An evolutionary approach to identify potentially protective B cell epitopes involved in naturally acquired immunity to malaria and the role of EBA-175 in protection amongst denizens of Bolifamba, Cameroon

BACKGROUND: The search for a vaccine against malaria caused by Plasmodium falciparum has lasted for more than 100 years, with considerable progress in the identification of a number of vaccine candidates. The post-genomic era offers new opportunities for an expedited search using rational vaccine de...

Descripción completa

Detalles Bibliográficos
Autores principales: Nyasa, Raymond B., Kimbi, Helen K., Zofou, Denis, DeBarry, Jeremy D., Kissinger, Jessica C., Titanji, Vincent P. K.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2016
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4875671/
https://www.ncbi.nlm.nih.gov/pubmed/27207101
http://dx.doi.org/10.1186/s12936-016-1337-z
_version_ 1782433134785069056
author Nyasa, Raymond B.
Kimbi, Helen K.
Zofou, Denis
DeBarry, Jeremy D.
Kissinger, Jessica C.
Titanji, Vincent P. K.
author_facet Nyasa, Raymond B.
Kimbi, Helen K.
Zofou, Denis
DeBarry, Jeremy D.
Kissinger, Jessica C.
Titanji, Vincent P. K.
author_sort Nyasa, Raymond B.
collection PubMed
description BACKGROUND: The search for a vaccine against malaria caused by Plasmodium falciparum has lasted for more than 100 years, with considerable progress in the identification of a number of vaccine candidates. The post-genomic era offers new opportunities for an expedited search using rational vaccine design and prioritization of key B-cell epitopes involved in natural acquired immunity. METHODS: Malaria vaccine candidate genes that have reached clinical trial were searched on an evolutionary relationship tree, to determine their level of lineage-specificity. Ten other genes with similar protein features and level of lineage specificity to the vaccine candidates were randomly selected, and computationally evaluated for the presence of B-cell epitopes. The protein fragment with maximum probability of putative epitopes were synthesized and used in an ELISA experiment to determine the presence of antibodies to these peptides, in the serum of malaria patients and healthy malaria uninfected inhabitants from a malaria endemic region (Bolifamba), alongside with a vaccine candidate EBA-175. RESULTS: Two peptide fragments of 25 and 30 amino acid length from PF3D7_1233400 and PF3D7_1437500 respectively, coded as PF4-123 and PF4-143 were shown to contain B-cell epitope(s). Total IgG antibodies to these peptides were not significantly different between sick and healthy participants, but cytophilic antibodies to these peptides were significantly higher in healthy participants (p < 0.03). Total IgG to the vaccine candidate EBA-175 was significantly higher in sick participants than in healthy participants, likewise cytophilic antibodies (p < 0.04). Antibodies to the peptides PF4-123 and PF4-143 correlated negatively (p = 0.025 and 0.008 and r = −0.291 and −0.345, respectively) to parasite load. Total IgG antibodies to EBA-175 showed a negative correlation to parasite load (r = −0.144), which was not significant (p = 0.276). Duration of stay in Bolifamba also negatively correlated with parasite load (p = 0.026, r = −0.419) and total IgG to PF4-143 was significantly associated with prolonged duration of stay in the locality of Bolifamba, Cameroon (p = 0.006, r = 0.361). CONCLUSIONS: The present study has identified two genes PF3D7_1233400 and PF3D7_1437500 containing peptide fragment (PF4-123 and PF4-143) with B-cell epitopes that are correlated with naturally acquired immunity to malaria. A pipeline has been developed for rapid identification of other B-cell epitopes involved in naturally acquired immunity.
format Online
Article
Text
id pubmed-4875671
institution National Center for Biotechnology Information
language English
publishDate 2016
publisher BioMed Central
record_format MEDLINE/PubMed
spelling pubmed-48756712016-05-22 An evolutionary approach to identify potentially protective B cell epitopes involved in naturally acquired immunity to malaria and the role of EBA-175 in protection amongst denizens of Bolifamba, Cameroon Nyasa, Raymond B. Kimbi, Helen K. Zofou, Denis DeBarry, Jeremy D. Kissinger, Jessica C. Titanji, Vincent P. K. Malar J Research BACKGROUND: The search for a vaccine against malaria caused by Plasmodium falciparum has lasted for more than 100 years, with considerable progress in the identification of a number of vaccine candidates. The post-genomic era offers new opportunities for an expedited search using rational vaccine design and prioritization of key B-cell epitopes involved in natural acquired immunity. METHODS: Malaria vaccine candidate genes that have reached clinical trial were searched on an evolutionary relationship tree, to determine their level of lineage-specificity. Ten other genes with similar protein features and level of lineage specificity to the vaccine candidates were randomly selected, and computationally evaluated for the presence of B-cell epitopes. The protein fragment with maximum probability of putative epitopes were synthesized and used in an ELISA experiment to determine the presence of antibodies to these peptides, in the serum of malaria patients and healthy malaria uninfected inhabitants from a malaria endemic region (Bolifamba), alongside with a vaccine candidate EBA-175. RESULTS: Two peptide fragments of 25 and 30 amino acid length from PF3D7_1233400 and PF3D7_1437500 respectively, coded as PF4-123 and PF4-143 were shown to contain B-cell epitope(s). Total IgG antibodies to these peptides were not significantly different between sick and healthy participants, but cytophilic antibodies to these peptides were significantly higher in healthy participants (p < 0.03). Total IgG to the vaccine candidate EBA-175 was significantly higher in sick participants than in healthy participants, likewise cytophilic antibodies (p < 0.04). Antibodies to the peptides PF4-123 and PF4-143 correlated negatively (p = 0.025 and 0.008 and r = −0.291 and −0.345, respectively) to parasite load. Total IgG antibodies to EBA-175 showed a negative correlation to parasite load (r = −0.144), which was not significant (p = 0.276). Duration of stay in Bolifamba also negatively correlated with parasite load (p = 0.026, r = −0.419) and total IgG to PF4-143 was significantly associated with prolonged duration of stay in the locality of Bolifamba, Cameroon (p = 0.006, r = 0.361). CONCLUSIONS: The present study has identified two genes PF3D7_1233400 and PF3D7_1437500 containing peptide fragment (PF4-123 and PF4-143) with B-cell epitopes that are correlated with naturally acquired immunity to malaria. A pipeline has been developed for rapid identification of other B-cell epitopes involved in naturally acquired immunity. BioMed Central 2016-05-20 /pmc/articles/PMC4875671/ /pubmed/27207101 http://dx.doi.org/10.1186/s12936-016-1337-z Text en © The Author(s). 2016 Open AccessThis article is distributed under the terms of the Creative Commons Attribution 4.0 International License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, distribution, and reproduction in any medium, provided you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated.
spellingShingle Research
Nyasa, Raymond B.
Kimbi, Helen K.
Zofou, Denis
DeBarry, Jeremy D.
Kissinger, Jessica C.
Titanji, Vincent P. K.
An evolutionary approach to identify potentially protective B cell epitopes involved in naturally acquired immunity to malaria and the role of EBA-175 in protection amongst denizens of Bolifamba, Cameroon
title An evolutionary approach to identify potentially protective B cell epitopes involved in naturally acquired immunity to malaria and the role of EBA-175 in protection amongst denizens of Bolifamba, Cameroon
title_full An evolutionary approach to identify potentially protective B cell epitopes involved in naturally acquired immunity to malaria and the role of EBA-175 in protection amongst denizens of Bolifamba, Cameroon
title_fullStr An evolutionary approach to identify potentially protective B cell epitopes involved in naturally acquired immunity to malaria and the role of EBA-175 in protection amongst denizens of Bolifamba, Cameroon
title_full_unstemmed An evolutionary approach to identify potentially protective B cell epitopes involved in naturally acquired immunity to malaria and the role of EBA-175 in protection amongst denizens of Bolifamba, Cameroon
title_short An evolutionary approach to identify potentially protective B cell epitopes involved in naturally acquired immunity to malaria and the role of EBA-175 in protection amongst denizens of Bolifamba, Cameroon
title_sort evolutionary approach to identify potentially protective b cell epitopes involved in naturally acquired immunity to malaria and the role of eba-175 in protection amongst denizens of bolifamba, cameroon
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4875671/
https://www.ncbi.nlm.nih.gov/pubmed/27207101
http://dx.doi.org/10.1186/s12936-016-1337-z
work_keys_str_mv AT nyasaraymondb anevolutionaryapproachtoidentifypotentiallyprotectivebcellepitopesinvolvedinnaturallyacquiredimmunitytomalariaandtheroleofeba175inprotectionamongstdenizensofbolifambacameroon
AT kimbihelenk anevolutionaryapproachtoidentifypotentiallyprotectivebcellepitopesinvolvedinnaturallyacquiredimmunitytomalariaandtheroleofeba175inprotectionamongstdenizensofbolifambacameroon
AT zofoudenis anevolutionaryapproachtoidentifypotentiallyprotectivebcellepitopesinvolvedinnaturallyacquiredimmunitytomalariaandtheroleofeba175inprotectionamongstdenizensofbolifambacameroon
AT debarryjeremyd anevolutionaryapproachtoidentifypotentiallyprotectivebcellepitopesinvolvedinnaturallyacquiredimmunitytomalariaandtheroleofeba175inprotectionamongstdenizensofbolifambacameroon
AT kissingerjessicac anevolutionaryapproachtoidentifypotentiallyprotectivebcellepitopesinvolvedinnaturallyacquiredimmunitytomalariaandtheroleofeba175inprotectionamongstdenizensofbolifambacameroon
AT titanjivincentpk anevolutionaryapproachtoidentifypotentiallyprotectivebcellepitopesinvolvedinnaturallyacquiredimmunitytomalariaandtheroleofeba175inprotectionamongstdenizensofbolifambacameroon
AT nyasaraymondb evolutionaryapproachtoidentifypotentiallyprotectivebcellepitopesinvolvedinnaturallyacquiredimmunitytomalariaandtheroleofeba175inprotectionamongstdenizensofbolifambacameroon
AT kimbihelenk evolutionaryapproachtoidentifypotentiallyprotectivebcellepitopesinvolvedinnaturallyacquiredimmunitytomalariaandtheroleofeba175inprotectionamongstdenizensofbolifambacameroon
AT zofoudenis evolutionaryapproachtoidentifypotentiallyprotectivebcellepitopesinvolvedinnaturallyacquiredimmunitytomalariaandtheroleofeba175inprotectionamongstdenizensofbolifambacameroon
AT debarryjeremyd evolutionaryapproachtoidentifypotentiallyprotectivebcellepitopesinvolvedinnaturallyacquiredimmunitytomalariaandtheroleofeba175inprotectionamongstdenizensofbolifambacameroon
AT kissingerjessicac evolutionaryapproachtoidentifypotentiallyprotectivebcellepitopesinvolvedinnaturallyacquiredimmunitytomalariaandtheroleofeba175inprotectionamongstdenizensofbolifambacameroon
AT titanjivincentpk evolutionaryapproachtoidentifypotentiallyprotectivebcellepitopesinvolvedinnaturallyacquiredimmunitytomalariaandtheroleofeba175inprotectionamongstdenizensofbolifambacameroon

Ejemplares similares