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Please use this identifier to cite or link to this item: http://hdl.handle.net/11154/2335

Title: Brucella spp. lumazine synthase: a novel adjuvant and antigen delivery system to effectively induce oral immunity
Authors: Rosas, G
Fragoso, G
Ainciart, N
Esquivel-Guadarrama, F
Santana, A
Bobes, RJ
Ramirez-Pliego, O
Toledo, A
Cruz-Revilla, C
Meneses, G
Berguer, P
Goldbaum, FA
Sciutto, E
Issue Date: 2006
Abstract: Brucella lumazine synthase (BLS) has been previously used with success as a delivery system for systemic immunization against murine cysticercosis. We herein determined the usefulness of BLS as a new antigen-delivery system and mucosal-adjuvant using KETc1, one of the peptides of the anti-cysticercosis vaccine. A protection of up to 98% was induced when KETc1 was used as a chimera fused to BLS. Used as adjuvant of KETc1, BLS also induced a high level of protection (79%), which did not significantly differ from that induced by the cholera toxin (74%). KETc1 and BLS administered separately also reduced the parasite load. KETc1 administered orally as a chimera, and to a lesser extent with BLS as adjuvant, elicited IgG and IgA specific antibodies, which were detectable both in fecal extracts and in sera, and increased B and CD4 activated cells. BLS-KETc1 also increased the levels of transcription of TNF-alpha, IL-2 and IFN gamma in Peyer's patches, and in spleen, only increased TNF-alpha was observed. Overall, these results showed that BLS can be used as both an antigen-carrier and as an adjuvant in the design of new oral subunit vaccines. (c) 2006 Elsevier SAS. All rights reserved.
URI: http://hdl.handle.net/11154/2335
ISSN: 1286-4579
Appears in Collections:Ciencias

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