Vaccination with Plasmodium vivax Duffy-binding protein inhibits parasite growth during controlled human malaria infection.
Mimi M HouJordan R BarrettYrene ThemistocleousThomas A RawlinsonAbabacar DioufFrancisco José MartínezCarolyn M NielsenAmelia M LiasLloyd D W KingNick J EdwardsNicola M GreenwoodLucy KinghamIan D PoultonBaktash KhozoeeCyndi G GeogheganSusanne H HodgsonDylan J Mac LochlainnJo SalkeldMicheline Guillotte-BlisnickChristèle HuonFranziska MohringJenny M ReimerVirander S ChauhanPaushali MukherjeeSumi BiswasIona J BrianAlison M LawrieJee-Sun ChoFay L NugentCarole A LongRobert William MoonKazutoyo MiuraSarah E SilkChetan E ChitnisAngela M MinassianSimon J DraperPublished in: Science translational medicine (2023)
There are no licensed vaccines against Plasmodium vivax . We conducted two phase 1/2a clinical trials to assess two vaccines targeting P. vivax Duffy-binding protein region II (PvDBPII). Recombinant viral vaccines using chimpanzee adenovirus 63 (ChAd63) and modified vaccinia virus Ankara (MVA) vectors as well as a protein and adjuvant formulation (PvDBPII/Matrix-M) were tested in both a standard and a delayed dosing regimen. Volunteers underwent controlled human malaria infection (CHMI) after their last vaccination, alongside unvaccinated controls. Efficacy was assessed by comparisons of parasite multiplication rates in the blood. PvDBPII/Matrix-M, given in a delayed dosing regimen, elicited the highest antibody responses and reduced the mean parasite multiplication rate after CHMI by 51% ( n = 6) compared with unvaccinated controls ( n = 13), whereas no other vaccine or regimen affected parasite growth. Both viral-vectored and protein vaccines were well tolerated and elicited expected, short-lived adverse events. Together, these results support further clinical evaluation of the PvDBPII/Matrix-M P. vivax vaccine.