| Literature DB >> 33857426 |
Carola Schäfer1, Nicholas Dambrauskas1, Laura M Reynolds1, Olesya Trakhimets1, Andrew Raappana1, Erika L Flannery1, Wanlapa Roobsoong2, Jetsumon Sattabongkot2, Sebastian A Mikolajczak1, Stefan H I Kappe3, D Noah Sather4.
Abstract
Latent forms of Plasmodium vivax, called hypnozoites, cause malaria relapses from the liver into the bloodstream and are a major obstacle to malaria eradication. To experimentally assess the impact of a partially protective pre-erythrocytic vaccine on reducing Plasmodium vivax relapses, we developed a liver-humanized mouse model that allows monitoring of relapses directly in the blood. We passively infused these mice with a suboptimal dose of an antibody that targets the circumsporozoite protein prior to challenge with P. vivax sporozoites. Although this regimen did not completely prevent primary infection, antibody-treated mice experienced 62% fewer relapses. The data constitute unprecedented direct experimental evidence that suboptimal efficacy of infection-blocking antibodies, while not completely preventing primary infection, has a pronounced benefit in reducing the number of relapses. These findings suggest that a partially efficacious pre-erythrocytic Plasmodium vivax vaccine can have a disproportionately high impact in positive public health outcomes.Entities:
Keywords: Plasmodium vivax; circumsporozoite protein; humanized mouse; liver chimeric mouse; pre-erythrocytic vaccine; relapsing malaria
Year: 2021 PMID: 33857426 DOI: 10.1016/j.chom.2021.03.011
Source DB: PubMed Journal: Cell Host Microbe ISSN: 1931-3128 Impact factor: 21.023