Generation of a Peptide Vaccine Candidate against Falciparum Placental Malaria Based on a Discontinuous Epitope

In pregnant women, infected red blood cells adhere to the placenta via the parasite protein VAR2CSA. Two vaccine candidates based on VAR2CSA are currently in clinical trials; however, these candidates failed to elicit strain-transcending antibody responses. We previously showed that a cross-reactive...

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Published inVaccines (Basel) Vol. 8; no. 3; p. 392
Main Authors Mitran, Catherine J, Higa, Lauren M, Good, Michael F, Yanow, Stephanie K
Format Journal Article
LanguageEnglish
Published Switzerland MDPI AG 18.07.2020
MDPI
Subjects
Antibodies
Antigens
Chemical bonds
Clinical trials
Communication
Design
Disulfide bonds
Epitopes
Erythrocytes
Immunization
Malaria
Monoclonal antibodies
Parasites
peptide
Peptides
Placenta
placental malaria
Plasmodium falciparum
Plasmodium vivax
Pregnancy
Proteins
PvDBP
vaccine
Vaccines
Vector-borne diseases
Canada
United States > US
Netherlands
Plasmodium falciparum
Plasmodium vivax
PvDBP
peptide
vaccine
placental malaria
VAR2CSA
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Summary:In pregnant women, infected red blood cells adhere to the placenta via the parasite protein VAR2CSA. Two vaccine candidates based on VAR2CSA are currently in clinical trials; however, these candidates failed to elicit strain-transcending antibody responses. We previously showed that a cross-reactive monoclonal antibody (3D10) raised against the antigen PvDBP targets epitopes in VAR2CSA. We now aim to design a peptide vaccine against VAR2CSA based on the epitope that generated 3D10. We mapped the epitope to subdomain 1 (SD1) of PvDBP and identified a peptide that contained the minimal sequence. However, this peptide did not elicit cross-reactive VAR2CSA antibodies in mice. When tested against a broader, overlapping peptide array spanning SD1, 3D10 in fact recognized a discontinuous epitope consisting of three segments of SD1. These findings presented the challenge to generate this larger structural epitope as a synthetic peptide since it is stabilized by two pairs of disulfide bonds. We overcame this using a synthetic scaffold to conformationally constrain the SD1 peptide and coupled it to keyhole limpet hemocyanin (KLH). The SD1-KLH conjugate elicited antibodies in mice that cross-reacted with VAR2CSA. This strategy successfully recapitulated a discontinuous epitope with a synthetic peptide and represents the first heterologous vaccine candidate against VAR2CSA.
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ISSN:2076-393X
2076-393X
DOI:10.3390/vaccines8030392