Avoiding Regions Symptomatic of Conformational and Functional Flexibility to Identify Antiviral Targets in Current and Future Coronaviruses

Jordon Rahaman; Jessica Siltberg-Liberles

doi:10.1093/gbe/evw246

Avoiding Regions Symptomatic of Conformational and Functional Flexibility to Identify Antiviral Targets in Current and Future Coronaviruses

Genome Biol Evol. 2016 Dec 31;8(11):3471-3484. doi: 10.1093/gbe/evw246.

Authors

Jordon Rahaman¹, Jessica Siltberg-Liberles^{2

3}

Affiliations

¹ Department of Biological Sciences, Florida International University, Miami, FL.
² Department of Biological Sciences, Florida International University, Miami, FL jliberle@fiu.edu.
³ Department of Biological Sciences, Biomolecular Sciences Institute, Florida International University, Miami, FL.

Abstract

Within the last 15 years, two related coronaviruses (Severe Acute Respiratory Syndrome [SARS]-CoV and Middle East Respiratory Syndrome [MERS]-CoV) expanded their host range to include humans, with increased virulence in their new host. Coronaviruses were recently found to have little intrinsic disorder compared with many other virus families. Because intrinsically disordered regions have been proposed to be important for rewiring interactions between virus and host, we investigated the conservation of intrinsic disorder and secondary structure in coronaviruses in an evolutionary context. We found that regions of intrinsic disorder are rarely conserved among different coronavirus protein families, with the primary exception of the nucleocapsid. Also, secondary structure predictions are only conserved across 50-80% of sites for most protein families, with the implication that 20-50% of sites do not have conserved secondary structure prediction. Furthermore, nonconserved structure sites are significantly less constrained in sequence divergence than either sites conserved in the secondary structure or sites conserved in loop. Avoiding regions symptomatic of conformational flexibility such as disordered sites and sites with nonconserved secondary structure to identify potential broad-specificity antiviral targets, only one sequence motif (five residues or longer) remains from the >10,000 starting sites across all coronaviruses in this study. The identified sequence motif is found within the nonstructural protein (NSP) 12 and constitutes an antiviral target potentially effective against the present day and future coronaviruses. On shorter evolutionary timescales, the SARS and MERS clades have more sequence motifs fulfilling the criteria applied. Interestingly, many motifs map to NSP12 making this a prime target for coronavirus antivirals.

Keywords: Coronavirus; MERS-CoV; divergence; evolution; evolutionary dynamics; structural disorder.

MeSH terms

Antiviral Agents / pharmacology
Binding Sites
Conserved Sequence
Evolution, Molecular
Genome, Viral
Intrinsically Disordered Proteins / chemistry
Intrinsically Disordered Proteins / genetics*
Middle East Respiratory Syndrome Coronavirus / drug effects
Middle East Respiratory Syndrome Coronavirus / genetics*
Nucleotide Motifs*
Protein Binding
Severe acute respiratory syndrome-related coronavirus / drug effects
Severe acute respiratory syndrome-related coronavirus / genetics*
Viral Proteins / chemistry
Viral Proteins / genetics*

Substances

Antiviral Agents
Intrinsically Disordered Proteins
Viral Proteins