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Rational design of a multi-valent human papillomavirus vaccine by capsomere-hybrid co-assembly of virus-like particles

Author

Listed:
  • Daning Wang

    (Xiamen University
    Xiamen University)

  • Xinlin Liu

    (Xiamen University
    Xiamen University)

  • Minxi Wei

    (Xiamen University
    Xiamen University)

  • Ciying Qian

    (Xiamen University
    Xiamen University)

  • Shuo Song

    (Xiamen University
    Xiamen University)

  • Jie Chen

    (Xiamen University
    Xiamen University)

  • Zhiping Wang

    (Xiamen University
    Xiamen University)

  • Qin Xu

    (Xiamen University
    Xiamen University)

  • Yurou Yang

    (Xiamen University
    Xiamen University)

  • Maozhou He

    (Xiamen University
    Xiamen University)

  • Xin Chi

    (Xiamen University
    Xiamen University)

  • Shiwen Huang

    (Xiamen University
    Xiamen University)

  • Tingting Li

    (Xiamen University
    Xiamen University)

  • Zhibo Kong

    (Xiamen University
    Xiamen University)

  • Qingbing Zheng

    (Xiamen University
    Xiamen University)

  • Hai Yu

    (Xiamen University
    Xiamen University)

  • Yingbin Wang

    (Xiamen University
    Xiamen University)

  • Qinjian Zhao

    (Xiamen University
    Xiamen University)

  • Jun Zhang

    (Xiamen University
    Xiamen University)

  • Ningshao Xia

    (Xiamen University
    Xiamen University)

  • Ying Gu

    (Xiamen University
    Xiamen University)

  • Shaowei Li

    (Xiamen University
    Xiamen University)

Abstract

The capsid of human papillomavirus (HPV) spontaneously arranges into a T = 7 icosahedral particle with 72 L1 pentameric capsomeres associating via disulfide bonds between Cys175 and Cys428. Here, we design a capsomere-hybrid virus-like particle (chVLP) to accommodate multiple types of L1 pentamers by the reciprocal assembly of single C175A and C428A L1 mutants, either of which alone encumbers L1 pentamer particle self-assembly. We show that co-assembly between any pair of C175A and C428A mutants across at least nine HPV genotypes occurs at a preferred equal molar stoichiometry, irrespective of the type or number of L1 sequences. A nine-valent chVLP vaccine—formed through the structural clustering of HPV epitopes—confers neutralization titers that are comparable with that of Gardasil 9 and elicits minor cross-neutralizing antibodies against some heterologous HPV types. These findings may pave the way for a new vaccine design that targets multiple pathogenic variants or cancer cells bearing diverse neoantigens.

Suggested Citation

  • Daning Wang & Xinlin Liu & Minxi Wei & Ciying Qian & Shuo Song & Jie Chen & Zhiping Wang & Qin Xu & Yurou Yang & Maozhou He & Xin Chi & Shiwen Huang & Tingting Li & Zhibo Kong & Qingbing Zheng & Hai Y, 2020. "Rational design of a multi-valent human papillomavirus vaccine by capsomere-hybrid co-assembly of virus-like particles," Nature Communications, Nature, vol. 11(1), pages 1-15, December.
  • Handle: RePEc:nat:natcom:v:11:y:2020:i:1:d:10.1038_s41467-020-16639-1
    DOI: 10.1038/s41467-020-16639-1
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