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A Short Double-Stapled Peptide Inhibits Respiratory Syncytial Virus Entry and Spreading.

Antimicrob. Agents Chemother.. 2017; 
GaillardVanessa,GallouxMarie,GarcinDominique,EléouëtJean-François,Le GofficRonan,LarcherThibaut,Rameix-WeltiMarie-Anne,BoukadiriAbdelhak,HéritierJulien,SeguraJean-Manuel,BaechlerElodie,ArrellMiriam,Mottet-OsmanGeneviève,NyanguileOrig
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摘要

Synthetic peptides derived from the heptad repeat (HR) of fusion (F) proteins can be used as dominant negative inhibitors to inhibit the fusion mechanism of class I viral F proteins. Here, we have performed a stapled-peptide scan across the HR2 domain of the respiratory syncytial virus (RSV) F protein with the aim to identify a minimal domain capable of disrupting the formation of the postfusion six-helix bundle required for viral cell entry. Constraining the peptides with a single staple was not sufficient to inhibit RSV infection. However, the insertion of double staples led to the identification of novel short stapled peptides that display nanomolar potency in HEp-2 cells and are exceptionally robust to ... More

关键词

respiratory syncytial virus,stapled pept