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A Multistage Formulation Based on Full-Length CSP and AMA-1 Ectodomain of Plasmodium vivax Induces High Antibody Titers and T-cells and Partially Protects Mice Challenged with a Transgenic Plasmodium berghei Parasite

Infections with Plasmodium vivax are predominant in the Americas, representing 75% of malaria cases. Previously perceived as benign, malaria vivax is, in fact, a highly debilitating and economically important disease. Considering the high complexity of the malaria parasite life cycle, it has been hy...

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Autores principales: Lima, Luciana C., Marques, Rodolfo F., Gimenez, Alba Marina, Françoso, Katia S., Aliprandini, Eduardo, Camargo, Tarsila M., Aguiar, Anna Caroline C., Pereira, Dhelio B., Renia, Laurent, Amino, Rogerio, Soares, Irene S.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2020
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7356588/
https://www.ncbi.nlm.nih.gov/pubmed/32560380
http://dx.doi.org/10.3390/microorganisms8060916
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author Lima, Luciana C.
Marques, Rodolfo F.
Gimenez, Alba Marina
Françoso, Katia S.
Aliprandini, Eduardo
Camargo, Tarsila M.
Aguiar, Anna Caroline C.
Pereira, Dhelio B.
Renia, Laurent
Amino, Rogerio
Soares, Irene S.
author_facet Lima, Luciana C.
Marques, Rodolfo F.
Gimenez, Alba Marina
Françoso, Katia S.
Aliprandini, Eduardo
Camargo, Tarsila M.
Aguiar, Anna Caroline C.
Pereira, Dhelio B.
Renia, Laurent
Amino, Rogerio
Soares, Irene S.
author_sort Lima, Luciana C.
collection PubMed
description Infections with Plasmodium vivax are predominant in the Americas, representing 75% of malaria cases. Previously perceived as benign, malaria vivax is, in fact, a highly debilitating and economically important disease. Considering the high complexity of the malaria parasite life cycle, it has been hypothesized that an effective vaccine formulation against Plasmodium should contain multiple antigens expressed in different parasite stages. Based on that, we analyzed a recombinant P. vivax vaccine formulation mixing the apical membrane antigen 1 ectodomain (PvAMA-1) and a full-length circumsporozoite protein (PvCSP-All(FL)) previously studied by our group, which elicits a potent antibody response in mice. Genetically distinct strains of mice (C57BL/6 and BALB/c) were immunized with the proteins, alone or in combination, in the presence of poly(I:C) adjuvant, a TLR3 agonist. In C57BL/6, high-antibody titers were induced against PvAMA-1 and the three PvCSP variants (VK210, VK247, and P. vivax-like). Meanwhile, mixing PvAMA-1 with PvCSP-All(FL) had no impact on total IgG antibody titers, which were long-lasting. Moreover, antibodies from immunized mice recognized VK210 sporozoites and blood-stage parasites by immunofluorescence assay. However, in the BALB/c model, the antibody response against PvCSP-All(FL) was relatively low. PvAMA-1-specific CD3(+)CD4(+) and CD3(+)CD8(+) T-cell responses were observed in C57BL/6 mice, and the cellular response was impaired by PvCSP-All(FL) combination. More relevant, the multistage vaccine formulation provided partial protection in mice challenged with a transgenic Plasmodium berghei sporozoite expressing the homologous PvCSP protein.
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spelling pubmed-73565882020-07-22 A Multistage Formulation Based on Full-Length CSP and AMA-1 Ectodomain of Plasmodium vivax Induces High Antibody Titers and T-cells and Partially Protects Mice Challenged with a Transgenic Plasmodium berghei Parasite Lima, Luciana C. Marques, Rodolfo F. Gimenez, Alba Marina Françoso, Katia S. Aliprandini, Eduardo Camargo, Tarsila M. Aguiar, Anna Caroline C. Pereira, Dhelio B. Renia, Laurent Amino, Rogerio Soares, Irene S. Microorganisms Article Infections with Plasmodium vivax are predominant in the Americas, representing 75% of malaria cases. Previously perceived as benign, malaria vivax is, in fact, a highly debilitating and economically important disease. Considering the high complexity of the malaria parasite life cycle, it has been hypothesized that an effective vaccine formulation against Plasmodium should contain multiple antigens expressed in different parasite stages. Based on that, we analyzed a recombinant P. vivax vaccine formulation mixing the apical membrane antigen 1 ectodomain (PvAMA-1) and a full-length circumsporozoite protein (PvCSP-All(FL)) previously studied by our group, which elicits a potent antibody response in mice. Genetically distinct strains of mice (C57BL/6 and BALB/c) were immunized with the proteins, alone or in combination, in the presence of poly(I:C) adjuvant, a TLR3 agonist. In C57BL/6, high-antibody titers were induced against PvAMA-1 and the three PvCSP variants (VK210, VK247, and P. vivax-like). Meanwhile, mixing PvAMA-1 with PvCSP-All(FL) had no impact on total IgG antibody titers, which were long-lasting. Moreover, antibodies from immunized mice recognized VK210 sporozoites and blood-stage parasites by immunofluorescence assay. However, in the BALB/c model, the antibody response against PvCSP-All(FL) was relatively low. PvAMA-1-specific CD3(+)CD4(+) and CD3(+)CD8(+) T-cell responses were observed in C57BL/6 mice, and the cellular response was impaired by PvCSP-All(FL) combination. More relevant, the multistage vaccine formulation provided partial protection in mice challenged with a transgenic Plasmodium berghei sporozoite expressing the homologous PvCSP protein. MDPI 2020-06-17 /pmc/articles/PMC7356588/ /pubmed/32560380 http://dx.doi.org/10.3390/microorganisms8060916 Text en © 2020 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Lima, Luciana C.
Marques, Rodolfo F.
Gimenez, Alba Marina
Françoso, Katia S.
Aliprandini, Eduardo
Camargo, Tarsila M.
Aguiar, Anna Caroline C.
Pereira, Dhelio B.
Renia, Laurent
Amino, Rogerio
Soares, Irene S.
A Multistage Formulation Based on Full-Length CSP and AMA-1 Ectodomain of Plasmodium vivax Induces High Antibody Titers and T-cells and Partially Protects Mice Challenged with a Transgenic Plasmodium berghei Parasite
title A Multistage Formulation Based on Full-Length CSP and AMA-1 Ectodomain of Plasmodium vivax Induces High Antibody Titers and T-cells and Partially Protects Mice Challenged with a Transgenic Plasmodium berghei Parasite
title_full A Multistage Formulation Based on Full-Length CSP and AMA-1 Ectodomain of Plasmodium vivax Induces High Antibody Titers and T-cells and Partially Protects Mice Challenged with a Transgenic Plasmodium berghei Parasite
title_fullStr A Multistage Formulation Based on Full-Length CSP and AMA-1 Ectodomain of Plasmodium vivax Induces High Antibody Titers and T-cells and Partially Protects Mice Challenged with a Transgenic Plasmodium berghei Parasite
title_full_unstemmed A Multistage Formulation Based on Full-Length CSP and AMA-1 Ectodomain of Plasmodium vivax Induces High Antibody Titers and T-cells and Partially Protects Mice Challenged with a Transgenic Plasmodium berghei Parasite
title_short A Multistage Formulation Based on Full-Length CSP and AMA-1 Ectodomain of Plasmodium vivax Induces High Antibody Titers and T-cells and Partially Protects Mice Challenged with a Transgenic Plasmodium berghei Parasite
title_sort multistage formulation based on full-length csp and ama-1 ectodomain of plasmodium vivax induces high antibody titers and t-cells and partially protects mice challenged with a transgenic plasmodium berghei parasite
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7356588/
https://www.ncbi.nlm.nih.gov/pubmed/32560380
http://dx.doi.org/10.3390/microorganisms8060916
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