Nature Communications (Jun 2023)

GRT-R910: a self-amplifying mRNA SARS-CoV-2 vaccine boosts immunity for ≥6 months in previously-vaccinated older adults

  • Christine D. Palmer,
  • Ciaran D. Scallan,
  • Lauren D. Kraemer Tardif,
  • Melissa A. Kachura,
  • Amy R. Rappaport,
  • Daniel O. Koralek,
  • Alison Uriel,
  • Leonid Gitlin,
  • Joshua Klein,
  • Matthew J. Davis,
  • Harshni Venkatraman,
  • Meghan G. Hart,
  • Jason R. Jaroslavsky,
  • Sonia Kounlavouth,
  • Martina Marrali,
  • Charmaine N. Nganje,
  • Kyounghwa Bae,
  • Tiffany Yan,
  • Katharyn Leodones,
  • Milana Egorova,
  • Sue-Jean Hong,
  • Jenchun Kuan,
  • Silvia Grappi,
  • Pedro Garbes,
  • Karin Jooss,
  • Andrew Ustianowski

DOI
https://doi.org/10.1038/s41467-023-39053-9
Journal volume & issue
Vol. 14, no. 1
pp. 1 – 17

Abstract

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Abstract SARS-CoV-2 has resulted in high levels of morbidity and mortality world-wide, and severe complications can occur in older populations. Humoral immunity induced by authorized vaccines wanes within 6 months, and frequent boosts may only offer transient protection. GRT-R910 is an investigational self-amplifying mRNA (samRNA)-based SARS-CoV-2 vaccine delivering full-length Spike and selected conserved non-Spike T cell epitopes. This study reports interim analyses for a phase I open-label dose-escalation trial evaluating GRT-R910 in previously vaccinated healthy older adults (NCT05148962). Primary endpoints of safety and tolerability were assessed. Most solicited local and systemic adverse events (AEs) following GRT-R910 dosing were mild to moderate and transient, and no treatment-related serious AEs were observed. The secondary endpoint of immunogenicity was assessed via IgG binding assays, neutralization assays, interferon-gamma ELISpot, and intracellular cytokine staining. Neutralizing antibody titers against ancestral Spike and variants of concern were boosted or induced by GRT-R910 and, contrasting to authorized vaccines, persisted through at least 6 months after the booster dose. GRT-R910 increased and/or broadened functional Spike-specific T cell responses and primed functional T cell responses to conserved non-Spike epitopes. This study is limited due to small sample size, and additional data from ongoing studies will be required to corroborate these interim findings.