A heterologous prime‐boost vaccination regimen using ORFF DNA and recombinant ORFF protein confers protective immunity against experimental visceral leishmaniasis

Tewary, Poonam ; Jain, Manju ; Sahani, Mayurbhai H. ; Saxena, Shailendra ; Madhubala, Rentala (2005) A heterologous prime‐boost vaccination regimen using ORFF DNA and recombinant ORFF protein confers protective immunity against experimental visceral leishmaniasis The Journal of Infectious Diseases, 191 (12). pp. 2130-2137. ISSN 0022-1899

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Official URL: http://www.jstor.org/stable/30077877?seq=1#page_sc...

Related URL: http://dx.doi.org/10.1086/430348

Abstract

Objective: We describe the effectiveness of a prime-boost vaccination regimen using the open-reading frame (ORFF) gene from the LD1 locus of Leishmania donovani. Methods: A group of BALE/c mice was immunized with the plasmid carrying the gene for ORFF (F/pcDNA 3.1) and given a booster dose of either the same DNA vaccine or a vaccine with a recombinant ORFF (rORFF) protein. Another group of BALE/c mice was immunized and given a booster dose of the rORFF protein vaccine. The protective efficacies of these vaccine formulations were compared after challenge with L. donovani stationary-phase promastigotes. Results: Mice given the prime-boost vaccination regimen had an enhanced reduction in parasite load (75%-80%), compared with that in mice given only the rORFF protein vaccine (45%-60%). However, the protective response induced in the prime-boost group was not more than that elicited in the DNA vaccine group. Immunization with only the rORFF protein vaccine did not induce the typical T helper response, whereas priming with the DNA vaccine resulted in enhanced production of immunoglobulin G2a and interferon-γ. Furthermore, priming with the DNA vaccine also led to enhanced proliferation of splenocytes, suggesting subsequent expansion of antigen-specific T cells. Conclusions: The heterologous prime-boost vaccination strategy may be utilized for visceral leishmaniasis.

Item Type:Article
Source:Copyright of this article belongs to Oxford University Press.
ID Code:111546
Deposited On:31 Jan 2018 04:04
Last Modified:31 Jan 2018 04:04

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