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Basic Characteristics of Mutations
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Mutation Site
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Y93H |
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Mutation Site Sentence
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In addition, a genotype 1b HCV-SGR, containing the L31V and Y93H substitutions, which confer high-level resistance to ledipasvir (714-fold increase in the LDV EC50 [data not shown]), remained fully sensitive to C31 and ALV (Table 2). |
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Mutation Level
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Amino acid level |
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Mutation Type
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Nonsynonymous substitution |
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Gene/Protein/Region
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NS5A |
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Standardized Encoding Gene
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NS5A
|
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Genotype/Subtype
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1b |
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Viral Reference
|
-
|
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Functional Impact and Mechanisms
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|
Disease
|
Cell line
|
|
Immune
|
- |
|
Target Gene
|
-
|
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Clinical and Epidemiological Correlations
|
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Clinical Information
|
- |
|
Treatment
|
LDV |
|
Location
|
- |
|
Literature Information
|
|
PMID
|
29760125
|
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Title
|
Characterization of the Anti-Hepatitis C Virus Activity of New Nonpeptidic Small-Molecule Cyclophilin Inhibitors with the Potential for Broad Anti-Flaviviridae Activity
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Author
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Nevers Q,Ruiz I,Ahnou N,Donati F,Brillet R,Softic L,Chazal M,Jouvenet N,Fourati S,Baudesson C,Bruscella P,Gelin M,Guichou JF,Pawlotsky JM,Ahmed-Belkacem A
|
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Journal
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Antimicrobial agents and chemotherapy
|
|
Journal Info
|
2018 Jun 26;62(7):e00126-18
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Abstract
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Although members of the Flaviviridae display high incidence, morbidity, and mortality rates, the development of specific antiviral drugs for each virus is unlikely. Cyclophilins, a family of host peptidyl-prolyl cis-trans isomerases (PPIases), play a pivotal role in the life cycles of many viruses and therefore represent an attractive target for broad-spectrum antiviral development. We report here the pangenotypic anti-hepatitis C virus (HCV) activity of a small-molecule cyclophilin inhibitor (SMCypI). Mechanistic and modeling studies revealed that the SMCypI bound to cyclophilin A in competition with cyclosporine (CsA), inhibited its PPIase activity, and disrupted the CypA-nonstructural protein 5A (NS5A) interaction. Resistance selection showed that the lead SMCypI hardly selected amino acid substitutions conferring low-level or no resistance in vitro Interestingly, the SMCypI selected D320E and Y321H substitutions, located in domain II of the NS5A protein. These substitutions were previously associated with low-level resistance to cyclophilin inhibitors such as alisporivir. Finally, the SMCypI inhibited the replication of other members of the Flaviviridae family with higher 50% effective concentrations (EC(50)s) than for HCV. Thus, because of its chemical plasticity and simplicity of synthesis, our new family of SMCypIs represents a promising new class of drugs with the potential for broad-spectrum anti-Flaviviridae activity as well as an invaluable tool to explore the role of cyclophilins in viral life cycles.
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Sequence Data
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-
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