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Infection and Immunity, October 2004, p. 5775-5782, Vol. 72, No. 10
0019-9567/04/$08.00+0     DOI: 10.1128/IAI.72.10.5775-5782.2004
Copyright © 2004, American Society for Microbiology. All Rights Reserved.

Comparison of Immunogenicities of Recombinant Plasmodium vivax Merozoite Surface Protein 1 19- and 42-Kilodalton Fragments Expressed in Escherichia coli

Suraksha Sachdeva, Gul Ahmad, Pawan Malhotra, Paushali Mukherjee, and V. S. Chauhan^*

International Centre for Genetic Engineering and Biotechnology, New Delhi, India

Received 1 September 2003/ Returned for modification 21 December 2003/ Accepted 14 July 2004

The 42- and 19-kDa C-terminal fragments of merozoite surface protein 1 (MSP-1₄₂ and MSP-1₁₉, respectively) are both promising blood-stage vaccine candidate antigens. At present, it is not clear which of the two antigens will be more suitable for inclusion in a cocktail malaria vaccine. In the present study, we expressed the two C-terminal fragments of Plasmodium vivax MSP-1 (PvMSP-1) in an Escherichia coli expression system and purified them by using a rapid two-step protocol. Both of the products were recognized by monoclonal antibodies against PvMSP-1 as well as by immune sera from several individuals exposed to P. vivax. We analyzed and compared the immunological responses to recombinant PvMSP-1₁₉ and PvMSP-1₄₂ in mice by using six different adjuvant formulations. Moderate to high antibody responses were observed with both of the antigens in different adjuvant formulations. Surprisingly, alum, which is generally considered to be a poor adjuvant for recombinant malaria antigens, was found to be as good an adjuvant as Montanide ISA 720, ASO2A, and other adjuvant formulations. Most adjuvant formulations induced high levels of immunoglobulin G1 (IgG1), followed by IgG3 and IgG2. Lymphocytes from animals in the PvMSP-1₄₂- and PvMSP-1₁₉-immunized groups showed proliferative responses upon stimulation with the respective antigens, and high levels of interleukin-4 (IL-4), IL-5, and gamma interferon were detected in the culture supernatants. Immunodepletion studies with sera from mice immunized with these two antigens showed that while immunization with PvMSP-1₄₂ does produce a PvMSP-1₁₉-specific response, a substantial portion is also focused on structures in PvMSP-1₄₂ not represented by the epidermal growth factor-like domains of PvMSP-1₁₉. These findings may have implications for the design of MSP-1-based vaccine constructs.

Editor: J. F. Urban, Jr.

S.S. and G.A. contributed equally to this work.

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