2004
DOI: 10.2174/1570180043485545
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Recombinant Murine Polyoma Virus-like-particles Induce Protective Antitumour Immunity

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Cited by 6 publications
(9 citation statements)
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“…From an immunological point of view, we present here a device which is very suitable for the in vivo delivery of fulllength proteins like tumor antigens, because heterologous polyoma capsoids displaying a CD8 T cell epitope were already able to protect inbred mice from lethal challenge with melanoma cells that express this relevant protein antigen (36). For this reason, these capsoid-based immunotherapeutics may offer new opportunities for the treatment of cancer patients.…”
Section: Discussionmentioning
confidence: 99%
“…From an immunological point of view, we present here a device which is very suitable for the in vivo delivery of fulllength proteins like tumor antigens, because heterologous polyoma capsoids displaying a CD8 T cell epitope were already able to protect inbred mice from lethal challenge with melanoma cells that express this relevant protein antigen (36). For this reason, these capsoid-based immunotherapeutics may offer new opportunities for the treatment of cancer patients.…”
Section: Discussionmentioning
confidence: 99%
“…Due to the high immunogenicity of heterologous PLPs consisting of the major polyomavirus coat protein VP1 and a foreign CD8 T cell epitope at its C-terminus it is possible to protect mice against B16-OVA melanoma [2]. Here we show that in mice protective anti-tumour immunity can be already induced by means of subcutaneous vaccination with particulate antigens, heterologous VP1-pentamers (8-9 nm in size).…”
mentioning
confidence: 77%
“…In this regard virus-like particles (VLPs) receive growing attention due to their capacity to elicit cell-mediated immunity with emphasis on CD8 T cell responses in the absence of immunostimulatory substances [3,11,17,19,22]. Therefore, we are currently developing a non-replicating antigen delivery system based on heterologous polyomaviruslike particles (PLPs) formed (i) by self-assembly of the viral VP1 coat protein displaying foreign T cell epitopes at its C-terminal end [5,6] or (ii) by the encapsulation of full-length proteins into the VP1-capsoid shell [1]. We have already analysed the capacity of chimeric PLPs to prime in vivo CD8 T cell responses [5,6].…”
Section: Introductionmentioning
confidence: 99%
“…Therefore, we are currently developing a non-replicating antigen delivery system based on heterologous polyomaviruslike particles (PLPs) formed (i) by self-assembly of the viral VP1 coat protein displaying foreign T cell epitopes at its C-terminal end [5,6] or (ii) by the encapsulation of full-length proteins into the VP1-capsoid shell [1]. We have already analysed the capacity of chimeric PLPs to prime in vivo CD8 T cell responses [5,6]. For this purpose, a protein fragment harbouring the immunodominant CD8 cytotoxic T lymphocyte epitope, residues 257-264 of ovalbumin (OVA), was genetically engineered to the C-terminal end of the VP1 protein resulting in the VP1-OVA 252-270 entity [5,6].…”
Section: Introductionmentioning
confidence: 99%
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