2006
DOI: 10.1111/j.1600-0463.2006.apm_395.x
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Immune response in rhesus macaques after mixed modality immunisations with DNA, recombinant adenovirus and recombinant gp120 from human immunodeficiency virus type 1

Abstract: The establishment of effective regimens for a vaccine against human immunodeficiency virus type 1 (HIV-1) is urgently needed. In the present study we have produced HIV-1 gp120 from a vaccine-relevant primary R5 isolate in recombinant vaccinia (rVV)-infected Vero cells. We have investigated the effect of boosting with this protein in mixed modality immunisations of rhesus macaques following different immunisation. As reported earlier, animals were primed with codon-optimised HIV-1(BX08)env DNA delivered as plas… Show more

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Cited by 14 publications
(14 citation statements)
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“…High-Ab titers have been reported following heterologous prime-boost regimens using adenovirus-MVA or two adenoviral vectors of heterologous serotype (9,11). We previously reported in mice using vaccines against MSP1 that even higher Ab titers can be achieved by combining vectored vaccines with protein-in-adjuvant vaccines (31), similar to that seen in studies of HIV-1 vaccine candidates (32)(33)(34)(35)(36). The data in this study of two viral-vectored vaccines and protein-in-adjuvant vaccines in rhesus macaques agreed with the previous murine data, demonstrating that moderately high IgG was induced against both alleles of AMA1 by AdCh63-MVA immunization and that even higher titers could be induced by protein-in-adjuvant boosting.…”
Section: Discussionsupporting
confidence: 50%
“…High-Ab titers have been reported following heterologous prime-boost regimens using adenovirus-MVA or two adenoviral vectors of heterologous serotype (9,11). We previously reported in mice using vaccines against MSP1 that even higher Ab titers can be achieved by combining vectored vaccines with protein-in-adjuvant vaccines (31), similar to that seen in studies of HIV-1 vaccine candidates (32)(33)(34)(35)(36). The data in this study of two viral-vectored vaccines and protein-in-adjuvant vaccines in rhesus macaques agreed with the previous murine data, demonstrating that moderately high IgG was induced against both alleles of AMA1 by AdCh63-MVA immunization and that even higher titers could be induced by protein-in-adjuvant boosting.…”
Section: Discussionsupporting
confidence: 50%
“…The genes were synthesised and codon‐optimised for efficient expression in ferrets and humans by GeneArt (Regensburg, Germany) and cloned into a modified pWRG7079 (PowderJect, Middleton, Wisconsin, USA) DNA vaccine vector 12 . H3N2 genes were cloned into a clinical pKCMV standard expression vector kindly provided by Britta Wahren, Karolinska Institute, Sweden 13 .…”
Section: Methodsmentioning
confidence: 99%
“…The genes were synthesised and codon-optimised for efficient expression in ferrets and humans by GeneArt (Regensburg, Germany) and cloned into a modified pWRG7079 (PowderJect, Middleton, Wisconsin, USA) DNA vaccine vector. 12 H3N2 genes were cloned into a clinical pKCMV standard expression vector kindly provided by Britta Wahren, Karolinska Institute, Sweden. 13 Key elements in the expression vectors are the Kozak ribosomal signal sequence, a kanamycin resistance gene, strong constitutive CMV-IE promoter, polyadenylation signals and an intron A sequence in the pWRG7079 vector.…”
Section: Construction Of the Dna Vaccinesmentioning
confidence: 99%
“…The construction of BX08 gp140 (GenBank JX473289) plasmid used codons from highly expressed human genes as described earlier (4648) and two other primary envs from Danish patients (ctl21 (JX473290) and ctl27 (JX473291) (49) were similarly codon optimized and cloned in the same expression plasmid with the key elements CMV IE promotor-enhancer, tPA secretion signal, and a bovine growth hormone poly A signal. Clones were verified by sequencing.…”
Section: Methodsmentioning
confidence: 99%