EClinicalMedicine (Jan 2021)

Safety and immunogenicity of INO-4800 DNA vaccine against SARS-CoV-2: A preliminary report of an open-label, Phase 1 clinical trial

  • Pablo Tebas,
  • ShuPing Yang,
  • Jean D. Boyer,
  • Emma L. Reuschel,
  • Ami Patel,
  • Aaron Christensen-Quick,
  • Viviane M. Andrade,
  • Matthew P. Morrow,
  • Kimberly Kraynyak,
  • Joseph Agnes,
  • Mansi Purwar,
  • Albert Sylvester,
  • Jan Pawlicki,
  • Elisabeth Gillespie,
  • Igor Maricic,
  • Faraz I. Zaidi,
  • Kevin Y. Kim,
  • Yaya Dia,
  • Drew Frase,
  • Patrick Pezzoli,
  • Katherine Schultheis,
  • Trevor R.F. Smith,
  • Stephanie J. Ramos,
  • Trevor McMullan,
  • Karen Buttigieg,
  • Miles W. Carroll,
  • John Ervin,
  • Malissa C. Diehl,
  • Elliott Blackwood,
  • Mammen P. Mammen,
  • Jessica Lee,
  • Michael J. Dallas,
  • Ami Shah Brown,
  • Jacqueline E. Shea,
  • J.Joseph Kim,
  • David B. Weiner,
  • Kate E. Broderick,
  • Laurent M. Humeau

Journal volume & issue
Vol. 31
p. 100689

Abstract

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Background: A vaccine against SARS-CoV-2 is of high urgency. Here the safety and immunogenicity induced by a DNA vaccine (INO-4800) targeting the full length spike antigen of SARS-CoV-2 are described. Methods: INO-4800 was evaluated in two groups of 20 participants, receiving either 1.0 mg or 2.0 mg of vaccine intradermally followed by CELLECTRA® EP at 0 and 4 weeks. Thirty-nine subjects completed both doses; one subject in the 2.0 mg group discontinued trial participation prior to receiving the second dose. ClinicalTrials.gov identifier: NCT04336410. Findings: The median age was 34.5, 55% (22/40) were men and 82.5% (33/40) white. Through week 8, only 6 related Grade 1 adverse events in 5 subjects were observed. None of these increased in frequency with the second administration. No serious adverse events were reported. All 38 subjects evaluable for immunogenicity had cellular and/or humoral immune responses following the second dose of INO-4800. By week 6, 95% (36/38) of the participants seroconverted based on their responses by generating binding (ELISA) and/or neutralizing antibodies (PRNT IC50), with responder geometric mean binding antibody titers of 655.5 [95% CI (255.6, 1681.0)] and 994.2 [95% CI (395.3, 2500.3)] in the 1.0 mg and 2.0 mg groups, respectively. For neutralizing antibody, 78% (14/18) and 84% (16/19) generated a response with corresponding geometric mean titers of 102.3 [95% CI (37.4, 280.3)] and 63.5 [95% CI (39.6, 101.8)], in the respective groups. By week 8, 74% (14/19) and 100% (19/19) of subjects generated T cell responses by IFN-ɣ ELISpot assay with the median SFU per 106 PBMC of 46 [95% CI (21.1, 142.2)] and 71 [95% CI (32.2, 194.4)] in the 1.0 mg and 2.0 mg groups, respectively. Flow cytometry demonstrated a T cell response, dominated by CD8+ T cells co-producing IFN-ɣ and TNF-α, without increase in IL-4. Interpretation: INO-4800 demonstrated excellent safety and tolerability and was immunogenic in 100% (38/38) of the vaccinated subjects by eliciting either or both humoral or cellular immune responses. Funding: Coalition for Epidemic Preparedness Innovations (CEPI).

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