A human monoclonal antibody blocks malaria transmission and defines a highly conserved neutralizing epitope on gametes

Author:

Coelho Camila H.,Tang Wai Kwan,Burkhardt Martin,Galson Jacob D.ORCID,Muratova Olga,Salinas Nichole D.,Alves e Silva Thiago Luiz,Reiter Karine,MacDonald Nicholas J.ORCID,Nguyen Vu,Herrera Raul,Shimp Richard,Narum David L.ORCID,Byrne-Steele Miranda,Pan Wenjing,Hou Xiaohong,Brown Brittany,Eisenhower Mary,Han Jian,Jenkins Bethany J.,Doritchamou Justin Y. A.ORCID,Smelkinson Margery G.ORCID,Vega-Rodríguez Joel,Trück JohannesORCID,Taylor Justin J.ORCID,Sagara Issaka,Renn Jonathan P.,Tolia Niraj H.ORCID,Duffy Patrick E.ORCID

Abstract

AbstractMalaria elimination requires tools that interrupt parasite transmission. Here, we characterize B cell receptor responses among Malian adults vaccinated against the first domain of the cysteine-rich 230 kDa gamete surface protein Pfs230, a key protein in sexual stage development of P. falciparum parasites. Among nine Pfs230 human monoclonal antibodies (mAbs) that we generated, one potently blocks transmission to mosquitoes in a complement-dependent manner and reacts to the gamete surface; the other eight show only low or no blocking activity. The structure of the transmission-blocking mAb in complex with vaccine antigen reveals a large discontinuous conformational epitope, specific to domain 1 of Pfs230 and comprising six structural elements in the protein. The epitope is conserved, suggesting the transmission-blocking mAb is broadly functional. This study provides a rational basis to improve malaria vaccines and develop therapeutic antibodies for malaria elimination.

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry

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