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Título
A Single Amino Acid Substitution in the Novel H7N9 Influenza A Virus NS1 Protein Increases CPSF30 Binding and Virulence
Autor
Publicado en
Journal of Virology. 2014, V. 88, n. 20, p. 12146-12151
Editorial
American Society for Microbiology
Fecha de publicación
2014
ISSN
0022-538X
DOI
10.1128/JVI.01567-14
Abstract
Although an effective interferon antagonist in human and avian cells, the novel H7N9 influenza virus NS1 protein is defective at inhibiting CPSF30. An I106M substitution in H7N9 NS1 can restore CPSF30 binding together with the ability to block host gene expression. Furthermore, a recombinant virus expressing H7N9 NS1-I106M replicates to higher titers in vivo, and is subtly more virulent, than the parental virus. Natural polymorphisms in H7N9 NS1 that enhance CPSF30 binding may be cause for concern.
Materia
Medicina
Medicine
Microbiología
Microbiology
Salud
Health
Enfermedades infecciosas
Communicable diseases
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