Structure of a rabies virus polymerase complex from electron cryo-microscopy

Horwitz, Joshua A.; Jenni, Simon; Whelan, Sean P. J.

doi:10.1101/794073

Cited by 20 publications

(39 citation statements)

References 37 publications

(41 reference statements)

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“…The interaction of rabies virus (RABV) P with RABV L is similar the VSV P-L interaction described here ( Figure S4C), with contacts that anchor the CD, MT, and CTD and stabilize a closed conformation of L (Horwitz et al, 2019). The P L sequences for the two viruses have diverged substantially, however, and the specific molecular interactions differ.…”

Section: Resultssupporting

confidence: 60%

Structure of the Vesicular Stomatitis Virus L Protein in Complex with Its Phosphoprotein Cofactor

et al. 2020

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Section: Resultssupporting

confidence: 60%

Structure of the Vesicular Stomatitis Virus L Protein in Complex with Its Phosphoprotein Cofactor

et al. 2020

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“…We favor the mononegavirus RdRP complex as a premier druggable target, based on its diverse enzymatic activities, its unique catalytic activity that lacks a cellular equivalent, and its critical importance for both viral replication and the expression of non-structural immunomodulatory viral proteins that counteract the host innate antiviral response (45). Groundbreaking progress in the structural understanding of the organization of mononegavirus polymerase complexes (29)(30)(31)(32) has established a foundation to define distinct druggable sites in the L polymerase.…”

Section: Discussionmentioning

confidence: 99%

“…This delayed polymerase arrest demonstrates that these compounds do not directly block phosphodiester bond formation. Structural evidence (29)(30)(31)(32)46) and functional characterization (27,34) rather indicates pharmacological interference with conformational changes of the polymerase as the enzyme transitions from initiation to RNA elongation mode.…”

Section: Discussionmentioning

confidence: 99%

“…Despite this high clinical promise, the molecular mechanism of polymerase inhibition by ERDRP-0519 and its physical target docking pose remained unknown, creating a knowledge gap hampering development of the inhibitor class against other mononegavirus targets. Several structural reconstructions of mononegavirus polymerase have been reported recently Cox et al 6 that provided essential insight into the organization of rhabdovirus (vesicular stomatitis virus and rabies virus (29,30)), pneumovirus (RSV (31)), and paramyxovirus (parainfluenzavirus 5 (PIV-5) (32)) polymerase complexes. This information established a framework for structural and mechanistic appreciation of polymerase inhibition by ERDRP-0519.…”

Section: Cox Et Almentioning

confidence: 99%

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Therapeutic Targeting of Measles Virus Polymerase with ERDRP-0519 Suppresses All RNA Synthesis Activity

Cox

Sourimant

Govindarajan

et al. 2020

Preprint

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Morbilliviruses, such as measles virus (MeV) and canine distemper virus (CDV), are highly infectious members of the paramyxovirus family. MeV is responsible for major morbidity and mortality in non-vaccinated populations. ERDRP-0519, a pan-morbillivirus small molecule inhibitor for the treatment of measles, targets the morbillivirus RNA-dependent RNA-polymerase (RdRP) complex and displayed unparalleled oral efficacy against lethal infection of ferrets with CDV, an established surrogate model for human measles. Resistance profiling identified the L subunit of the RdRP, which harbors all enzymatic activity of the polymerase complex, as the molecular target of inhibition. Here, we examined binding characteristics, physical docking site, and the molecular mechanism of action of ERDRP-0519 through label-free biolayer interferometry, photoaffinity cross-linking, and in vitro RdRP assays using purified MeV RdRP complexes and synthetic templates. Results demonstrate that unlike all other mononegavirus small molecule inhibitors identified to date, ERDRP-0519 inhibits all phosphodiester bond formation in both de novo initiation of RNA synthesis at the promoter and RNA elongation by a committed polymerase complex. Photocrosslinking and resistance profiling-informed ligand docking revealed that this unprecedented mechanism of action of ERDRP-0519 is due to simultaneous engagement of the L protein polyribonucleotidyl transferase (PRNTase)-like domain and the flexible intrusion loop by the compound, pharmacologically locking the polymerase in pre-initiation conformation. This study informs selection of ERDRP-0519 as clinical candidate for measles therapy and identifies a previously unrecognized druggable site in mononegavirus L polymerase proteins that can silence all synthesis of viral RNA.ImportanceThe mononegavirus order contains major established and recently emerged human pathogens. Despite the threat to human health, antiviral therapeutics directed against this order remain understudied. The mononegavirus polymerase complex represents a promising drug target due to its central importance for both virus replication and viral mitigation of the innate host antiviral response. In this study, we have mechanistically characterized a clinical candidate small-molecule MeV polymerase inhibitor. The compound blocked all phosphodiester bond formation activity, a unique mechanism of action unlike all other known mononegavirus polymerase inhibitors. Photocrosslinking-based target site mapping demonstrated that this class-defining prototype inhibitor stabilizes a pre-initiation conformation of the viral polymerase complex that sterically cannot accommodate template RNA. Function-equivalent druggable sites exist in all mononegavirus polymerases. In addition to its direct anti-MeV impact, the insight gained in this study can therefore serve as a blueprint for indication spectrum expansion through structure-informed scaffold engineering or targeted drug discovery.

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“…In humans, rabies is preventable by vaccination prior to or immediately after exposure, but there are no specific antiviral drugs available that target the virus directly (1). In PNAS, Horwitz et al (2) present a high-resolution electron cryomicroscopy structure of the RNA synthesis machine of RABV, providing valuable mechanistic insight into its activities and opening up the way toward developing antiviral approaches for this fatal virus.…”

mentioning

confidence: 99%

Insight into the multifunctional RNA synthesis machine of rabies virus

Fodor

2020

Proc. Natl. Acad. Sci. U.S.A.

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Structure of a rabies virus polymerase complex from electron cryo-microscopy

Cited by 20 publications

References 37 publications

Structure of the Vesicular Stomatitis Virus L Protein in Complex with Its Phosphoprotein Cofactor

Structure of the Vesicular Stomatitis Virus L Protein in Complex with Its Phosphoprotein Cofactor

Therapeutic Targeting of Measles Virus Polymerase with ERDRP-0519 Suppresses All RNA Synthesis Activity

Insight into the multifunctional RNA synthesis machine of rabies virus

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