AI Article Synopsis

  • The stability of foot-and-mouth disease virus (FMDV) is influenced by specific amino acid residues in its VP1 protein, particularly the N17D substitution.
  • Changes in charge at position VP1 17 affect the virus's resistance to acidic conditions, with negative charges enhancing stability while positive charges increase sensitivity.
  • The presence of viral RNA negatively impacts the stability of the virion, but this destabilizing effect can be mitigated by introducing certain negatively charged residues at position VP1 N17.

Article Abstract

Elucidation of the molecular basis of the stability of foot-and-mouth disease virus (FMDV) particles is relevant to understand key aspects of the virus cycle. Residue N17D in VP1, located at the capsid inner surface, modulates the resistance of FMDV virion to dissociation and inactivation at acidic pH. Here we have studied whether the virion-stabilizing effect of amino acid substitution VP1 N17D may be mediated by the alteration of electrostatic charge at this position and/or the presence of the viral RNA. Substitutions that either introduced a positive charge (R,K) or preserved neutrality (A) at position VP1 17 led to increased sensitivity of virions to inactivation at acidic pH, while replacement by negatively charged residues (D,E) increased the resistance of virions to acidic pH. The role in virion stability of viral RNA was addressed using FMDV empty capsids that have a virtually unchanged structure compared to the capsid in the RNA-filled virion, but that are considerably more resistant to acidic pH than WT virions, supporting a virion-destabilizing effect of the RNA. Remarkably, no differences were observed in the resistance to dissociation at acidic pH between the WT empty capsids and those harboring replacement N17D. Thus, the virion-destabilizing effect of viral RNA at acidic pH can be partially restored by introducing negatively charged residues at position VP1 N17.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6997383PMC
http://dx.doi.org/10.1038/s41598-020-58414-8DOI Listing

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