Journal ArticleDOI
Antigenicity and immunogenicity of an intracellular delivery system of major histocompatibility complex class I epitopes that bypasses proteasome processing.
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TLDR
The authors suggest an alternative strategy: the delivery of epitopes directly to the cell cytosol in a proteasome bypass mechanism of processing, useful for the development of efficient synthetic cell-free vaccines.Abstract:
Summary: The development of a cell-free synthetic vaccine to induce an effective cytotoxic T lymphocyte response is an important challenge in T-cell–mediated immunity. Because standard vaccinations with nominal epitopes were found to be only partially effective in vivo, the authors suggest an alternative strategy: the delivery of epitopes directly to the cell cytosol in a proteasome bypass mechanism of processing. Two model peptides, the presentation level on the cell surface of which can be directly assessed, were conjugated via a cross-linker to an internalization peptide derived from an antennapedia homeobox protein. The linker was designed to undergo spontaneous hydrolysis, after which the epitope is subsequently released. The conjugates were shown to enter RMA and P815 cells, where the epitopes were released mainly in cytosol and endogenously loaded on the major histocompatibility complex class I molecules to be presented on the cell surface. Concomitant inhibition of proteasome activity by MG132 significantly increased the presentation level of both model peptides, indicating proteasome-independent processing. This phenomenon was exploited to enhance the immunogenicity of the conjugates. Conjugates were emulsified with MG132 in incomplete Freund's adjuvant and injected into mouse footpads. Analysis of the draining lymph nodes indicated an increase in the percentage of both CD4+ and CD8+ lymphocytes. In vitro cytolytic assays implied significant, albeit moderate, priming only when the proteasome inhibitor was administered with the conjugate. This approach may be useful for the development of efficient synthetic cell-free vaccines.read more
Citations
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Journal ArticleDOI
Efficient Delivery of Antennapedia Homeodomain Fused to CTL Epitope with Liposomes into Dendritic Cells Results in the Activation of CD8+ T Cells
Ghania Chikh,Spencer Kong,Marcel B. Bally,Jean-Claude Meunier,Marie-Paule Schutze-Redelmeier +4 more
TL;DR: A hybrid CTL epitope delivery system consisting of AntpHD peptide vector formulated in liposomes as an alternative approach to bypass the need for SDS is developed and represents a novel approach for CTL vaccines that may have important applications for development of cancer vaccines.
References
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Journal ArticleDOI
Cell Internalization of the Third Helix of the Antennapedia Homeodomain Is Receptor-independent
Daniele Derossi,Sophie Calvet,Alain Trembleau,Alié Brunissen,Gérard Chassaing,Alain Prochiantz +5 more
TL;DR: The present demonstration, that a reverse helix and a helix composed of D-enantiomers still translocate across biological membranes at 4 and 37°C strongly suggests that the third helix of the homeodomain is internalized by a receptor-independent mechanism.
Journal ArticleDOI
In vivo priming of virus-specific cytotoxic T lymphocytes with synthetic lipopeptide vaccine
TL;DR: It is reported that synthetic viral peptides covalently linked to tripalmitoyl-S-glycerylcysteinyl-seryl-serine (P3CSS) can efficiently prime influenza-virus-specific CTL in vivo and are able to induce the same high-affinity CTL as does the infectious virus.
Journal ArticleDOI
Cell penetrating PNA constructs regulate galanin receptor levels and modify pain transmission in vivo.
Margus Pooga,Margus Pooga,Ursel Soomets,Ursel Soomets,Mattias Hällbrink,Andres Valkna,Andres Valkna,Külliki Saar,Khadijeh Rezaei,Ulrika Kahl,Jing-Xia Hao,Xiao-Jun Xu,Zsuzsanna Wiesenfeld-Hallin,Tomas Hökfelt,Tamas Bartfai,Tamas Bartfai,Ülo Langel +16 more
TL;DR: It is shown that a 21-mer PNA, complementary to the human galanin receptor type 1 mRNA, coupled to the cellular transporter peptides, transportan or pAntennapedia, is efficiently taken up into Bowes cells where they block the expression of Galanin receptors.
Journal ArticleDOI
Processing of some antigens by the standard proteasome but not by the immunoproteasome results in poor presentation by dendritic cells.
Sandra Morel,Frédéric Lévy,Odile Burlet-Schiltz,Francis Brasseur,Michael Probst-Kepper,Anne-Lise Peitrequin,Bernard Monsarrat,Robert Van Velthoven,Jean-Charles Cerottini,Thierry Boon,Jean Edouard Gairin,Benoît Van den Eynde +11 more
TL;DR: It is shown that dendritic cells also carry immunoproteasomes and fail to present this antigen, which may explain why the relevant CTL escape thymic deletion and are not regularly activated in the periphery.
Journal ArticleDOI
Intercellular delivery of functional p53 by the herpesvirus protein VP22.
TL;DR: It is shown that chimeric polypeptides, consisting of VP22 linked to the entire p53 protein, retain their ability to spread between cells and accumulate in recipient cell nuclei, indicating that VP22 delivery may have applications in gene therapy.
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