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Leishmania major: Protective capacity of DNA vaccine using amastin fused to HSV-1 VP22 and EGFP in BALB/c mice model |
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| Authors: | Bolhassani Azam Gholami Elham Zahedifard Farnaz Moradin Neda Parsi Parto Doustdari Fatemeh Seyed Negar Papadopoulou Barbara Rafati Sima |
| Affiliation: | aMolecular Immunology and Vaccine Research Laboratory, Pasteur Institute of Iran, 69 Pasteur Ave., Tehran 13164, Iran;bKhatam University, Tehran, Iran;cResearch Centre in Infectious Diseases, CHUL Research Centre and Department of Medical Biology, Faculty of Medicine, Laval University, 2705 Laurier Blvd., Quebec (QC), Canada G1V 4G2 |
| Abstract: | An intercellular spreading strategy using herpes simplex virus type 1 (HSV-1) VP22 protein is employed to enhance DNA vaccine potency of Leishmania major amastin antigen in BALB/c mice model. We evaluated the immunogenicity and protective efficacy of plasmid DNA vaccines encoding amastin-enhanced green fluorescent protein (EGFP) and VP22-amastin-EGFP. Optimal cell-mediated immune responses were observed in BALB/c mice immunized with VP22-amastin-EGFP as assessed by cytokine gene expression analysis using real time RT-PCR. Vaccination with the VP22-amastin-EGFP fusion construct elicited significantly higher IFN-gamma response upon antigen stimulation of splenocytes from immunized mice compared to amastin as a sole antigen. Mice immunized by VP22-amastin-EGFP showed partial protection following infectious challenge with L. major, as measured by parasite load in spleens. These results suggest that the development of DNA vaccines encoding VP22 fused to a target Leishmania antigen would be a promising strategy to improve immunogenicity and DNA vaccine potency. |
| Keywords: | DNA vaccination Leishmania Amastin Cutaneous leishmaniasis Herpes simplex virus type1 VP22 (HSV-1 VP22) Green fluorescent protein (GFP) |
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