Recombination Located over 2A-2B Junction Ribosome Frameshifting Region of Saffold Cardiovirus

Recombination Located over 2A-2B Junction Ribosome Frameshifting Region of Saffold Cardiovirus

Here we report the nearly full-length genome of a recombinant Saffold virus strain (SAFV-BR-193) isolated from a child with acute gastroenteritis. Evolutionary analysis performed using all available near-full length Saffold picornavirus genomes showed that the breakpoint found in the Brazilian strai...

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Veröffentlicht in:Viruses 2018-09, Vol.10 (10), p.520
Hauptverfasser: da Costa, Antônio Charlys, Luchs, Adriana, Milagres, Flávio Augusto de Pádua, Komninakis, Shirley Vasconcelos, Gill, Danielle Elise, Lobato, Márcia Cristina Alves Brito Sayão, Brustulin, Rafael, das Chagas, Rogério Togisaki, Abrão, Maria de Fátima Neves Dos Santos, Soares, Cassia Vitória de Deus Alves, Deng, Xutao, Sabino, Ester Cerdeira, Delwart, Eric, Leal, Élcio
Format: Artikel
Sprache:eng
Schlagworte:
Acute Disease
Brazil
cardiovirus
Cardiovirus - genetics
Cardiovirus Infections - virology
Child, Preschool
Feces - virology
Frameshifting, Ribosomal - genetics
Gastroenteritis - virology
Genome, Viral - genetics
GGUUUUU motif
Humans
Phylogeny
picornavirus
Recombination, Genetic - genetics
ribosomal frameshifting
RNA Replicase - genetics
RNA-dependent RNA-polymerase
saffold virus
Sequence Alignment
virome
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Zusammenfassung:Here we report the nearly full-length genome of a recombinant Saffold virus strain (SAFV-BR-193) isolated from a child with acute gastroenteritis. Evolutionary analysis performed using all available near-full length Saffold picornavirus genomes showed that the breakpoint found in the Brazilian strain (SAFV-BR-193) is indeed a recombination hotspot. Notably, this hotspot is located just one nucleotide after the ribosomal frameshift GGUUUUU motif in the SAFV genome. Empirical studies will be necessary to determine if this motif also affects the binding affinity of RNA-dependent RNA-polymerase (RdRp) and therefore increases the changes of RdRp swap between molecules during the synthesis of viral genomes.
ISSN:1999-4915
1999-4915
DOI:10.3390/v10100520