Evaluation of immune responses elicited in mice against a recombinant malaria vaccine based on Plasmodium vivax duffy binding protein

Yazdani, Syed Shams ; Shakri, Ahmad Rushdi ; Mukherjee, Paushali ; Baniwal, Sanjeev Kumar ; Chitnis, Chetan E. (2004) Evaluation of immune responses elicited in mice against a recombinant malaria vaccine based on Plasmodium vivax duffy binding protein Vaccine, 22 (27-28). pp. 3727-3737. ISSN 0264-410X

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Official URL: http://linkinghub.elsevier.com/retrieve/pii/S02644...

Related URL: http://dx.doi.org/10.1016/j.vaccine.2004.03.030

Abstract

Plasmodium vivax Duffy binding protein (PvDBP) binds the Duffy blood group antigen as the obligate receptor for erythrocyte invasion. We have tested in mice the immunogenicity of recombinant P. vivax region II (PvRII), the receptor-binding domain of PvDBP, formulated with five adjuvants, namely, Montanide ISA720, AS02A, alum, QS21 and MF59. All the formulations elicited high titer antibodies, with Montanide ISA720 and AS02A yielding the highest titers followed by MF59, QS21 and alum. Sera raised against PvRII formulated with AS02A and Montanide ISA720 followed by alum were most effective at blocking PvRII binding to erythrocytes in a functional assay. Analysis of cellular immune responses indicated that all adjuvant groups induced significant interferon-γ, with alum being the highest interferon-γ inducer. These results suggest that recombinant PvRII formulated with human compatible adjuvants is immunogenic in small animal models and that Montanide ISA720, AS02A and alum perform better than MF59 and QS21 in terms of their ability to elicit high titer binding inhibitory antibodies.

Item Type:Article
Source:Copyright of this article belongs to Elsevier Science.
Keywords:Malaria Vaccines; Blood-stage Malaria Vaccines; Erythrocyte Invasion; Erythrocyte Binding Proteins; Adjuvant Studies
ID Code:5567
Deposited On:19 Oct 2010 11:53
Last Modified:31 May 2011 06:18

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