Identification and Biological Evaluation of a Series of 1H-Benzo[de]isoquinoline-1,3(2H)-diones as Hepatitis C Virus NS5B Polymerase Inhibitors

Ontoria, Jesus M.; Rydberg, Edwin H.; Marco, Stefania Di; Tomei, Licia; Attenni, Barbara; Malancona, Savina; Hernando, José Ignacio Martı́n; Gennari, Nadia; Koch, Uwe; Narjes, Frank; Rowley, Michael; Summa, Vincenzo; Carroll, Steve; Olsen, David B.; Francesco, Raffaele De; Altamura, Sergio; Migliaccio, Giovanni; Carfı́, Andrea

doi:10.1021/jm900517t

Cited by 42 publications

(49 citation statements)

References 39 publications

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“…1) (15)(16)(17)(18)(19)(20)(21)(22)(23)(24). We will refer to NNI-1 and -2 as ''thumb inhibitors'' while NNI-3 and -4 will be referred to as ''palm inhibitors''.…”

Section: Introductionmentioning

confidence: 99%

Allosteric Inhibitors Have Distinct Effects, but Also Common Modes of Action, in the HCV Polymerase

Davis

Brown

Thorpe

2015

Biophysical Journal

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The RNA-dependent RNA polymerase from the Hepatitis C Virus (gene product NS5B) is a validated drug target because of its critical role in genome replication. There are at least four distinct allosteric sites on the polymerase to which several small molecule inhibitors bind. In addition, numerous crystal structures have been solved with different allosteric inhibitors bound to the polymerase. However, the molecular mechanisms by which these small molecules inhibit the enzyme have not been fully elucidated. There is evidence that allosteric inhibitors alter the intrinsic motions and distribution of conformations sampled by the enzyme. In this study we use molecular dynamics simulations to understand the structural and dynamic changes that result when inhibitors are bound at three different allosteric binding sites on the enzyme. We observe that ligand binding at each site alters the structure and dynamics of NS5B in a distinct manner. Nonetheless, our studies also highlight commonalities in the mechanisms of action of the different inhibitors. Each inhibitor alters the conformational states sampled by the enzyme, either by rigidifying the enzyme and preventing transitions between functional conformational states or by destabilizing the enzyme and preventing functionally relevant conformations from being adequately sampled. By illuminating the molecular mechanisms of allosteric inhibition, these studies delineate the intrinsic functional properties of the enzyme and pave the way for designing novel and more effective polymerase inhibitors. This information may also be important to understand how allosteric regulation occurs in related viral polymerases and other enzymes.

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“…1) (15)(16)(17)(18)(19)(20)(21)(22)(23)(24). We will refer to NNI-1 and -2 as ''thumb inhibitors'' while NNI-3 and -4 will be referred to as ''palm inhibitors''.…”

Section: Introductionmentioning

confidence: 99%

Allosteric Inhibitors Have Distinct Effects, but Also Common Modes of Action, in the HCV Polymerase

Davis

Brown

Thorpe

2015

Biophysical Journal

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“…To further improve the window between EC 50 and CC 50 , in compound 7c the basic amine was removed from the side chain and the benzyl moiety replaced by a carboxylic group. 9 While 7c showed modest potency, loosing both in enzymatic and cells assays and mainly with respect to genotype 1b, it was less cytotoxic (SI = 8). The beneficial effect of the carboxylic acid presence was not general since CO other analogs in the series exhibited a lower selectivity index (data not shown).…”

Section: Biological Resultsmentioning

confidence: 96%

“…7 Several small molecules acting as allosteric inhibitors of NS5B have been disclosed during the past years reflecting the major effort in this area from pharmaceutical industries and academia. 8 Recently, we disclosed a series of 1H-benzo[de]isoquinoline-1,3(2H)-diones as allosteric inhibitors of NS5B polymerase 9 (Table 1). The lead compound 1a showed nanomolar activity on the main NS5B polymerase genotypes (1b, 2b), while activity was in the micromolar range in the cell based assays (Table 1).…”

Section: Introductionmentioning

confidence: 99%

“…The tricyclic core interacts with a flat lipophilic surface, the bromophenyl substituent makes extensive Van der Waals and hydrophobic interactions, whereas the imide oxygens and heteroatoms of the ethanolamine side chain are involved in direct or water mediated H-bonds. 9 The bromine present in 1a can be replaced with a chlorine as in 1b without changing the activity profile both on the enzyme and in the cell based assay. The structural information gained with X-ray guided the SAR studies that culminated in the identification of the more active compound 2 in which the ethanolamine side chain had been substituted by a benzylpiperidine moiety.…”

Section: Introductionmentioning

confidence: 99%

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Allosteric inhibitors of hepatitis C virus NS5B polymerase thumb domain site II: Structure-based design and synthesis of new templates

Malancona

Donghi

Ferrara

et al. 2010

Bioorganic & Medicinal Chemistry

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“…Eighteen molecules [15,17,20,21,26,[28][29][30][31]34,35,38,44] with diverse structures (Fig. 1) and a fourfold activity spread (0.002-92 µM) were used to develop a pharmacophore model.…”

Section: Data Collection For Pharmacophore Generationmentioning

confidence: 99%

Combination of pharmacophore hypothesis and molecular docking to identify novel inhibitors of HCV NS5B polymerase

Harikishore

Lee

et al. 2015

Mol Divers

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Hepatitis C virus (HCV) infection or HCV-related liver diseases are now shown to cause more than 350,000 deaths every year. Adaptability of HCV genome to vary its composition and the existence of multiple strains makes it more difficult to combat the emergence of drug-resistant HCV infections. Among the HCV polyprotein which has both the structural and non-structural regions, the non-structural protein NS5B RNA-dependent RNA polymerase (RdRP) mainly mediates the catalytic role of RNA replication in conjunction with its viral protein machinery as well as host chaperone proteins. Lack of such RNA-dependent RNA polymerase enzyme in host had made it an attractive and hotly pursued target for drug discovery efforts. Recent drug discovery efforts targeting HCV RdRP have seen success with FDA approval for sofosbuvir as a direct-acting antiviral against HCV infection. However, variations in drug-binding sites induce drug resistance, and therefore targeting allosteric sites could delay the emergence of drug resistance. In this study, we focussed on allosteric thumb site II of the non-structural protein NS5B RNA-dependent RNA polymerase and developed a five-feature pharmacophore hypothesis/model which estimated the experimental activity with a strong correlation of 0.971 & 0.944 for training and test sets, respectively. Further, the Güner-Henry score of 0.6 suggests that the model was able to discern the active and inactive compounds and enrich the true positives during a database search. In this study, database search and molecular docking results supported by experimental HCV viral replication inhibition assays suggested ligands with best fitness to the pharmacophore model dock to the key residues involved in thumbs site II, which inhibited the HCV 1b viral replication in sub-micro-molar range.

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Identification and Biological Evaluation of a Series of 1H-Benzo[de]isoquinoline-1,3(2H)-diones as Hepatitis C Virus NS5B Polymerase Inhibitors

Cited by 42 publications

References 39 publications

Allosteric Inhibitors Have Distinct Effects, but Also Common Modes of Action, in the HCV Polymerase

Allosteric Inhibitors Have Distinct Effects, but Also Common Modes of Action, in the HCV Polymerase

Allosteric inhibitors of hepatitis C virus NS5B polymerase thumb domain site II: Structure-based design and synthesis of new templates

Combination of pharmacophore hypothesis and molecular docking to identify novel inhibitors of HCV NS5B polymerase

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