Comprehensive Intrinsic Disorder Analysis of 6108 Viral Proteomes: From the Extent of Intrinsic Disorder Penetrance to Functional Annotation of Disordered Viral Proteins

Authors

Naveen Kumar, ICAR- National Institute of High Security Animal Diseases
Rahul Kaushik, Laboratory for Structural Bioinformatics, Center for Biosystems Dynamics Research, RIKEN
Chandana Tennakoon, The Pirbright Institute, Woking GU24 0NF, UK
Vladimir N. Uversky, University of South FloridaFollow
Sonia Longhi, Aix Marseille Univ and CNRS,
Kam Y. Zhang, Laboratory for Structural Bioinformatics, Center for Biosystems Dynamics Research, RIKEN
Sandeep Bhatia, ICAR- National Institute of High Security Animal Diseases

Document Type

Article

Publication Date

2021

Keywords

intrinsically disordered proteins, viruses, gene ontology, post-translational modifications, subcellular localization

Digital Object Identifier (DOI)

https://doi.org/10.1021/acs.jproteome.1c00011

Abstract

Much of our understanding of proteins and proteomes comes from the traditional protein structure–function paradigm. However, in the last 2 decades, both computational and experimental studies have provided evidence that a large fraction of functional proteomes across different domains of life consists of intrinsically disordered proteins, thus triggering a quest to unravel and decipher protein intrinsic disorder. Unlike structured/ordered proteins, intrinsically disordered proteins/regions (IDPs/IDRs) do not possess a well-defined structure under physiological conditions and exist as highly dynamic conformational ensembles. In spite of this peculiarity, these proteins have crucial roles in cell signaling and regulation. To date, studies on the abundance and function of IDPs/IDRs in viruses are rather limited. To fill this gap, we carried out an extensive and thorough bioinformatics analysis of 283 000 proteins from 6108 reference viral proteomes. We analyzed protein intrinsic disorder from multiple perspectives, such as abundance of IDPs/IDRs across diverse virus types, their functional annotations, and subcellular localization in taxonomically divergent hosts. We show that the content of IDPs/IDRs in viral proteomes varies broadly as a function of virus genome types and taxonomically divergent hosts. We have combined the two most commonly used and accurate IDP predictors’ results with charge-hydropathy (CH) versus cumulative distribution function (CDF) plots to categorize the viral proteins according to their IDR content and physicochemical properties. Mapping of gene ontology on the disorder content of viral proteins reveals that IDPs are primarily involved in key virus–host interactions and host antiviral immune response downregulation, which are reinforced by the post-translational modifications tied to disorder-enriched viral proteins. The present study offers detailed insights into the prevalence of the intrinsic disorder in viral proteomes and provides appealing targets for the design of novel therapeutics.

Was this content written or created while at USF?

Yes

Citation / Publisher Attribution

American Chemical Society, v. 20, issue 5, p. 2704-2713

Scholar Commons Citation

Kumar, Naveen; Kaushik, Rahul; Tennakoon, Chandana; Uversky, Vladimir N.; Longhi, Sonia; Zhang, Kam Y.; and Bhatia, Sandeep, "Comprehensive Intrinsic Disorder Analysis of 6108 Viral Proteomes: From the Extent of Intrinsic Disorder Penetrance to Functional Annotation of Disordered Viral Proteins" (2021). Molecular Medicine Faculty Publications. 187.
https://digitalcommons.usf.edu/mme_facpub/187