Evaluation of Plasmodium falciparum MSP10 and its development as a serological tool for the Peruvian Amazon region

Abstract Background Different antigens are needed to characterize Plasmodium falciparum infection in terms of seroreactivity and targets for invasion inhibition, in order to guide and identify the proper use of such proteins as tools for the development of serological markers and/or as vaccine candi...

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Main Authors: Jorge Bendezu, Elizabeth Villasis, Sandra Morales Ruiz, Katherine Garro, Berónica Infante, Renzo Gutierrez-Loli, Pamela Rodríguez, Manolo Fernández-Díaz, Dionicia Gamboa, Katherine Torres
Format: Article
Language:English
Published: BMC 2019-09-01
Series:Malaria Journal
Subjects:
Online Access:http://link.springer.com/article/10.1186/s12936-019-2959-8
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spelling doaj-0d549ebaa7bd4cea8377e8b56352dcf12020-11-25T03:54:57ZengBMCMalaria Journal1475-28752019-09-0118111310.1186/s12936-019-2959-8Evaluation of Plasmodium falciparum MSP10 and its development as a serological tool for the Peruvian Amazon regionJorge Bendezu0Elizabeth Villasis1Sandra Morales Ruiz2Katherine Garro3Berónica Infante4Renzo Gutierrez-Loli5Pamela Rodríguez6Manolo Fernández-Díaz7Dionicia Gamboa8Katherine Torres9Laboratorios de Investigación y Desarrollo, FARVETLaboratorios de Investigación y Desarrollo “Abraham Vaisberg Wolach, Facultad de Ciencias y Filosofía, Universidad Peruana Cayetano HerediaLaboratorios de Investigación y Desarrollo, FARVETLaboratorios de Investigación y Desarrollo “Abraham Vaisberg Wolach, Facultad de Ciencias y Filosofía, Universidad Peruana Cayetano HerediaLaboratorios de Investigación y Desarrollo “Abraham Vaisberg Wolach, Facultad de Ciencias y Filosofía, Universidad Peruana Cayetano HerediaLaboratorios de Investigación y Desarrollo “Abraham Vaisberg Wolach, Facultad de Ciencias y Filosofía, Universidad Peruana Cayetano HerediaLaboratorios de Investigación y Desarrollo “Abraham Vaisberg Wolach, Facultad de Ciencias y Filosofía, Universidad Peruana Cayetano HerediaLaboratorios de Investigación y Desarrollo, FARVETLaboratorios de Investigación y Desarrollo “Abraham Vaisberg Wolach, Facultad de Ciencias y Filosofía, Universidad Peruana Cayetano HerediaLaboratorios de Investigación y Desarrollo “Abraham Vaisberg Wolach, Facultad de Ciencias y Filosofía, Universidad Peruana Cayetano HerediaAbstract Background Different antigens are needed to characterize Plasmodium falciparum infection in terms of seroreactivity and targets for invasion inhibition, in order to guide and identify the proper use of such proteins as tools for the development of serological markers and/or as vaccine candidates. Methods IgG responses in 84 serum samples from individuals with P. falciparum infection [classified as symptomatic (Sym) or asymptomatic (Asym)], or acute Plasmodium vivax infection, from the Peruvian Amazon region, were evaluated by enzyme-linked immunosorbent assays specific for a baculovirus-produced recombinant protein P. falciparum Merozoite Surface Protein 10 (rMSP10) and for non-EGF region selected peptides of PfMSP10 selected by a bioinformatics tool (PfMSP10-1, PfMSP10-2 and PfMSP10-3). Monoclonal antibodies against the selected peptides were evaluated by western blotting, confocal microscopy and inhibition invasion assays. Results Seroreactivity analysis of the P. falciparum Sym- and Asym-infected individuals against rMSP10 showed a higher response as compared to the individuals with P. vivax acute infection. IgG responses against peptide PfMSP10-1 were weak. Interestingly high IgG response was found against peptide PfMSP10-2 and the combination of peptides PfMSP10-1 + PfMSP10-2. Monoclonal antibodies were capable of detecting native PfMSP10 on purified schizonts by western blot and confocal microscopy. A low percentage of inhibition of merozoite invasion of erythrocytes in vitro was observed when the monoclonal antibodies were compared with the control antibody against AMA-1 antigen. Further studies are needed to evaluate the role of PfMSP10 in the merozoite invasion. Conclusions The rMSP10 and the PfMSP10-2 peptide synthesized for this study may be useful antigens for evaluation of P. falciparum malaria exposure in Sym and Asym individuals from the Peruvian Amazon region. Moreover, these antigens can be used for further investigation of the role of this protein in other malaria-endemic areas.http://link.springer.com/article/10.1186/s12936-019-2959-8Plasmodium falciparumPfMSP10Monoclonal antibodiesPeptides
collection DOAJ
language English
format Article
sources DOAJ
author Jorge Bendezu
Elizabeth Villasis
Sandra Morales Ruiz
Katherine Garro
Berónica Infante
Renzo Gutierrez-Loli
Pamela Rodríguez
Manolo Fernández-Díaz
Dionicia Gamboa
Katherine Torres
spellingShingle Jorge Bendezu
Elizabeth Villasis
Sandra Morales Ruiz
Katherine Garro
Berónica Infante
Renzo Gutierrez-Loli
Pamela Rodríguez
Manolo Fernández-Díaz
Dionicia Gamboa
Katherine Torres
Evaluation of Plasmodium falciparum MSP10 and its development as a serological tool for the Peruvian Amazon region
Malaria Journal
Plasmodium falciparum
PfMSP10
Monoclonal antibodies
Peptides
author_facet Jorge Bendezu
Elizabeth Villasis
Sandra Morales Ruiz
Katherine Garro
Berónica Infante
Renzo Gutierrez-Loli
Pamela Rodríguez
Manolo Fernández-Díaz
Dionicia Gamboa
Katherine Torres
author_sort Jorge Bendezu
title Evaluation of Plasmodium falciparum MSP10 and its development as a serological tool for the Peruvian Amazon region
title_short Evaluation of Plasmodium falciparum MSP10 and its development as a serological tool for the Peruvian Amazon region
title_full Evaluation of Plasmodium falciparum MSP10 and its development as a serological tool for the Peruvian Amazon region
title_fullStr Evaluation of Plasmodium falciparum MSP10 and its development as a serological tool for the Peruvian Amazon region
title_full_unstemmed Evaluation of Plasmodium falciparum MSP10 and its development as a serological tool for the Peruvian Amazon region
title_sort evaluation of plasmodium falciparum msp10 and its development as a serological tool for the peruvian amazon region
publisher BMC
series Malaria Journal
issn 1475-2875
publishDate 2019-09-01
description Abstract Background Different antigens are needed to characterize Plasmodium falciparum infection in terms of seroreactivity and targets for invasion inhibition, in order to guide and identify the proper use of such proteins as tools for the development of serological markers and/or as vaccine candidates. Methods IgG responses in 84 serum samples from individuals with P. falciparum infection [classified as symptomatic (Sym) or asymptomatic (Asym)], or acute Plasmodium vivax infection, from the Peruvian Amazon region, were evaluated by enzyme-linked immunosorbent assays specific for a baculovirus-produced recombinant protein P. falciparum Merozoite Surface Protein 10 (rMSP10) and for non-EGF region selected peptides of PfMSP10 selected by a bioinformatics tool (PfMSP10-1, PfMSP10-2 and PfMSP10-3). Monoclonal antibodies against the selected peptides were evaluated by western blotting, confocal microscopy and inhibition invasion assays. Results Seroreactivity analysis of the P. falciparum Sym- and Asym-infected individuals against rMSP10 showed a higher response as compared to the individuals with P. vivax acute infection. IgG responses against peptide PfMSP10-1 were weak. Interestingly high IgG response was found against peptide PfMSP10-2 and the combination of peptides PfMSP10-1 + PfMSP10-2. Monoclonal antibodies were capable of detecting native PfMSP10 on purified schizonts by western blot and confocal microscopy. A low percentage of inhibition of merozoite invasion of erythrocytes in vitro was observed when the monoclonal antibodies were compared with the control antibody against AMA-1 antigen. Further studies are needed to evaluate the role of PfMSP10 in the merozoite invasion. Conclusions The rMSP10 and the PfMSP10-2 peptide synthesized for this study may be useful antigens for evaluation of P. falciparum malaria exposure in Sym and Asym individuals from the Peruvian Amazon region. Moreover, these antigens can be used for further investigation of the role of this protein in other malaria-endemic areas.
topic Plasmodium falciparum
PfMSP10
Monoclonal antibodies
Peptides
url http://link.springer.com/article/10.1186/s12936-019-2959-8
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