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Small molecule degraders of the hepatitis C virus protease reduce susceptibility to resistance mutations.

Nat Commun. 2019-08; 
de WispelaereMélissanne,DuGuangyan,DonovanKatherine A,ZhangTinghu,EleuteriNicholas A,YuanJingting C,KalabathulaJoann,NowakRados?aw P,FischerEric S,GrayNathanael S,YangPriscil
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Proteins, Expression, Isolation and Analysis Equal amounts of proteins were fractionated on a 4–20% polyacrylamide gel (GenScript) and transferred to a polyvinylidene difluoride membrane (MilliporeSigma IPVH00010) using the Trans-Blot Turbo Transfer System (Bio-Rad Laboratories). Get A Quote

摘要

Targeted protein degradation is a promising drug development paradigm. Here we leverage this strategy to develop a new class of small molecule antivirals that induce proteasomal degradation of viral proteins. Telaprevir, a reversible-covalent inhibitor that binds to the hepatitis C virus (HCV) protease active site is conjugated to ligands that recruit the CRL4 ligase complex, yielding compounds that can both inhibit and induce the degradation of the HCV NS3/4A protease. An optimized degrader, DGY-08-097, potently inhibits HCV in a cellular infection model, and we demonstrate that protein degradation contributes to its antiviral activity. Finally, we show that this new class of antiviral agents can o... More

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