Lipopeptide presentation pathway in dendritic cells

Lipopeptides are currently being evaluated as candidate vaccines in human volunteers. They elicit cytotoxic responses from CD8 + T lymphocytes, whereas peptides without a lipidic moiety usually do not. The exact processing and presentation pathways leading to association with MHC class I molecules h...

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Veröffentlicht in:Immunology letters 2001-11, Vol.79 (1), p.97-100
Hauptverfasser: Hosmalin, Anne, Andrieu, Muriel, Loing, Estelle, Desoutter, Jean-François, Hanau, Daniel, Gras-Masse, Hélène, Dautry-Varsat, Alice, Guillet, Jean-Gérard
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Sprache:eng
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Zusammenfassung:Lipopeptides are currently being evaluated as candidate vaccines in human volunteers. They elicit cytotoxic responses from CD8 + T lymphocytes, whereas peptides without a lipidic moiety usually do not. The exact processing and presentation pathways leading to association with MHC class I molecules has not yet been defined. This is of particular interest in dendritic cells, which are required for primary T cell stimulation. We have tracked lipopeptides derived from an HLA-A2.1-restricted HIV-1 Reverse Transcriptase epitope, by N-terminal addition of an N-epsilon-palmitoyl-lysine. Entry of the lipopeptides into human monocyte-derived dendritic cells (MDC) was mediated by endocytosis, as assessed by colocalization using analogs labelled with rhodamine, and by confocal microscopy. This internalization in DC induced functional stimulation of CD8 + T lymphocytes specific for the epitopes, quantified by Interferon-γ ELISPOT assays. The peptide alone was not visualized inside the DC and was only presented through direct surface association to HLA-A*0201. Therefore, lipopeptides provide a model system to define precisely the cross-presentation pathways that lead exogenous proteins to associate with class I MHC molecules within dendritic cells. Using this approach, cross-presentation pathways can be better defined and vaccine lipopeptides can be further optimized for MHC class I association in human dendritic cells.
ISSN:0165-2478
1879-0542
DOI:10.1016/S0165-2478(01)00271-1