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

Cox, Robert; Toots, Märt; Yoon, Jeong-Joong; Sourimant, Julien; Lüdeke, Barbara; Fearns, Rachel; Bourque, Élyse; Patti, Joseph M.; Lee, Edward; Vernachio, John; Plemper, Richard K.

doi:10.1074/jbc.ra118.004862

Cited by 27 publications

(39 citation statements)

References 62 publications

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“…A total of 141,936 compounds were screened for inhibitory activity against recHPIV3-JS NanoLuc (MOI = 0.2 TCID 50 units/cell). HTS was carried out analogous to our previous reports 64 , 73 , with automated reading of plates 30 hours after infection. Raw data were imported into the MScreen IT environment and analyzed using data mining tools developed in-house or build into the MScreen package as described 64 , 73 .…”

Section: Methodsmentioning

confidence: 99%

“…HTS was carried out analogous to our previous reports 64 , 73 , with automated reading of plates 30 hours after infection. Raw data were imported into the MScreen IT environment and analyzed using data mining tools developed in-house or build into the MScreen package as described 64 , 73 . Hit candidates were defined as compounds with anti-HPIV3 active >2.66×SD in control-dependent mean percent inhibition calculation and >2.1×SD in control-independent mean robust z-score calculation.…”

Section: Methodsmentioning

confidence: 99%

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Orally efficacious broad-spectrum allosteric inhibitor of paramyxovirus polymerase

et al. 2020

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Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Orally efficacious broad-spectrum allosteric inhibitor of paramyxovirus polymerase

et al. 2020

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“…The existence of these pan-resistance sites suggests that it may be challenging to proactively counteract viral escape through synthetic scaffold optimization [69]. Supporting this notion, a large-scale high-throughput drug screen using a recombinant RSV strain carrying a signature pan-resistance mutation did not return any hits blocking F protein activity, although entry inhibitors typically emerge readily and are often pharmacodominant in anti-RSV drug screens [70,71]. Secondly, studies in the mouse RSV pathogenesis model have demonstrated early that signature pan-resistance mutations such as F D401E do not mandatorily coincide with viral attenuation in vivo [68], raising substantial concern that entry inhibitor-resistant RSV may emerge rapidly in the field, and remain pathogenic and possibly able to spread.…”

Section: Synthetic F Protein Blockersmentioning

confidence: 99%

“…Alternatively, allosteric and substrate-analog inhibitors of the RSV polymerase complex have been identified [70,[101][102][103][104][105], some of which likewise showed promising drug-like properties and potently blocked virus replication in cell culture and in vivo. Ultimately, the therapeutic targeting of the polymerase may be more fruitful for two main reasons [106]: (i) all enzymatic functions of the viral polymerase complex, initiation of RNA synthesis, RNA elongation, mRNA capping, and cap methylation, must be performed multiple times to complete an individual viral replication cycle, providing-in contrast to entry inhibition-repeated opportunities for interference, and (ii) polymerase blockers suppress not only the synthesis of structural virion components directly, but also heighten virus susceptibility to the innate host antiviral response, since they prevent the expression of viral non-structural immune-modulatory proteins that are essential for viral pathogenesis [107,108].…”

Section: Perspectives For Pneumo-and Paramyxovirus Entry Inhibitorsmentioning

confidence: 99%

Structural Insight into Paramyxovirus and Pneumovirus Entry Inhibition

Aggarwal

Plemper

2020

Viruses

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Paramyxoviruses and pneumoviruses infect cells through fusion (F) protein-mediated merger of the viral envelope with target membranes. Members of these families include a range of major human and animal pathogens, such as respiratory syncytial virus (RSV), measles virus (MeV), human parainfluenza viruses (HPIVs), and highly pathogenic Nipah virus (NiV). High-resolution F protein structures in both the metastable pre-and the postfusion conformation have been solved for several members of the families and a number of F-targeting entry inhibitors have progressed to advanced development or clinical testing. However, small-molecule RSV entry inhibitors have overall disappointed in clinical trials and viral resistance developed rapidly in experimental settings and patients, raising the question of whether the available structural information may provide a path to counteract viral escape through proactive inhibitor engineering. This article will summarize current mechanistic insight into F-mediated membrane fusion and examine the contribution of structural information to the development of small-molecule F inhibitors. Implications are outlined for future drug target selection and rational drug engineering strategies.Viruses 2020, 12, 342 2 of 16 from its natural bat host to domestic animals, resulting in case/fatality rates reaching from 40% to over 90% [9]. Continued spillover into the human population must be expected, and human-to-human transmission through respiratory secretions, urine, and saliva has been documented [10].Of the pneumoviruses, RSV infects almost all children before two years of age and is responsible for over 100,000 hospitalizations yearly in the United States alone. The monoclonal antibody palivizumab has been approved for immunoprophylaxis against RSV infection [11], however, use is restricted to high-risk patients due to the high-cost and need for prophylactic administration.Given the health, medical and economic burden associated with paramyxo-and pneumovirus infections, a major and currently unmet clinical need exists to expedite the development of novel safe and effective therapeutics for improved disease management and outbreak control. Current direct-acting therapeutics predominantly focus on preventing viral entry through neutralizing antibodies (nAbs) and on small-molecules targeting the envelope glycoproteins or inhibiting the viral RNA-dependent RNA polymerase (RdRP) complex. Reflecting major efforts to identify a cost-effective alternative to high-price passive immunization with anti-RSV nAbs, a number of compounds have entered advanced preclinical development and clinical testing in recent years (Table 1). Breakthroughs in the structural and functional characterization of the viral entry machinery and polymerase complexes in the past decade [12][13][14][15][16][17][18][19][20][21] have furthermore created a novel opportunity for structure-informed mechanistic characterization and ligand optimization.

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“…hRSV is an enveloped, negative-sense, and single-stranded RNA virus that encodes 10 genes that are translated into 11 proteins (Figure 1) (23). Its replication and gene transcription occur in the cytoplasm, thanks to the aid of an RNA-dependent RNA-polymerase that is encoded within the viral genome by the L gene (24, 25). For its adequate function, the L protein requires the viral phosphoprotein P, which associates to this RNA polymerase (26, 27).…”

Section: Hrsv Genes and The Virion Structurementioning

confidence: 99%

Immune-Modulation by the Human Respiratory Syncytial Virus: Focus on Dendritic Cells

2019

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The human respiratory syncytial virus (hRSV) is the leading cause of pneumonia in infants and produces a significant burden in the elderly. It can also infect and produce disease in otherwise healthy adults and recurrently infect those previously exposed to the virus. Importantly, recurrent infections are not necessarily a consequence of antigenic variability, as described for other respiratory viruses, but most likely due to the capacity of this virus to interfere with the host's immune response and the establishment of a protective and long-lasting immunity. Although some genes encoded by hRSV are known to have a direct participation in immune evasion, it seems that repeated infection is mainly given by its capacity to modulate immune components in such a way to promote non-optimal antiviral responses in the host. Importantly, hRSV is known to interfere with dendritic cell (DC) function, which are key cells involved in establishing and regulating protective virus-specific immunity. Notably, hRSV infects DCs, alters their maturation, migration to lymph nodes and their capacity to activate virus-specific T cells, which likely impacts the host antiviral response against this virus. Here, we review and discuss the most important and recent findings related to DC modulation by hRSV, which might be at the basis of recurrent infections in previously infected individuals and hRSV-induced disease. A focus on the interaction between DCs and hRSV will likely contribute to the development of effective prophylactic and antiviral strategies against this virus.

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

Cited by 27 publications

References 62 publications

Orally efficacious broad-spectrum allosteric inhibitor of paramyxovirus polymerase

Orally efficacious broad-spectrum allosteric inhibitor of paramyxovirus polymerase

Structural Insight into Paramyxovirus and Pneumovirus Entry Inhibition

Immune-Modulation by the Human Respiratory Syncytial Virus: Focus on Dendritic Cells

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