Nature Communications (Aug 2023)

Phase I/II trial of a peptide-based COVID-19 T-cell activator in patients with B-cell deficiency

  • Jonas S. Heitmann,
  • Claudia Tandler,
  • Maddalena Marconato,
  • Annika Nelde,
  • Timorshah Habibzada,
  • Susanne M. Rittig,
  • Christian M. Tegeler,
  • Yacine Maringer,
  • Simon U. Jaeger,
  • Monika Denk,
  • Marion Richter,
  • Melek T. Oezbek,
  • Karl-Heinz Wiesmüller,
  • Jens Bauer,
  • Jonas Rieth,
  • Marcel Wacker,
  • Sarah M. Schroeder,
  • Naomi Hoenisch Gravel,
  • Jonas Scheid,
  • Melanie Märklin,
  • Annika Henrich,
  • Boris Klimovich,
  • Kim L. Clar,
  • Martina Lutz,
  • Samuel Holzmayer,
  • Sebastian Hörber,
  • Andreas Peter,
  • Christoph Meisner,
  • Imma Fischer,
  • Markus W. Löffler,
  • Caroline Anna Peuker,
  • Stefan Habringer,
  • Thorsten O. Goetze,
  • Elke Jäger,
  • Hans-Georg Rammensee,
  • Helmut R. Salih,
  • Juliane S. Walz

DOI
https://doi.org/10.1038/s41467-023-40758-0
Journal volume & issue
Vol. 14, no. 1
pp. 1 – 10

Abstract

Read online

Abstract T-cell immunity is central for control of COVID-19, particularly in patients incapable of mounting antibody responses. CoVac-1 is a peptide-based T-cell activator composed of SARS-CoV-2 epitopes with documented favorable safety profile and efficacy in terms of SARS-CoV-2-specific T-cell response. We here report a Phase I/II open-label trial (NCT04954469) in 54 patients with congenital or acquired B-cell deficiency receiving one subcutaneous CoVac-1 dose. Immunogenicity in terms of CoVac-1-induced T-cell responses and safety are the primary and secondary endpoints, respectively. No serious or grade 4 CoVac-1-related adverse events have been observed. Expected local granuloma formation has been observed in 94% of study subjects, whereas systemic reactogenicity has been mild or absent. SARS-CoV-2-specific T-cell responses have been induced in 86% of patients and are directed to multiple CoVac-1 peptides, not affected by any current Omicron variants and mediated by multifunctional T-helper 1 CD4+ T cells. CoVac-1-induced T-cell responses have exceeded those directed to the spike protein after mRNA-based vaccination of B-cell deficient patients and immunocompetent COVID-19 convalescents with and without seroconversion. Overall, our data show that CoVac-1 induces broad and potent T-cell responses in patients with B-cell/antibody deficiency with a favorable safety profile, which warrants advancement to pivotal Phase III safety and efficacy evaluation. ClinicalTrials.gov identifier NCT04954469.