npj Vaccines (Feb 2024)

Immunogenicity phase II study evaluating booster capacity of nonadjuvanted AKS-452 SARS-Cov-2 RBD Fc vaccine

  • David G. Alleva,
  • Eline A. Feitsma,
  • Yester F. Janssen,
  • Hendrikus H. Boersma,
  • Thomas M. Lancaster,
  • Thillainaygam Sathiyaseelan,
  • Sylaja Murikipudi,
  • Andrea R. Delpero,
  • Melanie M. Scully,
  • Ramya Ragupathy,
  • Sravya Kotha,
  • Jeffrey R. Haworth,
  • Nishit J. Shah,
  • Vidhya Rao,
  • Shashikant Nagre,
  • Shannon E. Ronca,
  • Freedom M. Green,
  • Stephen A. Shaw,
  • Ari Aminetzah,
  • Schelto Kruijff,
  • Maarten Brom,
  • Gooitzen M. van Dam,
  • Todd C. Zion

DOI
https://doi.org/10.1038/s41541-024-00830-2
Journal volume & issue
Vol. 9, no. 1
pp. 1 – 12

Abstract

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Abstract AKS-452, a subunit vaccine comprising an Fc fusion of the ancestral wild-type (WT) SARS-CoV-2 virus spike protein receptor binding domain (SP/RBD), was evaluated without adjuvant in a single cohort, non-randomized, open-labelled phase II study (NCT05124483) at a single site in The Netherlands for safety and immunogenicity. A single 90 µg subcutaneous booster dose of AKS-452 was administered to 71 adults previously primed with a registered mRNA- or adenovirus-based vaccine and evaluated for 273 days. All AEs were mild and no SAEs were attributable to AKS-452. While all subjects showed pre-existing SP/RBD binding and ACE2-inhibitory IgG titers, 60–68% responded to AKS-452 via ≥2-fold increase from days 28 to 90 and progressively decreased back to baseline by day 180 (days 28 and 90 mean fold-increases, 14.7 ± 6.3 and 8.0 ± 2.2). Similar response kinetics against RBD mutant proteins (including omicrons) were observed but with slightly reduced titers relative to WT. There was an expected strong inverse correlation between day-0 titers and the fold-increase in titers at day 28. AKS-452 enhanced neutralization potency against live virus, consistent with IgG titers. Nucleocapsid protein (Np) titers suggested infection occurred in 66% (46 of 70) of subjects, in which only 20 reported mild symptomatic COVID-19. These favorable safety and immunogenicity profiles support booster evaluation in a planned phase III universal booster study of this room-temperature stable vaccine that can be rapidly and inexpensively manufactured to serve vaccination at a global scale without the need of a complex distribution or cold chain.