| dc.contributor.author |
Payne RO, Silk SE, Elias SC, Miura K, Diouf A, Galaway F, de Graaf H, Brendish NJ, Poulton ID, Griffiths OJ, Edwards NJ, Jin J, Labbé GM, Alanine DG, Siani L, Di Marco S, Roberts R, Green N, Berrie E, Ishizuka AS, Nielsen CM, Bardelli M, Partey FD, Ofori MF, Barfod L, Wambua J, Murungi LM, Osier FH, Biswas S, McCarthy JS, Minassian AM, Ashfield R, Viebig NK, Nugent FL, Douglas AD, Vekemans J, Wright GJ, Faust SN, Hill AV, Long CA, Lawrie AM, Draper SJ. |
|
| dc.description.abstract |
The development of a highly effective vaccine remains a key strategic goal to aid the
control and eventual eradication of Plasmodium falciparum malaria. In recent years, the
reticulocyte-binding protein homolog 5 (RH5) has emerged as the most promising bloodstage P. falciparum candidate antigen to date, capable of conferring protection against
stringent challenge in Aotus monkeys. We report on the first clinical trial to our
knowledge to assess the RH5 antigen - a dose-escalation phase Ia study in 24 healthy,
malaria-naive adult volunteers. We utilized established viral vectors, the replicationdeficient chimpanzee adenovirus serotype 63 (ChAd63), and the attenuated
orthopoxvirus modified vaccinia virus Ankara (MVA), encoding RH5 from the 3D7
clone of P. falciparum. Vaccines were administered i.m. in a heterologous prime-boost
regimen using an 8-week interval and were well tolerated. Vaccine-induced anti-RH5
serum antibodies exhibited cross-strain functional growth inhibition activity (GIA) in
vitro, targeted linear and conformational epitopes within RH5, and inhibited key
interactions within the RH5 invasion complex. This is the first time to our knowledge
that substantial RH5-specific responses have been induced by immunization in humans,
with levels greatly exceeding the serum antibody responses observed in African adults
following years of natural malaria exposure. These data support the progression of RH5-
based vaccines to human efficacy testing. |
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