Several domains from VAR2CSA can induce Plasmodium falciparum adhesion-blocking antibodies

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Several domains from VAR2CSA can induce Plasmodium falciparum adhesion-blocking antibodies. / Salanti, Ali; Resende, Mafalda; Ditlev, Sisse B; Pinto, Vera V; Dahlbäck, Madeleine; Andersen, Gorm; Manczak, Tom; Theander, Thor G; Nielsen, Morten A.

In: Malaria Journal, Vol. 9, No. 1, 2010, p. 11.

Research output: Contribution to journalJournal articleResearchpeer-review

Harvard

Salanti, A, Resende, M, Ditlev, SB, Pinto, VV, Dahlbäck, M, Andersen, G, Manczak, T, Theander, TG & Nielsen, MA 2010, 'Several domains from VAR2CSA can induce Plasmodium falciparum adhesion-blocking antibodies', Malaria Journal, vol. 9, no. 1, pp. 11. https://doi.org/10.1186/1475-2875-9-11

APA

Salanti, A., Resende, M., Ditlev, S. B., Pinto, V. V., Dahlbäck, M., Andersen, G., Manczak, T., Theander, T. G., & Nielsen, M. A. (2010). Several domains from VAR2CSA can induce Plasmodium falciparum adhesion-blocking antibodies. Malaria Journal, 9(1), 11. https://doi.org/10.1186/1475-2875-9-11

Vancouver

Salanti A, Resende M, Ditlev SB, Pinto VV, Dahlbäck M, Andersen G et al. Several domains from VAR2CSA can induce Plasmodium falciparum adhesion-blocking antibodies. Malaria Journal. 2010;9(1):11. https://doi.org/10.1186/1475-2875-9-11

Author

Salanti, Ali ; Resende, Mafalda ; Ditlev, Sisse B ; Pinto, Vera V ; Dahlbäck, Madeleine ; Andersen, Gorm ; Manczak, Tom ; Theander, Thor G ; Nielsen, Morten A. / Several domains from VAR2CSA can induce Plasmodium falciparum adhesion-blocking antibodies. In: Malaria Journal. 2010 ; Vol. 9, No. 1. pp. 11.

Bibtex

@article{412b738001d611df825d000ea68e967b,
title = "Several domains from VAR2CSA can induce Plasmodium falciparum adhesion-blocking antibodies",
abstract = "ABSTRACT: BACKGROUND: Malaria caused by Plasmodium falciparum can result in several different syndromes with severe clinical consequences for the about 200 million individuals infected each year. During pregnancy, women living in endemic areas become susceptible to malaria due to lack of antibodies against a unique P. falciparum membrane protein, named VAR2CSA. This antigen is not expressed in childhood infections, since it binds chondroitin sulphate A (CSA) expressed on the intervillous space in the placenta. A vaccine appears possible because women acquire protective antibodies hindering sequestration in the placenta as a function of parity. A challenge for vaccine development is to design small constructs of this large antigen, which can induce broadly protective antibodies. It has previously been shown that one domain of VAR2CSA, DBL4-FCR3, induces parasite adhesion-blocking antibodies. In this study, it is demonstrated that other domains of VAR2CSA also can induce antibodies with inhibitory activity. METHODS: All VAR2CSA domains from the 3D7 and HB3 parasites were produced in Baculovirus-transfected insect cells. Groups of three rats per protein were immunized and anti-sera were tested for surface reactivity against infected erythrocytes expressing FCR3 VAR2CSA and for the ability to inhibit FCR3CSA parasite adhesion to CSA. The fine specificity of the immune sera was analysed by VAR2CSA peptide arrays. RESULTS: Inhibitory antibodies were induced by immunization with DBL3-HB3 T1 and DBL1-3D7. However, unlike the previously characterised DBL4-FCR3 response the inhibitory response against DBL1-3D7 and DBL3-HB3 T1 was poorly reproduced in the second rounds of immunizations. CONCLUSION: It is possible to induce parasite adhesion-blocking antibodies when immunizing with a number of different VAR2CSA domains. This indicates that the CSA binding site in VAR2CSA is comprised of epitopes from different domains.",
author = "Ali Salanti and Mafalda Resende and Ditlev, {Sisse B} and Pinto, {Vera V} and Madeleine Dahlb{\"a}ck and Gorm Andersen and Tom Manczak and Theander, {Thor G} and Nielsen, {Morten A}",
year = "2010",
doi = "10.1186/1475-2875-9-11",
language = "English",
volume = "9",
pages = "11",
journal = "Malaria Journal",
issn = "1475-2875",
publisher = "BioMed Central",
number = "1",

}

RIS

TY - JOUR

T1 - Several domains from VAR2CSA can induce Plasmodium falciparum adhesion-blocking antibodies

AU - Salanti, Ali

AU - Resende, Mafalda

AU - Ditlev, Sisse B

AU - Pinto, Vera V

AU - Dahlbäck, Madeleine

AU - Andersen, Gorm

AU - Manczak, Tom

AU - Theander, Thor G

AU - Nielsen, Morten A

PY - 2010

Y1 - 2010

N2 - ABSTRACT: BACKGROUND: Malaria caused by Plasmodium falciparum can result in several different syndromes with severe clinical consequences for the about 200 million individuals infected each year. During pregnancy, women living in endemic areas become susceptible to malaria due to lack of antibodies against a unique P. falciparum membrane protein, named VAR2CSA. This antigen is not expressed in childhood infections, since it binds chondroitin sulphate A (CSA) expressed on the intervillous space in the placenta. A vaccine appears possible because women acquire protective antibodies hindering sequestration in the placenta as a function of parity. A challenge for vaccine development is to design small constructs of this large antigen, which can induce broadly protective antibodies. It has previously been shown that one domain of VAR2CSA, DBL4-FCR3, induces parasite adhesion-blocking antibodies. In this study, it is demonstrated that other domains of VAR2CSA also can induce antibodies with inhibitory activity. METHODS: All VAR2CSA domains from the 3D7 and HB3 parasites were produced in Baculovirus-transfected insect cells. Groups of three rats per protein were immunized and anti-sera were tested for surface reactivity against infected erythrocytes expressing FCR3 VAR2CSA and for the ability to inhibit FCR3CSA parasite adhesion to CSA. The fine specificity of the immune sera was analysed by VAR2CSA peptide arrays. RESULTS: Inhibitory antibodies were induced by immunization with DBL3-HB3 T1 and DBL1-3D7. However, unlike the previously characterised DBL4-FCR3 response the inhibitory response against DBL1-3D7 and DBL3-HB3 T1 was poorly reproduced in the second rounds of immunizations. CONCLUSION: It is possible to induce parasite adhesion-blocking antibodies when immunizing with a number of different VAR2CSA domains. This indicates that the CSA binding site in VAR2CSA is comprised of epitopes from different domains.

AB - ABSTRACT: BACKGROUND: Malaria caused by Plasmodium falciparum can result in several different syndromes with severe clinical consequences for the about 200 million individuals infected each year. During pregnancy, women living in endemic areas become susceptible to malaria due to lack of antibodies against a unique P. falciparum membrane protein, named VAR2CSA. This antigen is not expressed in childhood infections, since it binds chondroitin sulphate A (CSA) expressed on the intervillous space in the placenta. A vaccine appears possible because women acquire protective antibodies hindering sequestration in the placenta as a function of parity. A challenge for vaccine development is to design small constructs of this large antigen, which can induce broadly protective antibodies. It has previously been shown that one domain of VAR2CSA, DBL4-FCR3, induces parasite adhesion-blocking antibodies. In this study, it is demonstrated that other domains of VAR2CSA also can induce antibodies with inhibitory activity. METHODS: All VAR2CSA domains from the 3D7 and HB3 parasites were produced in Baculovirus-transfected insect cells. Groups of three rats per protein were immunized and anti-sera were tested for surface reactivity against infected erythrocytes expressing FCR3 VAR2CSA and for the ability to inhibit FCR3CSA parasite adhesion to CSA. The fine specificity of the immune sera was analysed by VAR2CSA peptide arrays. RESULTS: Inhibitory antibodies were induced by immunization with DBL3-HB3 T1 and DBL1-3D7. However, unlike the previously characterised DBL4-FCR3 response the inhibitory response against DBL1-3D7 and DBL3-HB3 T1 was poorly reproduced in the second rounds of immunizations. CONCLUSION: It is possible to induce parasite adhesion-blocking antibodies when immunizing with a number of different VAR2CSA domains. This indicates that the CSA binding site in VAR2CSA is comprised of epitopes from different domains.

U2 - 10.1186/1475-2875-9-11

DO - 10.1186/1475-2875-9-11

M3 - Journal article

C2 - 20064234

VL - 9

SP - 11

JO - Malaria Journal

JF - Malaria Journal

SN - 1475-2875

IS - 1

ER -

ID: 17007567