Prime-boost vaccination with chimpanzee adenovirus and modified vaccinia Ankara encoding TRAP provides partial protection against <i>Plasmodium falciparum</i> infection in Kenyan adults

Caroline Ogwang; Domtila Kimani; Nick J. Edwards; Rachel Roberts; Jedidah Mwacharo; Georgina Bowyer; Carly M. Bliss; Susanne H. Hodgson; Patricia Njuguna; Nicola K. Viebig; Alfredo Nicosia; Evelyn Gitau; Sandy Douglas; Joe Illingworth; Kevin Marsh; Alison M. Lawrie; Egeruan B. Imoukhuede; Katie Ewer; Britta C. Urban; Adrian V. S. Hill; Philip Bejon; the MVVC group; Odile Leroy; Badara Cissé; Sodiomon B. Sirima; Kalifa Bojang; Georgina Murphy; Henry Karanja; Lydiah Nyamako; Simone de Cassan; Ken Awuondo; Dominic Kwiatkowski; Kirk A. Rockett; Sarah C. Gilbert; Nicholas Anagnostou; Peninah Soipei; Judy Peshu; Ines Petersen; Brian Mutinda; Naomi Waithira; Mahfudh M. Bashraheil; Jimmy Shangala; Sarah Moyle; Eleanor Berrie; Geoffrey Targett; Mahamadou A. Théra; Paul Milligan; Bernhards Ogutu; Anthony Etyang

doi:10.1126/scitranslmed.aaa2373

Prime-boost vaccination with chimpanzee adenovirus and modified vaccinia Ankara encoding TRAP provides partial protection against <i>Plasmodium falciparum</i> infection in Kenyan adults

Caroline Ogwang(Kenya Medical Research Institute), Domtila Kimani(Kenya Medical Research Institute), Nick J. Edwards(Angkor Hospital for Children), Rachel Roberts(Angkor Hospital for Children), Jedidah Mwacharo(Kenya Medical Research Institute), Georgina Bowyer(Jenner Institute), Carly M. Bliss(Jenner Institute), Susanne H. Hodgson(Angkor Hospital for Children), Patricia Njuguna(Kenya Medical Research Institute), Nicola K. Viebig(Vienna Vaccine Safety Initiative), Alfredo Nicosia(European Federation of Animal Science), Evelyn Gitau(Kenya Medical Research Institute), Sandy Douglas(Angkor Hospital for Children), Joe Illingworth(Jenner Institute), Kevin Marsh(Angkor Hospital for Children), Alison M. Lawrie(Angkor Hospital for Children), Egeruan B. Imoukhuede(Angkor Hospital for Children), Katie Ewer(Jenner Institute), Britta C. Urban(Liverpool School of Tropical Medicine), Adrian V. S. Hill(Angkor Hospital for Children), Philip Bejon(Angkor Hospital for Children), the MVVC group, Odile Leroy, Badara Cissé, Sodiomon B. Sirima, Kalifa Bojang(Jenner Institute), Georgina Murphy, Henry Karanja, Lydiah Nyamako, Simone de Cassan, Ken Awuondo, Dominic Kwiatkowski, Kirk A. Rockett, Sarah C. Gilbert, Nicholas Anagnostou, Peninah Soipei, Judy Peshu, Ines Petersen, Brian Mutinda, Naomi Waithira, Mahfudh M. Bashraheil, Jimmy Shangala, Sarah Moyle, Eleanor Berrie, Geoffrey Targett, Mahamadou A. Théra, Paul Milligan, Bernhards Ogutu, Anthony Etyang

Science Translational Medicine

May 6, 2015

10.1126/scitranslmed.aaa2373

Cited by 131

Abstract

Protective immunity to the liver stage of the malaria parasite can be conferred by vaccine-induced T cells, but no subunit vaccination approach based on cellular immunity has shown efficacy in field studies. We randomly allocated 121 healthy adult male volunteers in Kilifi, Kenya, to vaccination with the recombinant viral vectors chimpanzee adenovirus 63 (ChAd63) and modified vaccinia Ankara (MVA), both encoding the malaria peptide sequence ME-TRAP (the multiple epitope string and thrombospondin-related adhesion protein), or to vaccination with rabies vaccine as a control. We gave antimalarials to clear parasitemia and conducted PCR (polymerase chain reaction) analysis on blood samples three times a week to identify infection with the malaria parasite Plasmodium falciparum. On Cox regression, vaccination reduced the risk of infection by 67% [95% confidence interval (CI), 33 to 83%; P = 0.002] during 8 weeks of monitoring. T cell responses to TRAP peptides 21 to 30 were significantly associated with protection (hazard ratio, 0.24; 95% CI, 0.08 to 0.75; P = 0.016).

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