Publication | Open Access
Musashi binding elements in Zika and related Flavivirus 3′UTRs: A comparative study in silico
21
Citations
77
References
2019
Year
Viral ReplicationGeneticsMolecular BiologyZika VirusVirus StructureArbovirusFlavivirus 3′UtrsRna Structure FormationVirus GeneViral GeneticsNeurovirologyVirologyGene ExpressionBioinformaticsComparative StudyFunctional GenomicsFlavivirusMolecular VirologyNatural SciencesPathogenesisRna FoldingMicrobiologySystems BiologyMedicine
Zika virus (ZIKV) belongs to a class of neurotropic viruses that have the ability to cause congenital infection, which can result in microcephaly or fetal demise. Recently, the RNA-binding protein Musashi-1 (Msi1), which mediates the maintenance and self-renewal of stem cells and acts as a translational regulator, has been associated with promoting ZIKV replication, neurotropism, and pathology. Msi1 predominantly binds to single-stranded motifs in the 3' untranslated region (UTR) of RNA that contain a UAG trinucleotide in their core. We systematically analyzed the properties of Musashi binding elements (MBEs) in the 3'UTR of flaviviruses with a thermodynamic model for RNA folding. Our results indicate that MBEs in ZIKV 3'UTRs occur predominantly in unpaired, single-stranded structural context, thus corroborating experimental observations by a biophysical model of RNA structure formation. Statistical analysis and comparison with related viruses show that ZIKV MBEs are maximally accessible among mosquito-borne flaviviruses. Our study addresses the broader question of whether other emerging arboviruses can cause similar neurotropic effects through the same mechanism in the developing fetus by establishing a link between the biophysical properties of viral RNA and teratogenicity. Moreover, our thermodynamic model can explain recent experimental findings and predict the Msi1-related neurotropic potential of other viruses.
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