We used the simian immunodeficiency virus mac251 (SIVmac251) macaque model to study the effect of the dose of mucosal exposure on vaccine efficacy. We immunized macaques with a DNA prime followed by SIV gp120 protein immunization with ALVAC-SIV and gp120 in alum, and we challenged them with SIVmac251 at either a single high dose or at two repeated low-dose exposures to a 10-fold-lower dose. Infection was neither prevented nor modified following a single high-dose challenge of the immunized macaques. However, two exposures to a 10-fold-lower dose resulted in protection from SIVmac251 acquisition in 3 out of 12 macaques. The remaining animals that were infected had a modulated pathogenesis, significant downregulation of interferon responsive genes, and upregulation of genes involved in B- and T-cell responses. Thus, the choice of the experimental model greatly influences the vaccine efficacy of vaccines for human immunodeficiency virus (HIV).

Protection afforded by an HIV vaccine candidate in macaques depends on the dose of SIVmac251 at challenge exposure / M. Vaccari, B.F. Keele, S.E. Bosinger, M.N. Doster, Z. Ma, J. Pollara, A. Hryniewicz, G. Ferrari, Y. Guan, D.N. Forthal, D. Venzon, C. Fenizia, T. Morgan, D. Montefiori, J.D. Lifson, C.J. Miller, G. Silvestri, M. Rosati, B.K. Felber, G.N. Pavlakis, J. Tartaglia, G. Franchini. - In: JOURNAL OF VIROLOGY. - ISSN 0022-538X. - 87:6(2013), pp. 3538-3548. [10.1128/JVI.02863-12]

Protection afforded by an HIV vaccine candidate in macaques depends on the dose of SIVmac251 at challenge exposure

M. Vaccari
Primo
;
C. Fenizia;
2013

Abstract

We used the simian immunodeficiency virus mac251 (SIVmac251) macaque model to study the effect of the dose of mucosal exposure on vaccine efficacy. We immunized macaques with a DNA prime followed by SIV gp120 protein immunization with ALVAC-SIV and gp120 in alum, and we challenged them with SIVmac251 at either a single high dose or at two repeated low-dose exposures to a 10-fold-lower dose. Infection was neither prevented nor modified following a single high-dose challenge of the immunized macaques. However, two exposures to a 10-fold-lower dose resulted in protection from SIVmac251 acquisition in 3 out of 12 macaques. The remaining animals that were infected had a modulated pathogenesis, significant downregulation of interferon responsive genes, and upregulation of genes involved in B- and T-cell responses. Thus, the choice of the experimental model greatly influences the vaccine efficacy of vaccines for human immunodeficiency virus (HIV).
Animals; Gene Products, env; Macaca; Molecular Sequence Data; SAIDS Vaccines; Sequence Analysis, DNA; Simian Acquired Immunodeficiency Syndrome; Simian Immunodeficiency Virus; Vaccines, DNA; Vaccines, Subunit; Immunology; Virology
Settore MED/04 - Patologia Generale
2013
Article (author)
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/2434/484915
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