Document Type
Article
Publication Date
2-17-2026
Abstract
Dengue virus (DENV) is a mosquito-transmitted flavivirus that circulates globally as four distinct serotypes and poses a substantial threat to public health. There are an estimated ~96 million symptomatic infections yearly, including severe cases of dengue fever, underscoring the urgency of identifying effective therapeutics targeting all four serotypes. Nucleoside analogs, which mimic endogenous nucleosides to inhibit viral RNA replication, offer a promising strategy for broad-spectrum antiviral development. Here, we conducted a high-throughput screen of 1,101 nucleoside analogs against DENV serotype 2 (DENV2) in a panel of human cell models, including human epithelial cells, hepatocytes, and fibroblasts. Candidates that were active against DENV2 were screened against all four serotypes. Since flaviviruses including West Nile virus and Zika virus are also important human pathogens, we screened these compounds for activity and identified compounds that were broadly active in these cellular and viral models. We further evaluated antivirals in primary human keratinocytes and fibroblasts, which are early targets of mosquito-transmitted DENV infection. From this screen, we identified 23 nucleoside analogs with broad antiviral activity against DENV and focused on two purine analogs UPGNUC255 and UPGNUC558, that demonstrated potent pan-flaviviral activity achieving >10-fold viral load reduction across all four DENV serotypes and other flaviviruses across cell models. Mechanistic studies revealed that both compounds target the viral RNA-dependent RNA polymerase (RdRp) domain of NS5. Resistance to UPGNUC558 was associated with a conserved S604T substitution, conferring cross-resistance to other 2'C-substituted nucleoside analogs. Resistance to UPGNUC255 was linked to a previously unknown R355Q mutation, located near the catalytic GDD motif of RdRp. These findings highlight UPGNUC255 and UPGNUC558 as promising leads for the development of broad-spectrum antiviral agents against flaviviruses.
Recommended Citation
Bhakt, Priyanka; Pokharel, Swechha; Li, Yue; Srivastava, Tamanna; Miller, Jesse; Dittmar, Mark; Zhu, Yongqing; Nguyen, David; Walter, Zachary; Ayyanathan, Kasirajan; Tudor, Matthew; Yu, Chenguang; Chatterjee, Arnab; Ramage, Holly; Schultz, David; and Cherry, Sara, "NS5-Targeting Nucleoside Analogs Inhibit Dengue Virus and Other Flaviviruses" (2026). Department of Microbiology and Immunology Faculty Papers. Paper 199.
https://jdc.jefferson.edu/mifp/199
Creative Commons License
This work is licensed under a Creative Commons Attribution 4.0 License.
S2 Fig. Chemical structures and dose response validation of indicated nucleoside analogs..tif (1634 kB)
S3 Fig. Orthogonal validation of nucleoside analogs activity across various cell models.tif (2079 kB)
S4 Fig. Orthogonal validation of nucleoside analog activity across DENV serotypes and other flaviviruses.tif (1945 kB)
S5 Fig. Nucleoside analog activity in primary cells.tif (1115 kB)
S6 Fig. Chemical structures of 2’ substituted nucleoside analogs..tif (1242 kB)
S7 Fig. Chemical structures of additional nucleoside analogs..tif (800 kB)
S8 Fig. WNV and ZIKV infect A549 and IMR90 cells..tif (3940 kB)
S9 Fig. Dose response analysis of UPGNUC255 derivatives against flaviviruses..tif (770 kB)
S10 Fig. Conserved residues are involved in nucleoside analog selection..tif (5945 kB)
S1 Table Primary screening data.xlsx (691 kB)
S2 Table Antiviral testing across flaviviruses.xlsx (665 kB)
S3 Table Primers used in this study.xlsx (11 kB)
S4 Table Raw data for manuscript.xlsx (238 kB)
PubMed ID
41701758
Language
English
Comments
This article is the author’s final published version in PLOS Pathogens, Volume 22, 2026, Article number e1013970.
The published version is available at https://doi.org/10.1371/journal.ppat.1013970. Copyright © 2026 Bhakt et al.