Potent hepatitis C inhibitors bind directly to NS5A and reduce its affinity for RNA

Ascher, David B.; Wielens, J.; Nero, Tracy L.; Doughty, Larissa; Morton, Craig J.; Parker, Michael W.

doi:10.1038/srep04765

Cited by 109 publications

(98 citation statements)

References 36 publications

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“…An additional report of direct binding to NS5A protein of DCV and the related compound ledipasvir also supports the direct association of NS5A RCIs with the NS5A protein (8). Immunomicroscopy analysis indicates that DCV binding results in the apparent disassociation of NS5A from the replication complex, consistent with other evidence that NS5A RCI binding has multiple effects (9-13).The use of functional NS5A affinity reagents (inhibitory crosslinkers, labeled NS5A proteins) and genetic variants has provided evidence for the presence of NS5A dimers and oligomers in cells, suggesting that NS5A-NS5A dimers may be necessary for HCV replication and NS5A function (7,14,15). Experiments using NS5A constructs tagged near domain 1 for binding of fluorescent labels detected a correlation between inhibitor activity and changes in fluorescent signal that is consistent with conformational changes in NS5A upon compound binding (14).…”

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confidence: 49%

“…A recent report (7) of DCV binding to Escherichia coli-expressed NS5A protein provided the first direct evidence that DCV binds to NS5A. The authors demonstrated that DCV binding can reduce the affinity of NS5A protein for viral RNA, supporting one potential mechanism of inhibition.…”

mentioning

confidence: 93%

“…The use of functional NS5A affinity reagents (inhibitory crosslinkers, labeled NS5A proteins) and genetic variants has provided evidence for the presence of NS5A dimers and oligomers in cells, suggesting that NS5A-NS5A dimers may be necessary for HCV replication and NS5A function (7,14,15). Experiments using NS5A constructs tagged near domain 1 for binding of fluorescent labels detected a correlation between inhibitor activity and changes in fluorescent signal that is consistent with conformational changes in NS5A upon compound binding (14).…”

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confidence: 98%

“…Experiments using NS5A constructs tagged near domain 1 for binding of fluorescent labels detected a correlation between inhibitor activity and changes in fluorescent signal that is consistent with conformational changes in NS5A upon compound binding (14). In addition, active compound immunoprecipitated more NS5A than an inactive analog, suggesting that binding of the inhibitor potentially stabilizes dimeric and higher-order NS5A multimers while modulating NS5A conformation.Computer-simulated docking of DCV to NS5A dimers has provided a framework for understanding the potency of DCV on different genotypes and the resistance variants selected by DCV monotherapy (7,9,16). A recent report of two additional crystal forms of NS5A domain 1 (gt 1a), together with the previously reported structures (17)(18)(19), suggests that NS5A domain 1 has…”

mentioning

confidence: 99%

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Synergistic Activity of Combined NS5A Inhibitors

O’Boyle

Nower

Gao

et al. 2016

Antimicrob Agents Chemother

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). To extend the characterization of NS5 A synergists, we tested new combinations of DCV and NS5A synergists against genotype (gt) 1 to 6 replicons and gt 1a, 2a, and 3a viruses. The kinetics of inhibition in HCV-infected cells treated with DCV, an NS5A synergist (NS5A-Syn), or a combination of DCV and NS5A-Syn were distinctive. Similar to activity observed clinically, DCV caused a multilog drop in HCV, followed by rebound due to the emergence of resistance. DCV-NS5A-Syn combinations were highly efficient at clearing cells of viruses, in line with the trend seen in replicon studies. The retreatment of resistant viruses that emerged using DCV monotherapy with DCV-NS5A-Syn resulted in a multilog drop and rebound in HCV similar to the initial decline and rebound observed with DCV alone on wild-type (WT) virus. A triple combination of DCV, NS5A-Syn, and a DAA targeting the NS3 or NS5B protein cleared the cells of viruses that are highly resistant to DCV. Our data support the observation that the cooperative interaction of DCV and NS5A-Syn potentiates both the genotype coverage and resistance barrier of DCV, offering an additional DAA option for combination therapy and tools for explorations of NS5A function. Hepatitis C virus (HCV) infections can be effectively cured using combinations of small-molecule direct-acting antivirals (DAAs) with different mechanisms of action. The nonstructural 5A replication complex inhibitor (NS5A RCI) class of compounds represented by daclatasvir (DCV) (BMS-790052, Daklinza; Bristol-Myers Squibb) has activity against genotypes (gts) 1a, 1b, 2a, 3a, 4a, 5a, and 6a and is the most potent class of HCV inhibitor yet described (1-3). NS3 protease inhibitors and NS5B polymerase inhibitors have thus far been the preferred DAA partners for DCV combination therapies (1). Combinations of small-molecule DAAs are required for effective curative oral therapies, because resistant variants existing in the quasispecies population in untreated HCV-infected patients are enriched during monotherapy. To prevent viral breakthrough or relapse and selection of resistant variants, multiple highly effective pangenotypic DAA combination therapies, with NS5A RCIs as the backbone, have been approved or are currently being developed (1, 4, 5).The binding site(s) for NS5A RCIs has been modeled based on biochemical and crystal structure data, implicating at least one site that spans a region between NS5A proteins that associate as dimers (6). Available evidence for NS5A inhibitor binding suggests that NS5A RCIs, such as DCV, bind tightly and specifically to NS5A protein dimers present in infected cells (6).A recent report (7) of DCV binding to Escherichia coli-expressed NS5A protein provided the first direct evidence that DCV binds to NS5A. The authors demonstrated that DCV binding can reduce the affinity of NS5A protein for viral RNA, supporting one potential mechanism of inhibition. An additional report of direct binding to NS5A protein of DCV and the related compound ledipasvir also supports the direct associatio...

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confidence: 49%

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confidence: 93%

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confidence: 98%

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confidence: 99%

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Synergistic Activity of Combined NS5A Inhibitors

O’Boyle

Nower

Gao

et al. 2016

Antimicrob Agents Chemother

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“…The cytoplasmic part of NS5A is composed of a well structured domain 1 (D1) and two intrinsically disordered domains (D2 and D3) that exist as highly dynamic interconverting conformers. NS5A-D1, which is the target of daclatasvir (7,17), contains a zinc finger motif and possesses RNA binding properties (18). Crystallographic studies revealed that this domain could adopt at least three different homodimeric conformations (19 -21), underscoring the multifunctionality of the protein.…”

Section: Hepatitis C Virus (Hcv)mentioning

confidence: 99%