Insight into Antigenic Diversity of VAR2CSA-DBL5ε Domain from Multiple Plasmodium falciparum Placental Isolates

BACKGROUND: Protection against pregnancy associated malaria (PAM) is associated with high levels of anti-VAR2CSA antibodies. This protection is obtained by the parity dependent acquisition of anti-VAR2CSA antibodies. Distinct parity-associated molecular signatures have been identified in VAR2CSA dom...

Descripción completa

Detalles Bibliográficos
Autores principales: Gnidehou, Sédami, Jessen, Leon, Gangnard, Stéphane, Ermont, Caroline, Triqui, Choukri, Quiviger, Mickael, Guitard, Juliette, Lund, Ole, Deloron, Philippe, Ndam, Nicaise Tuikue
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2010
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2948511/
https://www.ncbi.nlm.nih.gov/pubmed/20957045
http://dx.doi.org/10.1371/journal.pone.0013105
_version_ 1782187473742331904
author Gnidehou, Sédami
Jessen, Leon
Gangnard, Stéphane
Ermont, Caroline
Triqui, Choukri
Quiviger, Mickael
Guitard, Juliette
Lund, Ole
Deloron, Philippe
Ndam, Nicaise Tuikue
author_facet Gnidehou, Sédami
Jessen, Leon
Gangnard, Stéphane
Ermont, Caroline
Triqui, Choukri
Quiviger, Mickael
Guitard, Juliette
Lund, Ole
Deloron, Philippe
Ndam, Nicaise Tuikue
author_sort Gnidehou, Sédami
collection PubMed
description BACKGROUND: Protection against pregnancy associated malaria (PAM) is associated with high levels of anti-VAR2CSA antibodies. This protection is obtained by the parity dependent acquisition of anti-VAR2CSA antibodies. Distinct parity-associated molecular signatures have been identified in VAR2CSA domains. These two observations combined point to the importance of identifying VAR2CSA sequence variation, which facilitate parasitic evasion or subversion of host immune response. Highly conserved domains of VAR2CSA such as DBL5ε are likely to contain conserved epitopes, and therefore do constitute attractive targets for vaccine development. METHODOLOGY/PRINCIPAL FINDINGS: VAR2CSA DBL5ε-domain sequences obtained from cDNA of 40 placental isolates were analysed by a combination of experimental and in silico methods. Competition ELISA assays on two DBL5ε variants, using plasma samples from women from two different areas and specific mice hyperimmune plasma, indicated that DBL5ε possess conserved and cross-reactive B cell epitopes. Peptide ELISA identified conserved areas that are recognised by naturally acquired antibodies. Specific antibodies against these peptides labelled the native proteins on the surface of placental parasites. Despite high DBL5ε sequence homology among parasite isolates, sequence analyses identified motifs in DBL5ε that discriminate parasites according to donor's parity. Moreover, recombinant proteins of two VAR2CSA DBL5ε variants displayed diverse recognition patterns by plasma from malaria-exposed women, and diverse proteoglycan binding abilities. CONCLUSIONS/SIGNIFICANCE: This study provides insights into conserved and exposed B cell epitopes in DBL5ε that might be a focus for cross reactivity. The importance of sequence variation in VAR2CSA as a critical challenge for vaccine development is highlighted. VAR2CSA conformation seems to be essential to its functionality. Therefore, identification of sequence variation sites in distinct locations within VAR2CSA, affecting antigenicity and/or binding properties, is critical to the effort of developing an efficient VAR2CSA-based vaccine. Motifs associated with parasite segregation according to parity constitute one such site.
format Text
id pubmed-2948511
institution National Center for Biotechnology Information
language English
publishDate 2010
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-29485112010-10-18 Insight into Antigenic Diversity of VAR2CSA-DBL5ε Domain from Multiple Plasmodium falciparum Placental Isolates Gnidehou, Sédami Jessen, Leon Gangnard, Stéphane Ermont, Caroline Triqui, Choukri Quiviger, Mickael Guitard, Juliette Lund, Ole Deloron, Philippe Ndam, Nicaise Tuikue PLoS One Research Article BACKGROUND: Protection against pregnancy associated malaria (PAM) is associated with high levels of anti-VAR2CSA antibodies. This protection is obtained by the parity dependent acquisition of anti-VAR2CSA antibodies. Distinct parity-associated molecular signatures have been identified in VAR2CSA domains. These two observations combined point to the importance of identifying VAR2CSA sequence variation, which facilitate parasitic evasion or subversion of host immune response. Highly conserved domains of VAR2CSA such as DBL5ε are likely to contain conserved epitopes, and therefore do constitute attractive targets for vaccine development. METHODOLOGY/PRINCIPAL FINDINGS: VAR2CSA DBL5ε-domain sequences obtained from cDNA of 40 placental isolates were analysed by a combination of experimental and in silico methods. Competition ELISA assays on two DBL5ε variants, using plasma samples from women from two different areas and specific mice hyperimmune plasma, indicated that DBL5ε possess conserved and cross-reactive B cell epitopes. Peptide ELISA identified conserved areas that are recognised by naturally acquired antibodies. Specific antibodies against these peptides labelled the native proteins on the surface of placental parasites. Despite high DBL5ε sequence homology among parasite isolates, sequence analyses identified motifs in DBL5ε that discriminate parasites according to donor's parity. Moreover, recombinant proteins of two VAR2CSA DBL5ε variants displayed diverse recognition patterns by plasma from malaria-exposed women, and diverse proteoglycan binding abilities. CONCLUSIONS/SIGNIFICANCE: This study provides insights into conserved and exposed B cell epitopes in DBL5ε that might be a focus for cross reactivity. The importance of sequence variation in VAR2CSA as a critical challenge for vaccine development is highlighted. VAR2CSA conformation seems to be essential to its functionality. Therefore, identification of sequence variation sites in distinct locations within VAR2CSA, affecting antigenicity and/or binding properties, is critical to the effort of developing an efficient VAR2CSA-based vaccine. Motifs associated with parasite segregation according to parity constitute one such site. Public Library of Science 2010-10-01 /pmc/articles/PMC2948511/ /pubmed/20957045 http://dx.doi.org/10.1371/journal.pone.0013105 Text en Gnidehou et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Gnidehou, Sédami
Jessen, Leon
Gangnard, Stéphane
Ermont, Caroline
Triqui, Choukri
Quiviger, Mickael
Guitard, Juliette
Lund, Ole
Deloron, Philippe
Ndam, Nicaise Tuikue
Insight into Antigenic Diversity of VAR2CSA-DBL5ε Domain from Multiple Plasmodium falciparum Placental Isolates
title Insight into Antigenic Diversity of VAR2CSA-DBL5ε Domain from Multiple Plasmodium falciparum Placental Isolates
title_full Insight into Antigenic Diversity of VAR2CSA-DBL5ε Domain from Multiple Plasmodium falciparum Placental Isolates
title_fullStr Insight into Antigenic Diversity of VAR2CSA-DBL5ε Domain from Multiple Plasmodium falciparum Placental Isolates
title_full_unstemmed Insight into Antigenic Diversity of VAR2CSA-DBL5ε Domain from Multiple Plasmodium falciparum Placental Isolates
title_short Insight into Antigenic Diversity of VAR2CSA-DBL5ε Domain from Multiple Plasmodium falciparum Placental Isolates
title_sort insight into antigenic diversity of var2csa-dbl5ε domain from multiple plasmodium falciparum placental isolates
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2948511/
https://www.ncbi.nlm.nih.gov/pubmed/20957045
http://dx.doi.org/10.1371/journal.pone.0013105
work_keys_str_mv AT gnidehousedami insightintoantigenicdiversityofvar2csadbl5edomainfrommultipleplasmodiumfalciparumplacentalisolates
AT jessenleon insightintoantigenicdiversityofvar2csadbl5edomainfrommultipleplasmodiumfalciparumplacentalisolates
AT gangnardstephane insightintoantigenicdiversityofvar2csadbl5edomainfrommultipleplasmodiumfalciparumplacentalisolates
AT ermontcaroline insightintoantigenicdiversityofvar2csadbl5edomainfrommultipleplasmodiumfalciparumplacentalisolates
AT triquichoukri insightintoantigenicdiversityofvar2csadbl5edomainfrommultipleplasmodiumfalciparumplacentalisolates
AT quivigermickael insightintoantigenicdiversityofvar2csadbl5edomainfrommultipleplasmodiumfalciparumplacentalisolates
AT guitardjuliette insightintoantigenicdiversityofvar2csadbl5edomainfrommultipleplasmodiumfalciparumplacentalisolates
AT lundole insightintoantigenicdiversityofvar2csadbl5edomainfrommultipleplasmodiumfalciparumplacentalisolates
AT deloronphilippe insightintoantigenicdiversityofvar2csadbl5edomainfrommultipleplasmodiumfalciparumplacentalisolates
AT ndamnicaisetuikue insightintoantigenicdiversityofvar2csadbl5edomainfrommultipleplasmodiumfalciparumplacentalisolates

Ejemplares similares