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A single amino acid substitution in the capsid protein of Zika virus contributes to a neurovirulent phenotype

Author

Listed:
  • Guang-Yuan Song

    (Anhui Medical University
    Academy of Military Medical Sciences)

  • Xing-Yao Huang

    (Academy of Military Medical Sciences)

  • Meng-Jiao He

    (Academy of Military Medical Sciences)

  • Hang-Yu Zhou

    (Chinese Academy of Medical Sciences & Peking Union Medical College)

  • Rui-Ting Li

    (Academy of Military Medical Sciences)

  • Ying Tian

    (Anhui Medical University
    Academy of Military Medical Sciences)

  • Yan Wang

    (Tsinghua University)

  • Meng-Li Cheng

    (Academy of Military Medical Sciences)

  • Xiang Chen

    (Academy of Military Medical Sciences)

  • Rong-Rong Zhang

    (Academy of Military Medical Sciences)

  • Chao Zhou

    (Academy of Military Medical Sciences)

  • Jia Zhou

    (Academy of Military Medical Sciences)

  • Xian-Yang Fang

    (Chinese Academy of Sciences)

  • Xiao-Feng Li

    (Academy of Military Medical Sciences)

  • Cheng-Feng Qin

    (Anhui Medical University
    Academy of Military Medical Sciences)

Abstract

Increasing evidence shows the African lineage Zika virus (ZIKV) displays a more severe neurovirulence compared to the Asian ZIKV. However, viral determinants and the underlying mechanisms of enhanced virulence phenotype remain largely unknown. Herein, we identify a panel of amino acid substitutions that are unique to the African lineage of ZIKVs compared to the Asian lineage by phylogenetic analysis and sequence alignment. We then utilize reverse genetic technology to generate recombinant ZIKVs incorporating these lineage-specific substitutions based on an infectious cDNA clone of Asian ZIKV. Through in vitro characterization, we discover a mutant virus with a lysine to arginine substitution at position 101 of capsid (C) protein (termed K101R) displays a larger plaque phenotype, and replicates more efficiently in various cell lines. Moreover, K101R replicates more efficiently in mouse brains and induces stronger inflammatory responses than the wild type (WT) virus in neonatal mice. Finally, a combined analysis reveals the K101R substitution promotes the production of mature C protein without affecting its binding to viral RNA. Our study identifies the role of K101R substitution in the C protein in contributing to the enhanced virulent phenotype of the African lineage ZIKV, which expands our understanding of the complexity of ZIKV proteins.

Suggested Citation

  • Guang-Yuan Song & Xing-Yao Huang & Meng-Jiao He & Hang-Yu Zhou & Rui-Ting Li & Ying Tian & Yan Wang & Meng-Li Cheng & Xiang Chen & Rong-Rong Zhang & Chao Zhou & Jia Zhou & Xian-Yang Fang & Xiao-Feng L, 2023. "A single amino acid substitution in the capsid protein of Zika virus contributes to a neurovirulent phenotype," Nature Communications, Nature, vol. 14(1), pages 1-12, December.
  • Handle: RePEc:nat:natcom:v:14:y:2023:i:1:d:10.1038_s41467-023-42676-7
    DOI: 10.1038/s41467-023-42676-7
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    References listed on IDEAS

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    1. Ter Yong Tan & Guntur Fibriansah & Victor A. Kostyuchenko & Thiam-Seng Ng & Xin-Xiang Lim & Shuijun Zhang & Xin-Ni Lim & Jiaqi Wang & Jian Shi & Marc C. Morais & Davide Corti & Shee-Mei Lok, 2020. "Capsid protein structure in Zika virus reveals the flavivirus assembly process," Nature Communications, Nature, vol. 11(1), pages 1-13, December.
    2. Yang Liu & Jianying Liu & Senyan Du & Chao Shan & Kaixiao Nie & Rudian Zhang & Xiao-Feng Li & Renli Zhang & Tao Wang & Cheng-Feng Qin & Penghua Wang & Pei-Yong Shi & Gong Cheng, 2017. "Evolutionary enhancement of Zika virus infectivity in Aedes aegypti mosquitoes," Nature, Nature, vol. 545(7655), pages 482-486, May.
    3. Fabien Aubry & Sofie Jacobs & Maïlis Darmuzey & Sebastian Lequime & Leen Delang & Albin Fontaine & Natapong Jupatanakul & Elliott F. Miot & Stéphanie Dabo & Caroline Manet & Xavier Montagutelli & Arte, 2021. "Recent African strains of Zika virus display higher transmissibility and fetal pathogenicity than Asian strains," Nature Communications, Nature, vol. 12(1), pages 1-14, December.
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