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Antagonism of STAT1 by Nipah virus P gene products modulates disease course but not lethal outcome in the ferret model.

Sci Rep. 2019; 
Satterfield Benjamin A,Borisevich Viktoriya,Foster Stephanie L,Rodriguez Sergio E,Cross Robert W,Fenton Karla A,Agans Krystle N,Basler Christopher F,Geisbert Thomas W,Mire Ch
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Catalog Antibody The antisera were produced by GenScript (Piscataway, NJ) as described previously20 diluted in TTBS with 5% milk (P: 1:5,000; V: 1:500; W: 1:500) for 1 hour at room temperature, and washed 4 times in TTBS.  Get A Quote

摘要

Nipah virus (NiV) is a pathogenic paramyxovirus and zoononis with very high human fatality rates. Previous protein over-expression studies have shown that various mutations to the common N-terminal STAT1-binding motif of the NiV P, V, and W proteins affected the STAT1-binding ability of these proteins thus interfering with he JAK/STAT pathway and reducing their ability to inhibit type-I IFN signaling, but due to differing techniques it was unclear which amino acids were most important in this interaction or what impact this had on pathogenesis in vivo. We compared all previously described mutations in parallel and found the amino acid mutation Y116E demonstrated the greatest reduction in binding to STAT1 ... More

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