State of the Art in Respiratory Syncytial Virus Drug Discovery and Development

Cockerill, G. Stuart; Good, James A. D.; Mathews, Neil

doi:10.1021/acs.jmedchem.8b01361

Cited by 57 publications

(69 citation statements)

References 97 publications

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“…Nucleoside analogs that terminate RNA chain synthesis have been identified (Clarke et al, 2015;Deval et al, 2015;Wang et al, 2015), and one such compound, ALS-8176, has shown efficacy in RSV-infected adults (DeVincenzo et al, 2015). Several non-nucleoside small-molecule inhibitors have also been identified (Cockerill et al, 2019;Fearns and Deval, 2016), and although some (for example, BI-compound D) are known to disrupt RNA cap addition (Liuzzi et al, 2005), there are additional inhibitor classes for which the mechanism of action is not well understood (Duvall et al, 2016;McCutcheon et al, 2015). P serves as an essential polymerase cofactor that tethers L to the nucleoprotein-RNA complex (García et al, 1993;Grosfeld et al, 1995;Yu et al, 1995).…”

Section: Introductionmentioning

confidence: 99%

Structure of the Respiratory Syncytial Virus Polymerase Complex

Gilman

Liu

Fung

et al. 2019

Cell

140

209

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Graphical AbstractHighlights d Cryo-EM structure of RSV L bound by tetrameric RSV P solved to 3.2 Å d P tetramer adopts an asymmetric tentacular arrangement when bound to L d L priming loop adopts elongation-compatible state without PRNTase-RdRp separation d Structure rationalizes escape from small-molecule antivirals SUMMARY Numerous interventions are in clinical development for respiratory syncytial virus (RSV) infection, including small molecules that target viral transcription and replication. These processes are catalyzed by a complex comprising the RNA-dependent RNA polymerase (L) and the tetrameric phosphoprotein (P). RSV P recruits multiple proteins to the polymerase complex and, with the exception of its oligomerization domain, is thought to be intrinsically disordered. Despite their critical roles in RSV transcription and replication, structures of L and P have remained elusive. Here, we describe the 3.2-Å cryo-EM structure of RSV L bound to tetrameric P. The structure reveals a striking tentacular arrangement of P, with each of the four monomers adopting a distinct conformation. The structure also rationalizes inhibitor escape mutants and mutations observed in live-attenuated vaccine candidates. These results provide a framework for determining the molecular underpinnings of RSV replication and transcription and should facilitate the design of effective RSV inhibitors.

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Section: Introductionmentioning

confidence: 99%

Structure of the Respiratory Syncytial Virus Polymerase Complex

Gilman

Liu

Fung

et al. 2019

Cell

140

209

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“…Based on these predictions, we decided to stabilize the transient -helix of P (12)(13)(14)(15)(16)(17)(18)(19)(20)(21)(22)(23)(24). Given that at least 16 to 18 residues are usually required to successfully stabilize an -helix in aqueous solution (22), and that Phe28 appeared to fit well into the helical wheel representation, we decided to focus on P (11)(12)(13)(14)(15)(16)(17)(18)(19)(20)(21)(22)(23)(24)(25)(26)(27)(28)(29)(30). A stapled peptide scan of P (11)(12)(13)(14)(15)(16)(17)(18)(19)(20)(21)(22)(23)(24)(25)…”

Section: Resultsmentioning

confidence: 99%

“…Given that at least 16 to 18 residues are usually required to successfully stabilize an -helix in aqueous solution (22), and that Phe28 appeared to fit well into the helical wheel representation, we decided to focus on P (11)(12)(13)(14)(15)(16)(17)(18)(19)(20)(21)(22)(23)(24)(25)(26)(27)(28)(29)(30). A stapled peptide scan of P (11)(12)(13)(14)(15)(16)(17)(18)(19)(20)(21)(22)(23)(24)(25)(26)(27)(28)(29)(30) was performed by inserting the all-hydrocarbon cross-link at the hydrophilic face of the helix, the presumed non interacting face of the helix. (19).…”

Section: Resultsmentioning

confidence: 99%

Targeting the Respiratory Syncytial Virus N ⁰ -P Complex with Constrained α-Helical Peptides in Cells and Mice

Galloux

Gsponer

Gaillard

et al. 2020

Antimicrob Agents Chemother

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RSV is the main cause of severe respiratory infection in young children worldwide for which no therapies are approved for treatment. Recent clinical trials data resulting from the treatment of RSV infected patients with fusion or L polymerase inhibitors revealed the emergence of escape mutants highlighting the need for the discovery of inhibitors with novel mechanism of action. Here we describe stapled peptides derived from the N-terminus of the phosphoprotein P that act as replication inhibitors. We demonstrate that these peptides inhibit RSV replication in vitro and in vivo through preventing the formation of the N0-P complex. The present strategy provides a novel means of targeting RSV replication with constrained macrocyclic peptides or small-molecules and is broadly applicable to other viruses of the Mononegavirales order.

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“…Therapeutic monoclonal antibodies (mAbs) have become a prospective part of infectious diseases due to their specificity, limited off-target effects, and favourable safety profile. Primary examples of mAbs as treatment are palivizumab against respiratory syncytial virus and ZMapp against Ebola virus [17,18].…”

Section: Introductionmentioning

confidence: 99%

Generation of neutralizing and non-neutralizing monoclonal antibodies against H7N9 influenza virus

Yang

Xiao

et al. 2020

Emerging Microbes & Infections

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The H7N9 viruses have been circulating for six years. The insertion of a polybasic cleavage site in the haemagglutinin (HA) protein of H7N9 has resulted in the emergence of a highly pathogenic (HP) avian influenza virus. Currently, there are limited studies on neutralizing monoclonal antibodies(mAbs) against HP H7N9 AIVs. In this study, mice were immunized with inactivated H7N9 vaccine of A/ZJU01/PR8/2013 to produce murine mAbs. Finally, two murine mAbs against the HA of low pathogenic (LP) virus were produced and characterized. Characterization included determining mAbs binding breadth and affinity, in vitro neutralization capacity, and potential in vivo protection. Two of these mAbs, 1H10 and 2D1, have been identified to have therapeutic and prophylactic efficacy against the HP strain in mouse passive transfer-viral challenge experiments. The mAb 1H10 was most efficacious, even if the treatment-time was as late as 72 h post-infection, or the therapeutic dose was as low as 1 mg/kg; and it was confirmed to have haemagglutination inhibition and neutralizing activity on both LP-and HP-H7N9 strains. Further study indicated that the protection provided by 2D1 was mediated by antibody-dependent cellular cytotoxicity. The mAbs described here provide promising results and merit further development into potential antiviral therapeutics for H7N9 infection.

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State of the Art in Respiratory Syncytial Virus Drug Discovery and Development

Cited by 57 publications

References 97 publications

Structure of the Respiratory Syncytial Virus Polymerase Complex

Structure of the Respiratory Syncytial Virus Polymerase Complex

Targeting the Respiratory Syncytial Virus N ⁰ -P Complex with Constrained α-Helical Peptides in Cells and Mice

Generation of neutralizing and non-neutralizing monoclonal antibodies against H7N9 influenza virus

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State of the Art in Respiratory Syncytial Virus Drug Discovery and Development

Cited by 57 publications

References 97 publications

Structure of the Respiratory Syncytial Virus Polymerase Complex

Structure of the Respiratory Syncytial Virus Polymerase Complex

Targeting the Respiratory Syncytial Virus N 0 -P Complex with Constrained α-Helical Peptides in Cells and Mice

Generation of neutralizing and non-neutralizing monoclonal antibodies against H7N9 influenza virus

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Targeting the Respiratory Syncytial Virus N ⁰ -P Complex with Constrained α-Helical Peptides in Cells and Mice