EBioMedicine (Jan 2022)

Safety and immunogenicity of a measles-vectored SARS-CoV-2 vaccine candidate, V591 / TMV-083, in healthy adults: results of a randomized, placebo-controlled Phase I study

  • Odile Launay,
  • Cécile Artaud,
  • Marie Lachâtre,
  • Mohand Ait-Ahmed,
  • Jelle Klein,
  • Liem Binh Luong Nguyen,
  • Christine Durier,
  • Bastiaan Jansen,
  • Yvonne Tomberger,
  • Nathalie Jolly,
  • Anna Grossmann,
  • Houda Tabbal,
  • Jérémy Brunet,
  • Marion Gransagne,
  • Zaineb Choucha,
  • Damien Batalie,
  • Ana Delgado,
  • Matthias Müllner,
  • Roland Tschismarov,
  • Pieter-Jan Berghmans,
  • Annette Martin,
  • Katrin Ramsauer,
  • Nicolas Escriou,
  • Christiane Gerke

Journal volume & issue
Vol. 75
p. 103810

Abstract

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Summary: Background: V591 (TMV-083) is a live recombinant measles vector-based vaccine candidate expressing a pre-fusion stabilized SARS-CoV-2 spike protein. Methods: We performed a randomized, placebo-controlled Phase I trial with an unblinded dose escalation and a double-blind treatment phase at 2 sites in France and Belgium to evaluate the safety and immunogenicity of V591. Ninety healthy SARS-CoV-2 sero-negative adults (18-55 years of age) were randomized into 3 cohorts, each comprising 24 vaccinees and 6 placebo recipients. Participants received two intramuscular injections of a low dose vaccine (1 × 105 median Tissue Culture Infectious Dose [TCID50]), one or two injections of a high dose vaccine (1 × 106 TCID50), or placebo with a 28 day interval. Safety was assessed by solicited and unsolicited adverse events. Immunogenicity was measured by SARS-CoV-2 spike protein-binding antibodies, neutralizing antibodies, spike-specific T cell responses, and anti-measles antibodies. ClinicalTrials.gov, NCT04497298. Findings: Between Aug 10 and Oct 13, 2020, 148 volunteers were screened of whom 90 were randomized. V591 showed a good safety profile at both dose levels. No serious adverse events were reported. At least one treatment-related adverse event was reported by 15 (20.8%) participants receiving V591 vs. 6 (33.3%) of participants receiving placebo. Eighty-one percent of participants receiving two injections of V591 developed spike-binding antibodies after the second injection. However, neutralizing antibodies were detectable on day 56 only in 17% of participants receiving the low dose and 61% receiving the high dose (2 injections). Spike-specific T cell responses were not detected. Pre-existing anti-measles immunity had a statistically significant impact on the immune response to V591, which was in contrast to previous results with the measles vector-based chikungunya vaccine. Interpretation: While V591 was generally well tolerated, the immunogenicity was not sufficient to support further development.

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