Asymmetric binding to NS5A by daclatasvir (BMS-790052) and analogs suggests two novel modes of HCV inhibition

James H Nettles; Richard A Stanton; Joshua Broyde; Franck Amblard; Hongwang Zhang; Longhu Zhou; Junxing Shi; Tamara R McBrayer; Tony Whitaker; Steven J Coats; James J Kohler; Raymond F Schinazi

doi:10.1021/jm501291c

Asymmetric binding to NS5A by daclatasvir (BMS-790052) and analogs suggests two novel modes of HCV inhibition

J Med Chem. 2014 Dec 11;57(23):10031-43. doi: 10.1021/jm501291c. Epub 2014 Nov 3.

Authors

James H Nettles¹, Richard A Stanton, Joshua Broyde, Franck Amblard, Hongwang Zhang, Longhu Zhou, Junxing Shi, Tamara R McBrayer, Tony Whitaker, Steven J Coats, James J Kohler, Raymond F Schinazi

Affiliation

¹ Center for AIDS Research, Department of Pediatrics, Emory University School of Medicine , Atlanta, Georgia 30322, United States.

Abstract

Symmetric, dimeric daclatasvir (BMS-790052) is the clinical lead for a class of picomolar inhibitors of HCV replication. While specific, resistance-bearing mutations at positions 31 and 93 of domain I strongly suggest the viral NS5A as target, structural mechanism(s) for the drugs' activities and resistance remains unclear. Several previous models suggested symmetric binding modes relative to the homodimeric target; however, none can fully explain SAR details for this class. We present semiautomated workflows to model potential receptor conformations for docking. Surprisingly, ranking docked hits with our library-derived 3D-pharmacophore revealed two distinct asymmetric binding modes, at a conserved poly-proline region between 31 and 93, consistent with SAR. Interfering with protein-protein interactions at this membrane interface can explain potent inhibition of replication-complex formation, resistance, effects on lipid droplet distribution, and virion release. These detailed interaction models and proposed mechanisms of action will allow structure-based design of new NS5A directed compounds with higher barriers to HCV resistance.

Publication types

Research Support, N.I.H., Extramural
Research Support, U.S. Gov't, Non-P.H.S.

MeSH terms

Amino Acid Sequence
Antiviral Agents / pharmacology
Carbamates
Hepacivirus / drug effects
Imidazoles / metabolism*
Imidazoles / pharmacology
Molecular Docking Simulation
Pyrrolidines
Sequence Alignment
Structure-Activity Relationship
Valine / analogs & derivatives
Viral Nonstructural Proteins / antagonists & inhibitors
Viral Nonstructural Proteins / metabolism*
Virus Replication / drug effects

Substances

Antiviral Agents
Carbamates
Imidazoles
Pyrrolidines
Viral Nonstructural Proteins
NS-5 protein, hepatitis C virus
Valine
daclatasvir

Abstract

Publication types

MeSH terms

Substances

Grants and funding