Epistatic interactions promote persistence of NS3-Q80K in HCV infection by compensating for protein folding instability.

Georg Dultz,Sanjay Kumar Srikakulam,Michael Konetschnik,Tetsuro Shimakami,Nadezhda Tsankova Doncheva,Julia Dietz,Christoph Sarrazin,Ricardo M. Biondi,Stefan Zeuzem,Robert Tampé,Olga V. Kalinina,Christoph Welsch

Epistatic interactions promote persistence of NS3-Q80K in HCV infection by compensating for protein folding instability.

2021

Georg Dultz
Sanjay Kumar Srikakulam
Michael Konetschnik
Tetsuro Shimakami
Nadezhda Tsankova Doncheva
Julia Dietz
Christoph Sarrazin
Ricardo M. Biondi
Stefan Zeuzem
Robert Tampé
Olga V. Kalinina
Christoph Welsch

The Q80K polymorphism in the NS3-4A protease of the hepatitis C virus is associated with treatment failure of direct-acting antiviral agents. This polymorphism is highly prevalent in genotype 1a infections and stably transmitted between hosts. Here, we investigated the underlying molecular mechanisms of evolutionarily conserved coevolving amino acids in NS3-Q80K and revealed potential implications of epistatic interactions in immune escape and variants persistence. Using purified protein, we characterized the impact of epistatic amino acid substitutions on the physicochemical properties and peptide cleavage kinetics of the NS3-Q80K protease. We found that Q80K destabilized the protease protein fold (p

Keywords:

Protein folding
NS3
protease inhibitor
Amino acid
Resistance mutation
Hepatitis C virus
Epistasis
Genetics
Protease
Biology

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