并可能部分解释了为什么胎盘组织中的ZIKV感染会导致胎儿发育中的极端神经系统问题。

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