Repeat controlled human malaria infection of healthy UK adults with blood-stage Plasmodium falciparum: Safety and parasite growth dynamics

Author:

Salkeld Jo,Themistocleous Yrene,Barrett Jordan R.,Mitton Celia H.,Rawlinson Thomas A.,Payne Ruth O.,Hou Mimi M.,Khozoee Baktash,Edwards Nick J.,Nielsen Carolyn M.,Sandoval Diana Muñoz,Bach Florian A.,Nahrendorf Wiebke,Ramon Raquel Lopez,Baker Megan,Ramos-Lopez Fernando,Folegatti Pedro M.,Quinkert Doris,Ellis Katherine J.,Poulton Ian D.,Lawrie Alison M.,Cho Jee-Sun,Nugent Fay L.,Spence Philip J.,Silk Sarah E.,Draper Simon J.,Minassian Angela M.

Abstract

In endemic settings it is known that natural malaria immunity is gradually acquired following repeated exposures. Here we sought to assess whether similar acquisition of blood-stage malaria immunity would occur following repeated parasite exposure by controlled human malaria infection (CHMI). We report the findings of repeat homologous blood-stage Plasmodium falciparum (3D7 clone) CHMI studies VAC063C (ClinicalTrials.gov NCT03906474) and VAC063 (ClinicalTrials.gov NCT02927145). In total, 24 healthy, unvaccinated, malaria-naïve UK adult participants underwent primary CHMI followed by drug treatment. Ten of these then underwent secondary CHMI in the same manner, and then six of these underwent a final tertiary CHMI. As with primary CHMI, malaria symptoms were common following secondary and tertiary infection, however, most resolved within a few days of treatment and there were no long term sequelae or serious adverse events related to CHMI. Despite detectable induction and boosting of anti-merozoite serum IgG antibody responses following each round of CHMI, there was no clear evidence of anti-parasite immunity (manifest as reduced parasite growth in vivo) conferred by repeated challenge with the homologous parasite in the majority of volunteers. However, three volunteers showed some variation in parasite growth dynamics in vivo following repeat CHMI that were either modest or short-lived. We also observed no major differences in clinical symptoms or laboratory markers of infection across the primary, secondary and tertiary challenges. However, there was a trend to more severe pyrexia after primary CHMI and the absence of a detectable transaminitis post-treatment following secondary and tertiary infection. We hypothesize that this could represent the initial induction of clinical immunity. Repeat homologous blood-stage CHMI is thus safe and provides a model with the potential to further the understanding of naturally acquired immunity to blood-stage infection in a highly controlled setting.Clinical Trial RegistrationClinicalTrials.gov, identifier NCT03906474, NCT02927145.

Funder

United States Agency for International Development

Publisher

Frontiers Media SA

Subject

Immunology,Immunology and Allergy

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