Compositional diversity and evolutionary pattern of coronavirus accessory proteins

Accessory proteins play important roles in the interaction between coronaviruses and their hosts. Accordingly, a comprehensive study of the compositional diversity and evolutionary patterns of accessory proteins is critical to understanding the host adaptation and epidemic variation of coronaviruses. Here, we developed a standardized genome annotation tool for coronavirus (CoroAnnoter) by combining open reading frame prediction, transcription regulatory sequence recognition and homologous alignment. Using CoroAnnoter, we annotated 39 representative coronavirus strains to form a compositional profile for all of the accessary proteins. Large variations were observed in the number of accessory proteins of 1-10 for different coronaviruses, with SARS-CoV-2 and SARS-CoV having the most (9 and 10, respectively). The variation between SARS-CoV and SARS-CoV-2 accessory proteins could be traced back to related coronaviruses in other hosts. The genomic distribution of accessory proteins had significant intra-genus conservation and inter-genus diversity and could be grouped into 1, 4, 2 and 1 types for alpha-, beta-, gamma-, and delta-coronaviruses, respectively. Evolutionary analysis suggested that accessory proteins are more conservative locating before the N-terminal of proteins E and M (E-M), while they are more diverse after these proteins. Furthermore, comparison of virus-host interaction networks of SARS-CoV-2 and SARS-CoV accessory proteins showed that they share multiple antiviral signaling pathways, those involved in the apoptotic process, viral life cycle and response to oxidative stress. In summary, our study provides a tool for coronavirus genome annotation and builds a comprehensive profile for coronavirus accessory proteins covering their composition, classification, evolutionary pattern and host interaction.

Automated summary

Accessory proteins play crucial roles in coronavirus-host interactions. A standardized genome annotation tool, CoroAnnoter, was developed to study the composition, evolutionary patterns, and host interactions of accessory proteins in coronaviruses. Variations in the number of accessory proteins were observed among different coronaviruses, with SARS-CoV-2 and SARS-CoV having the most. Evolutionary analysis revealed conservation and diversity in the distribution of accessory proteins within and between different genera of coronaviruses. Additionally, comparison of virus-host interaction networks of SARS-CoV-2 and SARS-CoV accessory proteins showed shared antiviral signaling pathways and biological processes.