Leishmania major: immune response in BALB/c mice immunized with stress-inducible protein 1 encapsulated in liposomes |
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Authors: | Badiee Ali Jaafari Mahmoud R Khamesipour Ali |
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Affiliation: | School of Pharmacy, Biotechnology Research Center and Pharmaceutical Research Center, Mashhad University of Medical Sciences, P.O. Box 91775-1365, Mashhad, Iran. |
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Abstract: | Protection against leishmaniasis is depending upon generation of a Th1 type of immune response. Field trials of first generation Leishmania vaccine showed a limited efficacy even with multiple doses mainly due to lack of an appropriate adjuvant. In this study, susceptible BALB/c mice were immunized with rLmSTI1 encapsulated in liposomes to explore the extent of protection induced by Leishmania antigen encapsulated in the liposomes against challenge with Leishmania major. The results showed that s.c. immunization of BALB/c mice with liposomal rLmSTI1 induced a significant protection against challenge and a significant lower parasite burden in spleen up to 14 weeks after challenge. The protected animals showed a significantly smaller footpad thickness after challenge, and a higher level of anti-SLA IgG antibodies before and after challenge with a predominant IgG2a titer. The data supports the possibility of using liposomal Leishmania antigens as a vaccine. |
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Keywords: | Leishmaniasis Leishmania major Liposome LmSTI1 Adjuvant CMI Vaccine CMI, cell-mediated immunity LmSTI1, Leishmania major stress-inducible protein 1 rLmSTI1, recombinant LmSTI1 SLA, soluble Leishmania antigen Th1, T helper 1 Th2, T helper 2 rTSA, recombinant thiol-specific antioxidant LeIF, Leishmania elongation initiation factor MWt, molecular weight MPL, monophosphoryl lipid A MPL-SE, MPL with squalene CL, cutaneous leishmaniasis HI, humoral immune response APCs, antigen presenting cells DRV, dehydration-rehydration vesicle MLV, multilamellar vesicles SUV, small unilamellar vesicles SDS, sodium dodecyl sulfate SC, subcutaneously ELISA, enzyme-linked immunosorbent assays BSA, bovine serum albumin DC, dendritic cell MÔ, macrophage Ag, antigen IL-4, interleukin-4 IFN-γ, interferon gamma MHC major histocompatibility complex |
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