Evolving ribonucleocapsid assembly/packaging signals in the genomes of the human and animal coronaviruses: targeting, transmission and evolution
Vladimir R. Chechetkin, Vasily V. Lobzin

TL;DR
This study compares the evolution and distribution of ribonucleocapsid assembly signals across human and animal coronaviruses, revealing conserved motifs that could serve as therapeutic targets and insights into virus transmission and evolution.
Contribution
It provides a comprehensive comparative analysis of RNAPS in coronaviruses, identifying conserved motifs and their potential as therapeutic targets, advancing understanding of coronavirus evolution and transmission.
Findings
RNAPS are distributed quasi-periodically with a ~54 nt period.
Distribution of motifs correlates with known packaging signals.
Many motifs are highly conserved across coronavirus lineages.
Abstract
A world-wide COVID-19 pandemic intensified strongly the studies of molecular mechanisms related to the coronaviruses. The origin of coronaviruses and the risks of human-to-human, animal-to-human, and human-to-animal transmission of coronaviral infections can be understood only on a broader evolutionary level by detailed comparative studies. In this paper, we studied ribonucleocapsid assembly-packaging signals (RNAPS) in the genomes of all seven known pathogenic human coronaviruses, SARS-CoV, SARS-CoV-2, MERS-CoV, HCoV-OC43, HCoV-HKU1, HCoV-229E, and HCoV-NL63 and compared them with RNAPS in the genomes of the related animal coronaviruses including SARS-Bat-CoV, MERS-Camel-CoV, MHV, Bat-CoV MOP1, TGEV, and one of camel alphacoronaviruses. RNAPS in the genomes of coronaviruses were evolved due to weakly specific interactions between genomic RNA and N proteins in helical nucleocapsids.…
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