PLoS ONE (Jan 2009)

Phase 1/2a study of the malaria vaccine candidate apical membrane antigen-1 (AMA-1) administered in adjuvant system AS01B or AS02A.

  • Michele D Spring,
  • James F Cummings,
  • Christian F Ockenhouse,
  • Sheetij Dutta,
  • Randall Reidler,
  • Evelina Angov,
  • Elke Bergmann-Leitner,
  • V Ann Stewart,
  • Stacey Bittner,
  • Laure Juompan,
  • Mark G Kortepeter,
  • Robin Nielsen,
  • Urszula Krzych,
  • Ev Tierney,
  • Lisa A Ware,
  • Megan Dowler,
  • Cornelus C Hermsen,
  • Robert W Sauerwein,
  • Sake J de Vlas,
  • Opokua Ofori-Anyinam,
  • David E Lanar,
  • Jack L Williams,
  • Kent E Kester,
  • Kathryn Tucker,
  • Meng Shi,
  • Elissa Malkin,
  • Carole Long,
  • Carter L Diggs,
  • Lorraine Soisson,
  • Marie-Claude Dubois,
  • W Ripley Ballou,
  • Joe Cohen,
  • D Gray Heppner

DOI
https://doi.org/10.1371/journal.pone.0005254
Journal volume & issue
Vol. 4, no. 4
p. e5254

Abstract

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This Phase 1/2a study evaluated the safety, immunogenicity, and efficacy of an experimental malaria vaccine comprised of the recombinant Plasmodium falciparum protein apical membrane antigen-1 (AMA-1) representing the 3D7 allele formulated with either the AS01B or AS02A Adjuvant Systems.After a preliminary safety evaluation of low dose AMA-1/AS01B (10 microg/0.5 mL) in 5 adults, 30 malaria-naïve adults were randomly allocated to receive full dose (50 microg/0.5 mL) of AMA-1/AS01B (n = 15) or AMA-1/AS02A (n = 15), followed by a malaria challenge. All vaccinations were administered intramuscularly on a 0-, 1-, 2-month schedule. All volunteers experienced transient injection site erythema, swelling and pain. Two weeks post-third vaccination, anti-AMA-1 Geometric Mean Antibody Concentrations (GMCs) with 95% Confidence Intervals (CIs) were high: low dose AMA-1/AS01B 196 microg/mL (103-371 microg/mL), full dose AMA-1/AS01B 279 microg/mL (210-369 microg/mL) and full dose AMA-1/AS02A 216 microg/mL (169-276 microg/mL) with no significant difference among the 3 groups. The three vaccine formulations elicited equivalent functional antibody responses, as measured by growth inhibition assay (GIA), against homologous but not against heterologous (FVO) parasites as well as demonstrable interferon-gamma (IFN-gamma) responses. To assess efficacy, volunteers were challenged with P. falciparum-infected mosquitoes, and all became parasitemic, with no significant difference in the prepatent period by either light microscopy or quantitative polymerase chain reaction (qPCR). However, a small but significant reduction of parasitemia in the AMA-1/AS02A group was seen with a statistical model employing qPCR measurements.All three vaccine formulations were found to be safe and highly immunogenic. These immune responses did not translate into significant vaccine efficacy in malaria-naïve adults employing a primary sporozoite challenge model, but encouragingly, estimation of parasite growth rates from qPCR data may suggest a partial biological effect of the vaccine. Further evaluation of the immunogenicity and efficacy of the AMA-1/AS02A formulation is ongoing in a malaria-experienced pediatric population in Mali.www.clinicaltrials.gov NCT00385047.