Analysis of antibody profiles in symptomatic malaria in three sentinel sites of Ivory Coast by using multiplex, fluorescent, magnetic, bead-based serological assay (MAGPIX™)

BACKGROUND: Advances in malaria control have reduced the burden of disease resulting from exposure to parasite infections. The consequences on naturally acquired immunity are unclear. A magnetic bead-based immunoassay (MBA) to assess antibody levels in populations living in endemic areas was previou...

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Autores principales: Koffi, David, Touré, André Offianan, Varela, Marie-Louise, Vigan-Womas, Inès, Béourou, Sylvain, Brou, Somela, Ehouman, Marie-France, Gnamien, Laeticia, Richard, Vincent, Djaman, Joseph Allico, Perraut, Ronald
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2015
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4687342/
https://www.ncbi.nlm.nih.gov/pubmed/26692284
http://dx.doi.org/10.1186/s12936-015-1043-2
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author Koffi, David
Touré, André Offianan
Varela, Marie-Louise
Vigan-Womas, Inès
Béourou, Sylvain
Brou, Somela
Ehouman, Marie-France
Gnamien, Laeticia
Richard, Vincent
Djaman, Joseph Allico
Perraut, Ronald
author_facet Koffi, David
Touré, André Offianan
Varela, Marie-Louise
Vigan-Womas, Inès
Béourou, Sylvain
Brou, Somela
Ehouman, Marie-France
Gnamien, Laeticia
Richard, Vincent
Djaman, Joseph Allico
Perraut, Ronald
author_sort Koffi, David
collection PubMed
description BACKGROUND: Advances in malaria control have reduced the burden of disease resulting from exposure to parasite infections. The consequences on naturally acquired immunity are unclear. A magnetic bead-based immunoassay (MBA) to assess antibody levels in populations living in endemic areas was previously evaluated. In this study, the effect of clinical attacks on immunity was analysed in three sentinel sites of Ivory Coast. METHODS: Recombinant proteins or peptides derived from liver or blood stage antigens of Plasmodiumfalciparum (CSP, LSA1(41), LSA3, SALSA, PF13-DBL1α(1), GLURP, AMA1, MSP1p19, MSP4p20), the CSP of Plasmodium malariae and the salivary glands antigen of Anopheles gambiae (gSG6) were covalently linked to a colour-coded microsphere (Luminex™ beads) for the multiplex assay. ELISA was used for whole parasite extract antigen. Blood samples (n = 94) of patients consulting for symptomatic malaria attacks and living in three different malaria endemic settings (rural and periurban) were analysed. RESULTS: Highly variable seroprevalence of antibody responses against parasite antigens was found ranging from 3 (gSG6) to 97 % (MSP4p20). A marked prevalence and significantly higher level of antibodies was found in patients from the rural site (Korhogo), those harbouring the lowest level of parasitaemia. The use of whole schizont extract could not discriminate immunity level, contrary to parasite-derived recombinant proteins or peptides. Prevalence of responders to LSA1(41) and levels of antibodies to PF13 were significantly different between the three settings. Moreover, the post-treatment clearance of parasites was clearly associated with a significantly higher level of antibody response for almost 50 % of the parasite antigens tested. CONCLUSION: The multiplex MBA-Magpix technology assay provides an accurate high throughput monitoring of parasite-specific antibodies during symptomatic malaria. The levels of antibody responses may provide a risk criterion with respect to the degree of parasitic infection. Additionally, they can be used as an indicator in the implementation of malaria prevention and local control strategies.
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spelling pubmed-46873422015-12-23 Analysis of antibody profiles in symptomatic malaria in three sentinel sites of Ivory Coast by using multiplex, fluorescent, magnetic, bead-based serological assay (MAGPIX™) Koffi, David Touré, André Offianan Varela, Marie-Louise Vigan-Womas, Inès Béourou, Sylvain Brou, Somela Ehouman, Marie-France Gnamien, Laeticia Richard, Vincent Djaman, Joseph Allico Perraut, Ronald Malar J Research BACKGROUND: Advances in malaria control have reduced the burden of disease resulting from exposure to parasite infections. The consequences on naturally acquired immunity are unclear. A magnetic bead-based immunoassay (MBA) to assess antibody levels in populations living in endemic areas was previously evaluated. In this study, the effect of clinical attacks on immunity was analysed in three sentinel sites of Ivory Coast. METHODS: Recombinant proteins or peptides derived from liver or blood stage antigens of Plasmodiumfalciparum (CSP, LSA1(41), LSA3, SALSA, PF13-DBL1α(1), GLURP, AMA1, MSP1p19, MSP4p20), the CSP of Plasmodium malariae and the salivary glands antigen of Anopheles gambiae (gSG6) were covalently linked to a colour-coded microsphere (Luminex™ beads) for the multiplex assay. ELISA was used for whole parasite extract antigen. Blood samples (n = 94) of patients consulting for symptomatic malaria attacks and living in three different malaria endemic settings (rural and periurban) were analysed. RESULTS: Highly variable seroprevalence of antibody responses against parasite antigens was found ranging from 3 (gSG6) to 97 % (MSP4p20). A marked prevalence and significantly higher level of antibodies was found in patients from the rural site (Korhogo), those harbouring the lowest level of parasitaemia. The use of whole schizont extract could not discriminate immunity level, contrary to parasite-derived recombinant proteins or peptides. Prevalence of responders to LSA1(41) and levels of antibodies to PF13 were significantly different between the three settings. Moreover, the post-treatment clearance of parasites was clearly associated with a significantly higher level of antibody response for almost 50 % of the parasite antigens tested. CONCLUSION: The multiplex MBA-Magpix technology assay provides an accurate high throughput monitoring of parasite-specific antibodies during symptomatic malaria. The levels of antibody responses may provide a risk criterion with respect to the degree of parasitic infection. Additionally, they can be used as an indicator in the implementation of malaria prevention and local control strategies. BioMed Central 2015-12-21 /pmc/articles/PMC4687342/ /pubmed/26692284 http://dx.doi.org/10.1186/s12936-015-1043-2 Text en © Koffi et al. 2015 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
Koffi, David
Touré, André Offianan
Varela, Marie-Louise
Vigan-Womas, Inès
Béourou, Sylvain
Brou, Somela
Ehouman, Marie-France
Gnamien, Laeticia
Richard, Vincent
Djaman, Joseph Allico
Perraut, Ronald
Analysis of antibody profiles in symptomatic malaria in three sentinel sites of Ivory Coast by using multiplex, fluorescent, magnetic, bead-based serological assay (MAGPIX™)
title Analysis of antibody profiles in symptomatic malaria in three sentinel sites of Ivory Coast by using multiplex, fluorescent, magnetic, bead-based serological assay (MAGPIX™)
title_full Analysis of antibody profiles in symptomatic malaria in three sentinel sites of Ivory Coast by using multiplex, fluorescent, magnetic, bead-based serological assay (MAGPIX™)
title_fullStr Analysis of antibody profiles in symptomatic malaria in three sentinel sites of Ivory Coast by using multiplex, fluorescent, magnetic, bead-based serological assay (MAGPIX™)
title_full_unstemmed Analysis of antibody profiles in symptomatic malaria in three sentinel sites of Ivory Coast by using multiplex, fluorescent, magnetic, bead-based serological assay (MAGPIX™)
title_short Analysis of antibody profiles in symptomatic malaria in three sentinel sites of Ivory Coast by using multiplex, fluorescent, magnetic, bead-based serological assay (MAGPIX™)
title_sort analysis of antibody profiles in symptomatic malaria in three sentinel sites of ivory coast by using multiplex, fluorescent, magnetic, bead-based serological assay (magpix™)
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4687342/
https://www.ncbi.nlm.nih.gov/pubmed/26692284
http://dx.doi.org/10.1186/s12936-015-1043-2
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