Pathogens and Immunity (Sep 2024)

Escape of SARS-CoV-2 Variants KP.1.1, LB.1, and KP.3.3 From Approved Monoclonal Antibodies

  • Delphine Planas,
  • Isabelle Staropoli,
  • Cyril Planchais,
  • Emilie Yab,
  • Banujaa Jeyarajah,
  • Yannis Rahou,
  • Matthieu Prot,
  • Florence Guivel-Benhassine,
  • Frederic Lemoine,
  • Vincent Enouf,
  • Etienne Simon-Loriere,
  • Hugo Mouquet,
  • Marie-Anne Rameix-Welti,
  • Olivier Schwartz

DOI
https://doi.org/10.20411/pai.v10i1.752
Journal volume & issue
Vol. 10, no. 1

Abstract

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Background: First-generation anti-SARS-CoV-2 monoclonal antibodies (mAbs) used for prophylaxis or therapeutic purposes in immunocompromised patients have been withdrawn because of the emergence of resistant Omicron variants. In 2024, 2 novel mAbs, VYD222/Pemivibart and AZD3152/Sipavibart, were approved by health authorities, but their activity against contemporary JN.1 sublineages is poorly characterized. Methods: We isolated authentic JN.1.1, KP.1.1, LB.1, and KP.3.3 viruses and evaluated their sensitivity to neutralization by these mAbs in 2 target cell lines. Results: Compared to ancestral strains, VYD222/Pemivibart remained moderately active against JN.1 subvariants, with a strong increase of 50% Inhibitory Concentration (IC50), reaching up to 3 to 15 µg/mL for KP.3.3. AZD3152/Sipavibart neutralized JN.1.1 but lost antiviral efficacy against KP.1.1, LB.1, and KP.3.3. Conclusions: Our results highlight the need for a close clinical monitoring of VYD222/Pemivibart and raise concerns about the clinical efficacy of AZD3152/Sipavibart.