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Immunization with V987H-stabilized Spike glycoprotein protects K18-hACE2 mice and golden Syrian hamsters upon SARS-CoV-2 infection

  • C Avila-Nieto
  • , J Vergara-Alert
  • , P Amengual-Rigo
  • , E Ainsua-Enrich
  • , M Brustolin
  • , MLR de la Concepción
  • , N Pedreño-Lopez
  • , J Rodon
  • , V Urrea
  • , E Pradenas
  • , S Marfil
  • , E Ballana
  • , E Riveira-Muñoz
  • , M Pérez
  • , N Roca
  • , F Tarrés-Freixas
  • , G Cantero
  • , A Pons-Grifols
  • , C Rovirosa
  • , C Aguilar-Gurrieri
  • R Ortiz, A Barajas, B Trinité, R Lepore, J Muñoz-Basagoiti, D Perez-Zsolt, N Izquierdo-Useros, A Valencia, J Blanco, V Guallar, B Clotet, J Segalés, J Carrillo

Research output: Contribution to journalA1: Peer-reviewed journal articlespeer-review

Abstract

Safe and effective severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) vaccines are crucial to fight against the coronavirus disease 2019 pandemic. Most vaccines are based on a mutated version of the Spike glycoprotein [K986P/V987P (S-2P)] with improved stability, yield and immunogenicity. However, S-2P is still produced at low levels. Here, we describe the V987H mutation that increases by two-fold the production of the recombinant Spike and the exposure of the receptor binding domain (RBD). S-V987H immunogenicity is similar to S-2P in mice and golden Syrian hamsters (GSH), and superior to a monomeric RBD. S-V987H immunization confer full protection against severe disease in K18-hACE2 mice and GSH upon SARS-CoV-2 challenge (D614G or B.1.351 variants). Furthermore, S-V987H immunized K18-hACE2 mice show a faster tissue viral clearance than RBD- or S-2P-vaccinated animals challenged with D614G, B.1.351 or Omicron BQ1.1 variants. Thus, S-V987H protein might be considered for future SARS-CoV-2 vaccines development.
Original languageEnglish
Article number2349
JournalNature Communications
Volume15
Number of pages18
ISSN2041-1723
DOIs
Publication statusPublished - 2024

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