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Molecular mechanism of antibody neutralization of coxsackievirus A16

Author

Listed:
  • Chao Zhang

    (University of Chinese Academy of Sciences
    Fudan University)

  • Caixuan Liu

    (Chinese Academy of Sciences)

  • Jinping Shi

    (University of Chinese Academy of Sciences)

  • Yalei Wang

    (University of Chinese Academy of Sciences)

  • Cong Xu

    (Chinese Academy of Sciences)

  • Xiaohua Ye

    (University of Chinese Academy of Sciences)

  • Qingwei Liu

    (University of Chinese Academy of Sciences)

  • Xue Li

    (University of Chinese Academy of Sciences)

  • Weihua Qiao

    (University of Chinese Academy of Sciences)

  • Yannan Yin

    (University of Chinese Academy of Sciences)

  • Yao Cong

    (Chinese Academy of Sciences)

  • Zhong Huang

    (University of Chinese Academy of Sciences
    Fudan University)

Abstract

Coxsackievirus A16 (CVA16) causes hand, foot and mouth disease in infants and young children. However, no vaccine or anti-viral agent is currently available for CVA16. Here, the functions and working mechanisms of two CVA16-specific neutralizing monoclonal antibodies (MAbs), 9B5 and 8C4, are comprehensively investigated. Both 9B5 and 8C4 display potent neutralization in vitro and prophylactic and therapeutic efficacy in a mouse model of CVA16 infection. Mechanistically, 9B5 exerts neutralization primarily through inhibiting CVA16 attachment to cell surface via blockade of CVA16 binding to its attachment receptor, heparan sulfate, whereas 8C4 functions mainly at the post-attachment stage of CVA16 entry by interfering with the interaction between CVA16 and its uncoating receptor SCARB2. Cryo-EM studies show that 9B5 and 8C4 target distinct epitopes located at the 5-fold and 3-fold protrusions of CVA16 capsids, respectively, and exhibit differential binding preference to three forms of naturally occurring CVA16 particles. Moreover, 9B5 and 8C4 are compatible in formulating an antibody cocktail which displays the ability to prevent virus escape seen with individual MAbs. Together, our work elucidates the functional and structural basis of CVA16 antibody-mediated neutralization and protection, providing important information for design and development of effective CVA16 vaccines and antibody therapies.

Suggested Citation

  • Chao Zhang & Caixuan Liu & Jinping Shi & Yalei Wang & Cong Xu & Xiaohua Ye & Qingwei Liu & Xue Li & Weihua Qiao & Yannan Yin & Yao Cong & Zhong Huang, 2022. "Molecular mechanism of antibody neutralization of coxsackievirus A16," Nature Communications, Nature, vol. 13(1), pages 1-16, December.
    • Handle: RePEc:nat:natcom:v:13:y:2022:i:1:d:10.1038_s41467-022-35575-w
    DOI: 10.1038/s41467-022-35575-w
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    References listed on IDEAS

    as
    1. Chao Zhang & Cong Xu & Wenlong Dai & Yifan Wang & Zhi Liu & Xueyang Zhang & Xuesong Wang & Haikun Wang & Sitang Gong & Yao Cong & Zhong Huang, 2021. "Functional and structural characterization of a two-MAb cocktail for delayed treatment of enterovirus D68 infections," Nature Communications, Nature, vol. 12(1), pages 1-16, December.
    2. Chao Zhang & Yifan Wang & Yuanfei Zhu & Caixuan Liu & Chenjian Gu & Shiqi Xu & Yalei Wang & Yu Zhou & Yanxing Wang & Wenyu Han & Xiaoyu Hong & Yong Yang & Xueyang Zhang & Tingfeng Wang & Cong Xu & Qin, 2021. "Development and structural basis of a two-MAb cocktail for treating SARS-CoV-2 infections," Nature Communications, Nature, vol. 12(1), pages 1-16, December.
    3. Yuguang Zhao & Daming Zhou & Tao Ni & Dimple Karia & Abhay Kotecha & Xiangxi Wang & Zihe Rao & E. Yvonne Jones & Elizabeth E. Fry & Jingshan Ren & David I. Stuart, 2020. "Hand-foot-and-mouth disease virus receptor KREMEN1 binds the canyon of Coxsackie Virus A10," Nature Communications, Nature, vol. 11(1), pages 1-8, December.
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