Merozoite Surface Protein 1 of Plasmodium vivax Induces a Protective Response against Plasmodium cynomolgi Challenge in Rhesus Monkeys

Author:

Dutta Sheetij1,Kaushal Deep C.2,Ware Lisa A.1,Puri Sunil K.3,Kaushal Nuzhat A.3,Narula Atul2,Upadhyaya D. S.4,Lanar David E.1

Affiliation:

1. Department of Immunology, Walter Reed Army Institute of Research, Silver Spring, Maryland 20910

2. Division of Microbiology

3. Division of Parasitology

4. Division of Lab Animals, Central Drug Research Institute, Lucknow 226001, India

Abstract

ABSTRACT The 42-kDa fragment of the merozoite surface protein 1 (MSP-1 42 ) is a leading candidate for the development of a vaccine to control malaria. We previously reported a method for the production of Plasmodium vivax MSP-1 42 (PvMSP-1 42 ) as a soluble protein (S. Dutta, L. W. Ware, A. Barbosa, C. F. Ockenhouse, and D. E. Lanar, Infect. Immun. 69: 5464-5470, 2001). We report here a process to manufacture the same PvMSP-1 42 protein but as an insoluble inclusion body-derived protein which was then refolded in vitro. We compared the immunogenicity and protective efficacy of the soluble and refolded forms of PvMSP-1 42 protein by using a heterologous but closely related P. cynomolgi -rhesus monkey challenge model. As comparative controls we also expressed, purified, and immunized rhesus with the soluble and refolded forms of the P. cynomolgi MSP-1 42 (PcMSP-1 42 ) proteins. All proteins induced equally high-titer, cross-reacting antibodies. Upon challenge with P. cynomolgi , none of the MSP-1 42 -vaccinated groups demonstrated sterile protection or a delay in the prepatent period. However, following an initial rise in parasitemia, all MSP-1-vaccinated animals had significantly lower parasite burdens as indicated by lower cumulative parasitemia, lower peak parasitemia, lower secondary peak parasitemia, and lower average daily parasitemia compared to the adjuvant control group ( P < 0.05). Except the soluble PcMSP-1 42 group, monkeys in all other groups had fewer numbers of days with parasitemia of >10,000 parasites mm −3 . Interestingly, there was no significant difference in the level of partial protection observed in the homologous and heterologous groups in this challenge model. The soluble and refolded forms of PcMSP-1 42 and PvMSP-1 42 proteins also appeared to have a similar partially protective effect.

Publisher

American Society for Microbiology

Subject

Infectious Diseases,Immunology,Microbiology,Parasitology

Reference46 articles.

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4. Ballou, W. R., M. Arevalo-Herrera, D. Carucci, T. L. Richie, G. Corradin, C. L. Diggs, P. Druilhe, B. K. Giersing, A. Saul, D. G. Heppner, K. E. Kester, D. E. Lanar, J. Lyon, A. V. Hill, W. Pan, and J. D. Cohen. 2004. Update on the clinical development of candidate malaria vaccines. Am. J. Trop. Med. Hyg.71(Suppl. 2):239-247.

5. Benjamin, P. A., I. T. Ling, G. Clottey, L. M. Valero, S. A. Ogun, S. L. Fleck, D. Walliker, W. D. Morgan, B. Birdsall, J. Feeney, and A. A. Holder. 1999. Antigenic and sequence diversity at the C-terminus of the merozoite surface protein-1 from rodent malaria isolates, and the binding of protective monoclonal antibodies. Mol. Biochem. Parasitol.104:147-156.

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