Abstract
Retroviruses infect almost all vertebrates, from humans to domestic and farm animals, from primates to wild animals, where they cause severe diseases, including immunodeficiencies, neurological disorders, and cancer. Nonhuman retroviruses have also been recently associated with human diseases. To date, no effective treatments are available; therefore, finding retrovirus-specific therapeutic targets is becoming an impelling issue. G-Quadruplexes are four-stranded nucleic acid structures that form in guanine-rich regions. Highly conserved G-quadruplexes located in the long-terminal-repeat (LTR) promoter of HIV-1 were shown to modulate the virus transcription machinery; moreover, the astonishingly high degree of conservation of G-quadruplex sequences in all primate lentiviruses corroborates the idea that these noncanonical nucleic acid structures are crucial elements in the lentiviral biology and thus have been selected for during evolution. In this work, we aimed at investigating the presence and conservation of G-quadruplexes in the Retroviridae family. Genomewide bioinformatics analysis showed that, despite their documented high genetic variability, most retroviruses contain highly conserved putative G-quadruplex-forming sequences in their promoter regions. Biophysical and biomolecular assays proved that these sequences actually fold into G-quadruplexes in physiological concentrations of relevant cations and that they are further stabilized by ligands. These results validate the relevance of G-quadruplexes in retroviruses and endorse the employment of G-quadruplex ligands as innovative antiretroviral drugs. This study indicates new possible pathways in the management of retroviral infections in humans and animal species. Moreover, it may shed light on the mechanism and functions of retrovirus genomes and derived transposable elements in the human genome.
Highlights
Retroviruses (RVs) are the most ancient known viruses: their origin dates back to more than 450 million years ago.[1]
Conserved G-quadruplexes located in the long-terminal-repeat (LTR) promoter of human immunodeficiency virus type 1 (HIV-1) were shown to modulate the virus transcription machinery; the astonishingly high degree of conservation of G-quadruplex sequences in all primate lentiviruses corroborates the idea that these noncanonical nucleic acid structures are crucial elements in the lentiviral biology and have been selected for during evolution
We initially investigated the presence of Putative Quadruplex-Forming Sequences (PQSs) in the full-length genomes of all RVs, with the exception of lentiviruses as that genus had been previously examined for the presence of G4s
Summary
Retroviruses (RVs) are the most ancient known viruses: their origin dates back to more than 450 million years ago.[1]. G4 correlation with transcription-factor binding sites suggests exploitation of structural conserved elements as mechanosensors in the regulation of key viral steps.[13] In general, bioinformatics studies traced putative G4-forming sequences (PQSs) in almost all human viruses: most of these viral PQSs are characterized by high degrees of conservation and statistically significant distributions, implying essential biological roles.[14] Altogether, these findings show that despite the large mutation rates of viruses, G4s represent key elements in the viral life cycle and are interesting targets in the development of innovative drugs In this context, with the purpose of examining the presence and role of G4s in the retroviral machinery and of identifying new targets for antiretroviral therapy, here we sought to investigate the G4 distribution and conservation in the whole Retroviridae family, and we present a comprehensive analysis of G4s within the RV genomes. Despite plentiful differences among RVs, G4s in regulatory regions represent a feature common to all genera
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