Identification of Non-Nucleoside Inhibitors of the Respiratory Syncytial Virus Polymerase Complex

Jiménez-Somarribas, Alberto; Mao, Shuli; Yoon, Jeong-Joong; Weisshaar, Marco; Cox, Robert; Marengo, Jose R.; Mitchell, David; Morehouse, Zachary P.; Yan, Dan; Solís, Iván; Liotta, Dennis; Natchus, Michael G.; Plemper, Richard K.

doi:10.1021/acs.jmedchem.6b01568

Cited by 9 publications

(25 citation statements)

References 34 publications

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“…We also did not discover any entry inhibitors capable of blocking the pan-entry inhibitor-resistant (15) recombinant RSV-A2-L19F D489E -FireSMASh reporter virus used in this screen, which corroborates the conclusions of previous, independent screens that tested different chemical libraries against the same reporter strains (19,20). Combined, the results of these drug screens corroborate our earlier prediction that overcoming RSV pan-resistance with small-molecule entry inhibitors will be challenging (19,25,27).…”

Section: Characterization and Sar Of An Rsv Rdrp Inhibitorsupporting

confidence: 87%

“…To gain an initial understanding of how GRP-156784 responds to synthetic modification, we launched a ligand-driven SAR development strategy. All chemical analogs were tested for cytotoxicity and antiviral potency against RSV A2-L19F using an automated assay pipeline that we recently developed for standardized SAR profiling (19,25,27,28). The chemical scaffold was hypothetically divided into three distinct sections (Fig.…”

Section: Structure-activity Relationship (Sar) Development For Hit Opmentioning

confidence: 99%

“…In our experience, ligand-driven QSARs show good predictive power for second-stage optimization, provided they are informed by meaningful training and test sets (27,(45)(46)(47). Particularly detrimental to model accuracy are data sets representing overlapping, but distinct, SARs, such as antiviral activity due to specific target binding and cytotoxic effects.…”

Section: Characterization and Sar Of An Rsv Rdrp Inhibitormentioning

confidence: 99%

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Development of an allosteric inhibitor class blocking RNA elongation by the respiratory syncytial virus polymerase complex

Cox

Toots

Yoon

et al. 2018

Journal of Biological Chemistry

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Respiratory syncytial virus (RSV) represents a significant health threat to infants and to elderly or immunocompromised individuals. There are currently no vaccines available to prevent RSV infections, and disease management is largely limited to supportive care, making the identification and development of effective antiviral therapeutics against RSV a priority. To identify effective chemical scaffolds for managing RSV disease, we conducted a high-throughput anti-RSV screen of a 57,000-compound library. We identified a hit compound that specifically blocked activity of the RSV RNA-dependent RNA polymerase (RdRp) complex, initially with moderate low-micromolar potency. Mechanistic characterization in an RSV RdRp assay indicated that representatives of this compound class block elongation of RSV RNA products after initial extension by up to three nucleotides. Synthetic hit-to-lead exploration yielded an informative 3D quantitative structure-activity relationship (3D-QSAR) model and resulted in analogs with more than 20-fold improved potency and selectivity indices (SIs) of>1,000. However, first-generation leads exhibited limited water solubility and poor metabolic stability. A second optimization strategy informed by the 3D-QSAR model combined with pharmacokinetics (PK) predictions yielded an advanced lead, AVG-233, that demonstrated nanomolar activity against both laboratory-adapted RSV strains and clinical RSV isolates. This anti-RSV activity extended to infection of established cell lines and primary human airway cells. PK profiling in mice revealed 34% oral bioavailability of AVG-233 and sustained high drug levels in the circulation after a single oral dose of 20 mg/kg. This promising first-in-class lead warrants further development as an anti-RSV drug.

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Section: Characterization and Sar Of An Rsv Rdrp Inhibitorsupporting

confidence: 87%

Section: Structure-activity Relationship (Sar) Development For Hit Opmentioning

confidence: 99%

Section: Characterization and Sar Of An Rsv Rdrp Inhibitormentioning

confidence: 99%

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Development of an allosteric inhibitor class blocking RNA elongation by the respiratory syncytial virus polymerase complex

Cox

Toots

Yoon

et al. 2018

Journal of Biological Chemistry

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“…Through a dual-pathogen (31,32) HTS campaign that affords the simultaneous identification of RSV and IAV inhibitors, we identified NHC, a pyrimidine ribonucleoside analog, as a hit candidate that integrates promising potency with a broadened indication spectrum. NHC was previously associated with antiviral activity against positivestrand RNA viruses (36-39), but PK/PD profiles have not been determined, and in vivo efficacy is untested.…”

Section: Discussionmentioning

confidence: 99%

“…Toward the ultimate goal of identifying developable broad-spectrum medications against influenza-like disease, we have established and validated a replicationcompetent dual RSV and influenza A virus (IAV) reporter virus-based high-throughput screening (HTS) assay that allows the simultaneous identification of IAV-specific, RSVspecific, and dually active, potentially broad-spectrum, hit candidates (30). The first implementation of this protocol against a large open discovery library of smallmolecule compounds has yielded promising target-specific inhibitors of RSV (31) and influenza virus (32), but broad-spectrum hits remained limited to undesirable scaffolds and clinically undevelopable compounds interfering with pyrimidine de novo synthesis (32)(33)(34). In this study, we applied the assay to a collection of ribonucleoside analogs.…”

mentioning

confidence: 99%

Orally Efficacious Broad-Spectrum Ribonucleoside Analog Inhibitor of Influenza and Respiratory Syncytial Viruses

Yoon

Toots

Lee

et al. 2018

Antimicrob Agents Chemother

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180

193

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Morbidity and mortality resulting from influenza-like disease are a threat, especially for older adults. To improve case management, next-generation broad-spectrum antiviral therapeutics that are efficacious against major drivers of influenza-like disease, including influenza viruses and respiratory syncytial virus (RSV), are urgently needed. Using a dual-pathogen high-throughput screening protocol for influenza A virus (IAV) and RSV inhibitors, we have identified -hydroxycytidine (NHC) as a potent inhibitor of RSV, influenza B viruses, and IAVs of human, avian, and swine origins. Biochemical polymerase assays and viral RNA sequencing revealed that the ribonucleotide analog is incorporated into nascent viral RNAs in place of cytidine, increasing the frequency of viral mutagenesis. Viral passaging in cell culture in the presence of an inhibitor did not induce robust resistance. Pharmacokinetic profiling demonstrated dose-dependent oral bioavailability of 36 to 56%, sustained levels of the active 5'-triphosphate anabolite in primary human airway cells and mouse lung tissue, and good tolerability after extended dosing at 800 mg/kg of body weight/day. The compound was orally efficacious against RSV and both seasonal and highly pathogenic avian IAVs in mouse models, reducing lung virus loads and alleviating disease biomarkers. Oral dosing reduced IAV burdens in a guinea pig transmission model and suppressed virus spread to uninfected contact animals through direct transmission. Based on its broad-spectrum efficacy and pharmacokinetic properties, NHC is a promising candidate for future clinical development as a treatment option for influenza-like diseases.

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Synthesis, antimicrobial and anti‐tubercular activity study of N‐(substituted‐benzyl)‐4‐(trifluoromethyl)thiazole‐2‐sulfonamide and 2‐(N‐(substituted‐benzyl)sulfamoyl)thiazole‐4‐carboxylic acid

Bhujbal¹,

Gaikwad

Jagdale³

et al. 2021

J Chinese Chemical Soc

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A series of novel N‐(substituted‐benzyl)‐4‐(trifluoromethyl)thiazole‐2‐sulfonamide (4a‐4i) and 2‐(N‐[2‐chlorobenzyl]sulfamoyl)thiazole‐4‐carboxylic acid (7a‐7i) derivatives were synthesized from readily available 4‐(trifluoromethyl)thiazol‐2‐amine (1) and ethyl 2‐aminothiazole‐4‐carboxylate (5), respectively. Eighteen novel thiazole‐2‐sulfonamide derivatives were synthesized. The targets were synthesized through a series of reactions involving diazotization and sulfonamide coupling reactions. All the synthesized compounds were characterized by 1H NMR, 19F, 13C NMR, HRMS, and HPLC analytical techniques. All the synthetic derivatives were evaluated for their antimicrobial activity (minimum inhibitory concentration) against a series of strains of Bacillus subtillis, Staphylococcus aureus, and Escherichia coli for antibacterial activity and against the strains of Candida albicans, Aspergillus flavus, and Aspergillus niger for antifungal activity. Also synthetic derivatives were tested for their in vitro anti‐tubercular (Mycobacterium tuberculosis: H37 Rv, MDR, and XDR strains) activities. Most of compounds showed moderate to good activity for antimicrobial and anti‐tubercular strains. The compounds 4b (MIC = 12.5 μg/ml and 3.125 μM), 4c (MIC = 1.562 μM), 4d (MIC = 12.5 μg/ml), 7b (MIC = 12.5 μg/ml), 7c (MIC = 26 μg/ml and 1.562 μM), and 7i (MIC = 26 μg/ml and 6.25 μM) showed good antimicrobial and anti‐tubercular activity in the range of (MIC = 12.5–26 μg/ml) and (MIC = 1.562–6.25 μM) against tested strains, while some derivatives show moderate inhibitions through the series.

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Identification of Non-Nucleoside Inhibitors of the Respiratory Syncytial Virus Polymerase Complex

Cited by 9 publications

References 34 publications

Development of an allosteric inhibitor class blocking RNA elongation by the respiratory syncytial virus polymerase complex

Development of an allosteric inhibitor class blocking RNA elongation by the respiratory syncytial virus polymerase complex

Orally Efficacious Broad-Spectrum Ribonucleoside Analog Inhibitor of Influenza and Respiratory Syncytial Viruses

Synthesis, antimicrobial and anti‐tubercular activity study of N‐(substituted‐benzyl)‐4‐(trifluoromethyl)thiazole‐2‐sulfonamide and 2‐(N‐(substituted‐benzyl)sulfamoyl)thiazole‐4‐carboxylic acid

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