Literature DB >> 31873071

Human cytomegalovirus interactome analysis identifies degradation hubs, domain associations and viral protein functions.

Luis V Nobre1, Katie Nightingale1, Benjamin J Ravenhill1, Robin Antrobus1, Lior Soday1, Jenna Nichols2, James A Davies3, Sepehr Seirafian3, Eddie Cy Wang3, Andrew J Davison2, Gavin Wg Wilkinson3, Richard J Stanton3, Edward L Huttlin4, Michael P Weekes1.   

Abstract

Human cytomegalovirus (HCMV) extensively modulates host cells, downregulating >900 human proteins during viral replication and degrading ≥133 proteins shortly after infection. The mechanism of degradation of most host proteins remains unresolved, and the functions of many viral proteins are incompletely characterised. We performed a mass spectrometry-based interactome analysis of 169 tagged, stably-expressed canonical strain Merlin HCMV proteins, and two non-canonical HCMV proteins, in infected cells. This identified a network of >3400 virus-host and >150 virus-virus protein interactions, providing insights into functions for multiple viral genes. Domain analysis predicted binding of the viral UL25 protein to SH3 domains of NCK Adaptor Protein-1. Viral interacting proteins were identified for 31/133 degraded host targets. Finally, the uncharacterised, non-canonical ORFL147C protein was found to interact with elements of the mRNA splicing machinery, and a mutational study suggested its importance in viral replication. The interactome data will be important for future studies of herpesvirus infection.
© 2019, Nobre et al.

Entities:  

Keywords:  computational biology; host-pathogen interaction; human; human cytomegalovirus; immune evasion; infectious disease; microbiology; protein-protein interaction; proteomics; systems biology; systems virology; virus

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Year:  2019        PMID: 31873071      PMCID: PMC6959991          DOI: 10.7554/eLife.49894

Source DB:  PubMed          Journal:  Elife        ISSN: 2050-084X            Impact factor:   8.140


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