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An adenosine analog shows high antiviral potency against coronavirus and arenavirus mainly through an unusual base pairing mode

Author

Listed:
  • Xiaoying Jia

    (No. 262 Jin Long Street)

  • Xuping Jing

    (No. 262 Jin Long Street)

  • Ming Li

    (University of Science and Technology of China)

  • Minli Gao

    (Chinese Academy of Sciences)

  • Yao Zhong

    (No. 262 Jin Long Street
    University of Chinese Academy of Sciences)

  • Entao Li

    (University of Science and Technology of China
    University of Science and Technology of China)

  • Yang Liu

    (No. 262 Jin Long Street)

  • Rui Li

    (No. 262 Jin Long Street)

  • Guoqiang Yao

    (Chinese Academy of Sciences)

  • Qiaojie Liu

    (No. 262 Jin Long Street)

  • Minmin Zhou

    (No. 262 Jin Long Street
    University of Chinese Academy of Sciences)

  • Yuxia Hou

    (No. 262 Jin Long Street
    University of Chinese Academy of Sciences)

  • Linfeng An

    (University of Science and Technology of China)

  • Yibao Hong

    (University of Science and Technology of China)

  • Shanshan Li

    (University of Science and Technology of China)

  • Jiancun Zhang

    (Chinese Academy of Sciences)

  • Wei Wang

    (No. 262 Jin Long Street)

  • Kaiming Zhang

    (University of Science and Technology of China
    University of Science and Technology of China
    Key Laboratory of Anhui Province for Emerging and Reemerging Infectious Diseases)

  • Peng Gong

    (No. 262 Jin Long Street
    Nankai University)

  • Sandra Chiu

    (University of Science and Technology of China
    University of Science and Technology of China
    Key Laboratory of Anhui Province for Emerging and Reemerging Infectious Diseases)

Abstract

By targeting the essential viral RNA-dependent RNA polymerase (RdRP), nucleoside analogs (NAs) have exhibited great potential in antiviral therapy for RNA virus-related diseases. However, most ribose-modified NAs do not present broad-spectrum features, likely due to differences in ribose-RdRP interactions across virus families. Here, we show that HNC-1664, an adenosine analog with modifications both in ribose and base, has broad-spectrum antiviral activity against positive-strand coronaviruses and negative-strand arenaviruses. Importantly, treatment with HNC-1664 demonstrate anti-SARS-CoV-2 efficacy in infected K18-human ACE2 mice, with reduced viral titer and mortality, as well as improved lung injury. Enzymology data demonstrate that HNC-1664 inhibits RNA synthesis mainly at the pre-catalysis stage. The cryo-EM structures of HNC-1664-bound RdRP-RNA complexes from both SARS-CoV-2 and LASV reveal an unusual base pairing mode of HNC-1664 in part due to its base modification, thus revealing its great potency in binding but not catalysis. Under certain circumstances, 1664-TP can be slowly incorporated by RdRP through regular Watson-Crick base pairing, as evidenced by enzymology data and an HNC-1664-incorporated crystal structure of the RdRP-RNA complex. Overall, HNC-1664 achieves broad-spectrum characteristics by favoring an alternative base pairing strategy to non-catalytically block RNA synthesis, providing a novel concept for the rational development of NA drugs.

Suggested Citation

  • Xiaoying Jia & Xuping Jing & Ming Li & Minli Gao & Yao Zhong & Entao Li & Yang Liu & Rui Li & Guoqiang Yao & Qiaojie Liu & Minmin Zhou & Yuxia Hou & Linfeng An & Yibao Hong & Shanshan Li & Jiancun Zha, 2024. "An adenosine analog shows high antiviral potency against coronavirus and arenavirus mainly through an unusual base pairing mode," Nature Communications, Nature, vol. 15(1), pages 1-16, December.
    • Handle: RePEc:nat:natcom:v:15:y:2024:i:1:d:10.1038_s41467-024-54918-3
    DOI: 10.1038/s41467-024-54918-3
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