Tyrosine 110 in the measles virus phosphoprotein is required to block STAT1 phosphorylation

Tyrosine 110 in the measles virus phosphoprotein is required to block STAT1 phosphorylation

Abstract The measles virus (MV) P gene encodes three proteins: P, an essential polymerase cofactor, and C and V, which have multiple functions including immune evasion. We show here that the MV P protein also contributes to immune evasion, and that tyrosine 110 is required to block nuclear transloca...

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Veröffentlicht in:Virology (New York, N.Y.) N.Y.), 2007-03, Vol.360 (1), p.72-83
Hauptverfasser: Devaux, Patricia, von Messling, Veronika, Songsungthong, Warangkhana, Springfeld, Christoph, Cattaneo, Roberto
Format: Artikel
Sprache:eng
Schlagworte:
60 APPLIED LIFE SCIENCES
Animals
Base Sequence
Cell Nucleus - metabolism
Cercopithecus aethiops
GENES
HeLa Cells
Humans
IMMUNITY
Immunity, Innate
Infectious Disease
Innate immunity
INTERFERON
Interferon signaling
Interferon Type I - pharmacology
Measles - immunology
Measles - virology
MEASLES VIRUS
Measles virus - metabolism
Molecular Sequence Data
Phosphoprotein
PHOSPHOPROTEINS
Phosphoproteins - chemistry
Phosphoproteins - genetics
Phosphoproteins - metabolism
PHOSPHORYLATION
Phosphorylation - drug effects
POLYMERASES
Sequence Alignment
Signal Transduction
STAT1 Transcription Factor - metabolism
TRANSCRIPTION FACTORS
TRANSLOCATION
TYROSINE
Tyrosine - physiology
VACCINES
Vero Cells
Viral Proteins - chemistry
Viral Proteins - genetics
Viral Proteins - metabolism
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Zusammenfassung:Abstract The measles virus (MV) P gene encodes three proteins: P, an essential polymerase cofactor, and C and V, which have multiple functions including immune evasion. We show here that the MV P protein also contributes to immune evasion, and that tyrosine 110 is required to block nuclear translocation of the signal transducer and activator of transcription factors (STAT) after interferon type I treatment. In particular, MV P inhibits STAT1 phosphorylation. This is shown not only by transient expression but also by reverse genetic analyses based on a new functional infectious cDNA derived from a MV vaccine vial (Moraten strain). Our study also identifies a conserved sequence around P protein tyrosine 110 as a candidate interaction site with a cellular protein.
ISSN:0042-6822
1096-0341
DOI:10.1016/j.virol.2006.09.049