HSV-1 single-cell analysis reveals the activation of anti-viral and developmental programs in distinct sub-populations

生物 病毒复制 重编程 人口 病毒学 单纯疱疹病毒 固有免疫 病毒释放 干扰素 病毒 基因表达 基因 胚胎干细胞 病毒进入 细胞 细胞生物学 遗传学 免疫系统 先天免疫系统 人口学 社会学
作者
Nir Drayman,Parthiv Patel,Luke Vistain,Savaş Tay
出处
期刊:eLife [eLife Sciences Publications Ltd]
卷期号:8 被引量:144
标识
DOI:10.7554/elife.46339
摘要

Viral infection is usually studied at the population level by averaging over millions of cells. However, infection at the single-cell level is highly heterogeneous, with most infected cells giving rise to no or few viral progeny while some cells produce thousands. Analysis of Herpes Simplex virus 1 (HSV-1) infection by population-averaged measurements has taught us a lot about the course of viral infection, but has also produced contradictory results, such as the concurrent activation and inhibition of type I interferon signaling during infection. Here, we combine live-cell imaging and single-cell RNA sequencing to characterize viral and host transcriptional heterogeneity during HSV-1 infection of primary human cells. We find extreme variability in the level of viral gene expression among individually infected cells and show that these cells cluster into transcriptionally distinct sub-populations. We find that anti-viral signaling is initiated in a rare group of abortively infected cells, while highly infected cells undergo cellular reprogramming to an embryonic-like transcriptional state. This reprogramming involves the recruitment of β-catenin to the host nucleus and viral replication compartments, and is required for late viral gene expression and progeny production. These findings uncover the transcriptional differences in cells with variable infection outcomes and shed new light on the manipulation of host pathways by HSV-1.

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