Human sterile immunity to Plasmodium vivax malaria correlates with specific antibody response elicited by immunization with radiation-attenuated sporozoites

Author:

Lopez-Perez Mary1,Jain Aarti2,Davies D. Huw2,Vásquez-Jiménez Juan M.1,Herrera Sonia M3,Oñate José4,Felgner Philip L.2,Herrera Sócrates1,Arévalo-Herrera Myriam1

Affiliation:

1. Malaria Vaccine and Drug Development Center (MVDC), Cali, Colombia

2. University of California Irvine

3. Caucaseco Scientific Research Center

4. Centro Medico Imbanaco, QuironSalud

Abstract

Abstract Malaria sterile immunity has been reproducibly induced by immunization with Plasmodium radiation-attenuated sporozoites (RAS). Analyses of sera from RAS-immunized individuals allowed the identification of P. falciparum antigens, such as the circumsporozoite protein (CSP), the basis for the RTS, S vaccine. Similar advances in P. vivax (Pv) vaccination have been elusive. We previously reported 42% (5/12) of sterile protection in malaria-unexposed, Duffy-positive (Fy+) volunteers immunized with PvRAS followed by a controlled human malaria infection (CHMI). Using a custom protein microarray displaying 515 Pv antigens, we found that PvRAS group seroreactivity was lower in protected than non-protected volunteers. Nevertheless, protected volunteers showed higher reactivity to PvCSP and other antigens. In Fy- volunteers immunized with non-irradiated Pv-infected mosquitoes, parasite reactivity increased throughout immunizations. Mock-vaccinated Fy + volunteers developed a vigorous response to CHMI. These findings allowed the identification of novel parasite antigens currently being pursued as vaccine candidates.

Publisher

Research Square Platform LLC

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