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Design, structure and plasma binding of ancestral β-CoV scaffold antigens

Author

Listed:
  • David Hueting

    (KTH Royal Institute of Technology
    KTH Royal Institute of Technology)

  • Karen Schriever

    (KTH Royal Institute of Technology
    KTH Royal Institute of Technology)

  • Rui Sun

    (Karolinska Institutet)

  • Stelios Vlachiotis

    (Karolinska Institutet)

  • Fanglei Zuo

    (Karolinska Institutet)

  • Likun Du

    (Karolinska Institutet)

  • Helena Persson

    (KTH Royal Institute of Technology
    Science for Life Laboratory)

  • Camilla Hofström

    (KTH Royal Institute of Technology
    Science for Life Laboratory)

  • Mats Ohlin

    (Science for Life Laboratory
    Lund University)

  • Karin Walldén

    (Stockholm University)

  • Marcus Buggert

    (Karolinska Institutet)

  • Lennart Hammarström

    (Karolinska Institutet)

  • Harold Marcotte

    (Karolinska Institutet)

  • Qiang Pan-Hammarström

    (Karolinska Institutet)

  • Juni Andréll

    (Stockholm University
    Karolinska Institutet)

  • Per-Olof Syrén

    (KTH Royal Institute of Technology
    KTH Royal Institute of Technology)

Abstract

We report the application of ancestral sequence reconstruction on coronavirus spike protein, resulting in stable and highly soluble ancestral scaffold antigens (AnSAs). The AnSAs interact with plasma of patients recovered from COVID-19 but do not bind to the human angiotensin-converting enzyme 2 (ACE2) receptor. Cryo-EM analysis of the AnSAs yield high resolution structures (2.6–2.8 Å) indicating a closed pre-fusion conformation in which all three receptor-binding domains (RBDs) are facing downwards. The structures reveal an intricate hydrogen-bonding network mediated by well-resolved loops, both within and across monomers, tethering the N-terminal domain and RBD together. We show that AnSA-5 can induce and boost a broad-spectrum immune response against the wild-type RBD as well as circulating variants of concern in an immune organoid model derived from tonsils. Finally, we highlight how AnSAs are potent scaffolds by replacing the ancestral RBD with the wild-type sequence, which restores ACE2 binding and increases the interaction with convalescent plasma.

Suggested Citation

  • David Hueting & Karen Schriever & Rui Sun & Stelios Vlachiotis & Fanglei Zuo & Likun Du & Helena Persson & Camilla Hofström & Mats Ohlin & Karin Walldén & Marcus Buggert & Lennart Hammarström & Harold, 2023. "Design, structure and plasma binding of ancestral β-CoV scaffold antigens," Nature Communications, Nature, vol. 14(1), pages 1-14, December.
  • Handle: RePEc:nat:natcom:v:14:y:2023:i:1:d:10.1038_s41467-023-42200-x
    DOI: 10.1038/s41467-023-42200-x
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    References listed on IDEAS

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