Structural basis for neutralization of Plasmodium vivax by naturally acquired human antibodies that target DBP

被引:0
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作者
Darya Urusova
Lenore Carias
Yining Huang
Vanessa C. Nicolete
Jean Popovici
Camille Roesch
Nichole D. Salinas
Sebastien Dechavanne
Benoit Witkowski
Marcelo U. Ferreira
John H. Adams
Michael L. Gross
Christopher L. King
Niraj H. Tolia
机构
[1] Washington University School of Medicine,Department of Molecular Microbiology
[2] Case Western Reserve University,Center for Global Health and Diseases
[3] Washington University in St Louis,Department of Chemistry
[4] University of Sao Paulo,Department of Parasitology
[5] Pasteur Institute in Cambodia,Malaria Molecular Epidemiology Unit
[6] National Institute of Allergy and Infectious Diseases,Laboratory of Malaria Immunology and Vaccinology
[7] National Institutes of Health,Department of Global Health, College of Public Health
[8] University of South Florida,Department of Chemistry
[9] Washington University in St Louis,Bioproduct Research and Development, Lilly Research Laboratories
[10] Eli Lilly and Company,undefined
来源
Nature Microbiology | 2019年 / 4卷
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摘要
The Plasmodium vivax Duffy-binding protein (DBP) is a prime target of the protective immune response and a promising vaccine candidate for P. vivax malaria. Naturally acquired immunity (NAI) protects against malaria in adults residing in infection-endemic regions, and the passive transfer of malarial immunity confers protection. A vaccine that replicates NAI will effectively prevent disease. Here, we report the structures of DBP region II in complex with human-derived, neutralizing monoclonal antibodies obtained from an individual in a malaria-endemic area with NAI. We identified protective epitopes using X-ray crystallography, hydrogen–deuterium exchange mass spectrometry, mutational mapping and P. vivax invasion studies. These approaches reveal that naturally acquired human antibodies neutralize P. vivax by targeting the binding site for Duffy antigen receptor for chemokines (DARC) and the dimer interface of P. vivax DBP. Antibody binding is unaffected by polymorphisms in the vicinity of epitopes, suggesting that the antibodies have evolved to engage multiple polymorphic variants of DBP. The human antibody epitopes are broadly conserved and are distinct from previously defined epitopes for broadly conserved murine monoclonal antibodies. A library of globally conserved epitopes of neutralizing human antibodies offers possibilities for rational design of strain-transcending DBP-based vaccines and therapeutics against P. vivax.
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页码:1486 / 1496
页数:10
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