A virally encoded high-resolution screen of cytomegalovirus dependencies

Genetic screens have transformed our ability to interrogate cellular factor requirements for viral infections 1 , 2 , but most current approaches are limited in their sensitivity, biased towards early stages of infection and provide only simplistic phenotypic information that is often based on survi...

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Veröffentlicht in:Nature (London) 2024-06, Vol.630 (8017), p.712-719
Hauptverfasser: Finkel, Yaara, Nachshon, Aharon, Aharon, Einav, Arazi, Tamar, Simonovsky, Elena, Dobešová, Martina, Saud, Zack, Gluck, Avi, Fisher, Tal, Stanton, Richard J., Schwartz, Michal, Stern-Ginossar, Noam
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Sprache:eng
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Zusammenfassung:Genetic screens have transformed our ability to interrogate cellular factor requirements for viral infections 1 , 2 , but most current approaches are limited in their sensitivity, biased towards early stages of infection and provide only simplistic phenotypic information that is often based on survival of infected cells 2 – 4 . Here, by engineering human cytomegalovirus to express single guide RNA libraries directly from the viral genome, we developed virus-encoded CRISPR-based direct readout screening (VECOS), a sensitive, versatile, viral-centric approach that enables profiling of different stages of viral infection in a pooled format. Using this approach, we identified hundreds of host dependency and restriction factors and quantified their direct effects on viral genome replication, viral particle secretion and infectiousness of secreted particles, providing a multi-dimensional perspective on virus–host interactions. These high-resolution measurements reveal that perturbations altering late stages in the life cycle of human cytomegalovirus (HCMV) mostly regulate viral particle quality rather than quantity, establishing correct virion assembly as a critical stage that is heavily reliant on virus–host interactions. Overall, VECOS facilitates systematic high-resolution dissection of the role of human proteins during the infection cycle, providing a roadmap for in-depth study of host–herpesvirus interactions. A genetic screen that expresses single guide RNA libraries targeting host genes in the human cytomegalovirus genome enables identification of host factors and provides insights into their roles during the viral replication cycle.
ISSN:0028-0836
1476-4687
1476-4687
DOI:10.1038/s41586-024-07503-z