生物
清脆的
人巨细胞病毒
转录组
宿主因子
寄主(生物学)
病毒学
计算生物学
RNA干扰
功能基因组学
遗传学
基因
病毒
基因组学
基因表达
基因组
核糖核酸
作者
Marco Y. Hein,Jonathan S. Weissman
标识
DOI:10.1038/s41587-021-01059-3
摘要
Understanding how viral and host factors interact and how perturbations impact infection is the basis for designing antiviral interventions. Here we define the functional contribution of each viral and host factor involved in human cytomegalovirus infection in primary human fibroblasts through pooled CRISPR interference and nuclease screening. To determine how genetic perturbation of critical host and viral factors alters the timing, course and progression of infection, we applied Perturb-seq to record the transcriptomes of tens of thousands of CRISPR-modified single cells and found that, normally, most cells follow a stereotypical transcriptional trajectory. Perturbing critical host factors does not change the stereotypical transcriptional trajectory per se but can stall, delay or accelerate progression along the trajectory, allowing one to pinpoint the stage of infection at which host factors act. Conversely, perturbation of viral factors can create distinct, abortive trajectories. Our results reveal the roles of host and viral factors and provide a roadmap for the dissection of host–pathogen interactions. Pooled and single-cell CRISPR screens provide a detailed map of human cytomegalovirus infection.
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