Brequinar potently inhibits measles virus replication by targeting pyrimidine biosynthesis and shows an additive antiviral effect when combined with remdesivir.
Vero cells expressing the measles virus (MeV) receptor and human B cells
Brequinar (alone and in combination with remdesivir)
Inhibition of measles virus (MeV) replicationsurrogate
Brequinar is a potent inhibitor of measles virus replication in vitro by targeting pyrimidine biosynthesis, suggesting potential for repurposing as an antiviral therapy.
Measles virus (MeV) is highly contagious. Vaccination is the most effective strategy to prevent the infection; however, global measles vaccination coverage is declining, and the incidence of measles outbreaks is increasing. These trends highlight the unmet need for antiviral therapies, particularly for individuals who cannot rely solely on vaccination. In this study, we screened a library of safe-in-human broad-spectrum antiviral agents to identify inhibitors of MeV replication. Among the identified leading candidates, brequinar demonstrated potent antiviral activity, profoundly inhibiting MeV replication in both Vero cells expressing the MeV receptor and human B cells. Supplementation with uridine largely reversed the antiviral effect of brequinar, identifying pyrimidine biosynthesis as the mechanism of action. Furthermore, brequinar exhibited an additive antiviral effect when combined with remdesivir, a direct-acting antiviral drug. Collectively, these findings demonstrated brequinar as a potent inhibitor of MeV replication through targeting the pyrimidine biosynthetic pathway, supporting its potential of repurposing as a therapeutic candidate against MeV.
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Yang Wang
Xin Wang
Rik L. de Swart
Antiviral Research
Erasmus University Rotterdam
Erasmus MC
Norwegian University of Science and Technology
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Wang et al. (Sat,) reported a other. Brequinar potently inhibits measles virus replication by targeting pyrimidine biosynthesis and shows an additive antiviral effect when combined with remdesivir.
www.synapsesocial.com/papers/69df2a4be4eeef8a2a6af737 — DOI: https://doi.org/10.1016/j.antiviral.2026.106413