4.5 Article

Preliminary studies on the immunogenicity of a prime-and-trap malaria vaccine in nonhuman primates

Journal

VACCINE
Volume 41, Issue 38, Pages 5494-5498

Publisher

ELSEVIER SCI LTD
DOI: 10.1016/j.vaccine.2023.07.067

Keywords

Malaria; Vaccine; Macaque

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The development of next-generation vaccines against Plasmodium falciparum (Pf) is a priority. Many existing malaria vaccines target the pre-erythrocytic sporozoite (SPZ) and liver stages, but they require multiple doses and have suboptimal efficacy against field-transmitted malaria.
Development of next-generation vaccines against Plasmodium falciparum (Pf) is a priority. Many malaria vaccines target the pre-erythrocytic sporozoite (SPZ) and liver stages. These include subunit vaccines based on the Pf circumsporozoite protein (CSP) and attenuated PfSPZ vaccines. However, these strategies require 3-4 doses and have not achieved optimal efficacy against field-transmitted malaria. Prime-and-trap is a recently developed twostep heterologous vaccine strategy that combines priming with DNA encoding CSP followed by a single dose of attenuated SPZ. This strategy aims to induce CD8+ T cells that can eliminate parasites in the liver. Prior data has demonstrated that prime-and-trap with P. yoelii CSP and PySPZ was immunogenic and protective in mice. Here we report preliminary data on the immunogenicity of PfCSP prime and PfSPZ trap vaccine in rhesus macaques. This vaccine induced PfCSP-specific antibodies and T cell responses in all animals. However, response magnitude differed between individuals, suggesting further study is required.

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