Research

Satisfactory safety and immunogenicity of MSP3 malaria vaccine candidate in Tanzanian children aged 12–24 months

John PA Lusingu^1*, Samwel Gesase¹, Salum Msham¹, Filbert Francis¹, Martha Lemnge¹, Misago Seth¹, Samwel Sembuche¹, Acleus Rutta¹, Daniel Minja¹, Method D Segeja¹, Samuel Bosomprah², Simon Cousens², Ramadhani Noor³, Roma Chilengi³ and Pierre Druilhe⁴

• * Corresponding author: John PA Lusingu jpalusingu@yahoo.co.uk

Author Affiliations

¹ National Institute for Medical Research, Tanga Centre, Tanzania

² London School of Hygiene and Tropical Medicine, London, UK

³ African Malaria Network Trust, Dar es Salaam, Tanzania

⁴ Institut Pasteur Paris, Paris, France

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Malaria Journal 2009, 8:163 doi:10.1186/1475-2875-8-163

Published: 17 July 2009

Abstract

Background

Development and deployment of an effective malaria vaccine would complement existing malaria control measures. A blood stage malaria vaccine candidate, Merozoite Surface Protein-3 (MSP3), produced as a long synthetic peptide, has been shown to be safe in non-immune and semi-immune adults. A phase Ib dose-escalating study was conducted to assess the vaccine's safety and immunogenicity in children aged 12 to 24 months in Korogwe, Tanzania (ClinicalTrials.gov number: NCT00469651).

Methods

This was a double-blind, randomized, controlled, dose escalation phase Ib trial, in which children were given one of two different doses of the MSP3 antigen (15 μg or 30 μg) or a control vaccine (Engerix B). Children were randomly allocated either to the MSP3 candidate malaria vaccine or the control vaccine administered at a schedule of 0, 1, and 2 months. Immunization with lower and higher doses was staggered for safety reasons starting with the lower dose. The primary endpoint was safety and reactogenicity within 28 days post-vaccination. Blood samples were obtained at different time points to measure immunological responses. Results are presented up to 84 days post-vaccination.

Results

A total of 45 children were enrolled, 15 in each of the two MSP3 dose groups and 15 in the Engerix B group. There were no important differences in reactogenicity between the two MSP3 groups and Engerix B. Grade 3 adverse events were infrequent; only five were detected throughout the study, all of which were transient and resolved without sequelae. No serious adverse event reported was considered to be related to MSP3 vaccine. Both MSP3 dose regimens elicited strong cytophilic IgG responses (subclasses IgG1 and IgG3), the isotypes involved in the monocyte-dependant mechanism of Plasmodium falciparum parasite-killing. The titers reached are similar to those from African adults having reached a state of premunition. Furthermore, vaccination induced seroconversion in all vaccinees.

Conclusion

The MSP3 malaria vaccine candidate was safe, well tolerated and immunogenic in children aged 12–24 months living in a malaria endemic community. Given the vaccine's safety and its induction of cytophilic IgG responses, its efficacy against P. falciparum infection and disease needs to be evaluated in Phase 2 studies.