Safety and immunogenicity of novel recombinant BCG and modified vaccinia virus ankara vaccines in neonate rhesus macaques
Safety and immunogenicity of novel recombinant BCG and modified vaccinia virus ankara vaccines in neonate rhesus macaques
Although major inroads into making antiretroviral therapy available in resource-poor countries have been made, there is an urgent need for an effective vaccine administered shortly after birth, which would protect infants from acquiring human immunodeficiency virus type 1 (HIV-1) through breast-feeding. Bacillus Calmette-Guérin (BCG) is given to most infants at birth, and its recombinant form could be used to prime HIV-1-specific responses for a later boost by heterologous vectors delivering the same HIV-1-derived immunogen. Here, two groups of neonate Indian rhesus macaques were immunized with either novel candidate vaccine BCG.HIVA401 or its parental strain AERAS-401, followed by two doses of recombinant modified vaccinia virus Ankara MVA.HIVA. The HIVA immunogen is derived from African clade A HIV-1. All vaccines were safe, giving local reactions consistent with the expected response at the injection site. No systemic adverse events or gross abnormality was seen at necropsy. Both AERAS-401 and BCG.HIVA401 induced high frequencies of BCG-specific IFN-γ-secreting lymphocytes that declined over 23 weeks, but the latter failed to induce detectable HIV-1-specific IFN-γ responses. MVA.HIVA elicited HIV-1-specific IFN-γ responses in all eight animals, but, except for one animal, these responses were weak. The HIV-1-specific responses induced in infants were lower compared to historic data generated by the two HIVA vaccines in adult animals but similar to other recombinant poxviruses tested in this model. This is the first time these vaccines were tested in newborn monkeys. These results inform further infant vaccine development and provide comparative data for two human infant vaccine trials of MVA.HIVA.
7815–7821
Rosario, M.
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Fulkerson, J.
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Soneji, S.
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Parker, J.
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Im, Eung-Jun
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Borthwick, N.
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Bridgeman, A.
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Bourne, C.
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Joseph, J.
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Sadoff, J. C.
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Hanke, T.
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1 August 2010
Rosario, M.
34c69b08-bfac-4547-970b-5d7f3f94bf90
Fulkerson, J.
702c4993-f157-4306-a901-79df0a68852f
Soneji, S.
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Parker, J.
979fbb42-5897-4fbe-a32e-06793f9f99ed
Im, Eung-Jun
adcbe83f-df50-424e-8ff6-d1ffaa25703d
Borthwick, N.
c67c1b51-3749-4892-a634-9e04e2fe3e26
Bridgeman, A.
4c169e86-e119-4740-a1c2-ba8a872a8cee
Bourne, C.
c17aed54-c75b-4e82-957b-81b3279dfa01
Joseph, J.
a761a535-adc8-4e5a-b7c7-e78ad4f245c3
Sadoff, J. C.
9c44b99d-5fa5-4d01-86d2-cc99962f09df
Hanke, T.
8b2d9730-f490-4a67-bfe9-c9e867a6979c
Rosario, M., Fulkerson, J., Soneji, S., Parker, J., Im, Eung-Jun, Borthwick, N., Bridgeman, A., Bourne, C., Joseph, J., Sadoff, J. C. and Hanke, T.
(2010)
Safety and immunogenicity of novel recombinant BCG and modified vaccinia virus ankara vaccines in neonate rhesus macaques.
Journal of Virology, 84 (15), .
(doi:10.1128/jvi.00726-10).
Abstract
Although major inroads into making antiretroviral therapy available in resource-poor countries have been made, there is an urgent need for an effective vaccine administered shortly after birth, which would protect infants from acquiring human immunodeficiency virus type 1 (HIV-1) through breast-feeding. Bacillus Calmette-Guérin (BCG) is given to most infants at birth, and its recombinant form could be used to prime HIV-1-specific responses for a later boost by heterologous vectors delivering the same HIV-1-derived immunogen. Here, two groups of neonate Indian rhesus macaques were immunized with either novel candidate vaccine BCG.HIVA401 or its parental strain AERAS-401, followed by two doses of recombinant modified vaccinia virus Ankara MVA.HIVA. The HIVA immunogen is derived from African clade A HIV-1. All vaccines were safe, giving local reactions consistent with the expected response at the injection site. No systemic adverse events or gross abnormality was seen at necropsy. Both AERAS-401 and BCG.HIVA401 induced high frequencies of BCG-specific IFN-γ-secreting lymphocytes that declined over 23 weeks, but the latter failed to induce detectable HIV-1-specific IFN-γ responses. MVA.HIVA elicited HIV-1-specific IFN-γ responses in all eight animals, but, except for one animal, these responses were weak. The HIV-1-specific responses induced in infants were lower compared to historic data generated by the two HIVA vaccines in adult animals but similar to other recombinant poxviruses tested in this model. This is the first time these vaccines were tested in newborn monkeys. These results inform further infant vaccine development and provide comparative data for two human infant vaccine trials of MVA.HIVA.
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Accepted/In Press date: 12 May 2010
Published date: 1 August 2010
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Local EPrints ID: 480609
URI: http://eprints.soton.ac.uk/id/eprint/480609
ISSN: 0022-538X
PURE UUID: 7842c401-a523-476f-91b6-9150f38bc18c
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Date deposited: 07 Aug 2023 16:51
Last modified: 18 Mar 2024 03:50
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Author:
M. Rosario
Author:
J. Fulkerson
Author:
S. Soneji
Author:
Eung-Jun Im
Author:
N. Borthwick
Author:
A. Bridgeman
Author:
C. Bourne
Author:
J. Joseph
Author:
J. C. Sadoff
Author:
T. Hanke
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