Theiler's murine encephalomyelitis virus contrasts with encephalomyocarditis and foot-and-mouth disease viruses in its functional utilization of the StopGo non-standard translation mechanism

G. Loughran, J. E. Libbey, S. Uddowla, M. F. Scallan, M. D. Ryan, R. S. Fujinami, E. Rieder, J. F. Atkins*

*Corresponding author for this work

Research output: Contribution to journalArticlepeer-review

Abstract

The picornaviruses' genome consists of a positive-sense ssRNA. Like many picornaviruses, cardioviruses synthesize two distinct polyprotein precursors from adjacent but non-overlapping genome segments. Both the [L-1ABCD-2A] and the [2BC-3ABCD] polyproteins are proteolytically processed to yield mature capsid and non-structural proteins, respectively. An unusual translational event, known as 'StopGo' or 'Stop-Carry on', is responsible for the release of the [L-1ABCD-2A] polyprotein from the ribosome and synthesis of the N-terminal amino acid of the [2BC-3ABCD] polyprotein. A common feature of these viruses is the presence of a highly conserved signature sequence for StopGo: -D(V/I)ExNPG(down arrow) P-, where -D(V/I)ExNPG are the last 7 aa of 2A, and the last P- is the first amino acid of 2B. Here, we report that, in contrast to encephalomyocarditis virus and foot-and-mouth disease virus, a functional StopGo does not appear to be essential for Theiler's murine encephalomyelitis virus viability when tested in vitro and in vivo.

Original languageEnglish
Pages (from-to)348-353
Number of pages6
JournalJournal of General Virology
Volume94
DOIs
Publication statusPublished - Feb 2013

Keywords

  • CLEAVAGE ACTIVITIES
  • 2A-LIKE SEQUENCES
  • IN-VITRO
  • POLYPROTEIN
  • SITE
  • REGION
  • APHTHOVIRUS
  • PRECURSORS
  • CODON
  • MICE

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