Birth of new protein folds and functions in the virome

Summary Rapid virus evolution generates proteins essential to infectivity and replication but with unknown function due to extreme sequence divergence 1 . Using a database of 67,715 newly predicted protein structures from 4,463 eukaryotic viral species, we found that 62% of viral proteins are evolutionarily young and lack homologs in the Alphafold database 2,3 . Among the 38% of more ancient viral proteins, many have non-viral structural homologs that revealed surprising similarities between human pathogens and their eukaryotic hosts. Structural comparisons suggested putative functions for >25% of unannotated viral proteins, including those with roles in the evasion of innate immunity. In particular, RNA ligase T- (ligT) like phosphodiesterases were found to resemble phage-encoded proteins that hydrolyze the host immune-activating cyclic dinucleotides 3’3’ and 2’3’ cyclic G-A monophosphate (cGAMP). Experimental analysis showed that ligT homologs encoded by avian poxviruses likewise hydrolyze 2’3’ cGAMP, showing that ligT-mediated targeting of cGAMP is an evolutionarily conserved mechanism of immune evasion present in both bacteriophage and eukaryotic viruses. Together, the viral protein structural database and analytics presented here afford new opportunities to identify mechanisms of virus-host interactions that are common across the virome.