| Literature DB >> 17804752 |
Chiara Napoletano1, Aurelia Rughetti, Mads P Agervig Tarp, Julia Coleman, Eric P Bennett, Gianfranco Picco, Patrizio Sale, Kaori Denda-Nagai, Tatsuro Irimura, Ulla Mandel, Henrik Clausen, Luigi Frati, Joyce Taylor-Papadimitriou, Joy Burchell, Marianna Nuti.
Abstract
The type of interaction between tumor-associated antigens and specialized antigen-presenting cells such as dendritic cells (DCs) is critical for the type of immunity that will be generated. MUC1, a highly O-glycosylated mucin, is overexpressed and aberrantly glycosylated in several tumor histotypes. This results in the expression of tumor-associated glycoforms and in MUC1 carrying the tumor-specific glycan Tn (GalNAcalpha1-O-Ser/Thr). Glycopeptides corresponding to three tandem repeats of MUC1, enzymatically glycosylated with 9 or 15 mol of GalNAc, were shown to specifically bind and to be internalized by immature monocyte-derived DCs (iDCs). Binding required calcium and the GalNAc residue and was competed out by GalNAc polymer and Tn-MUC1 or Tn-MUC2 glycopeptides. The macrophage galactose-type C-type lectin (MGL) receptor expressed on iDCs was shown to be responsible for the binding. Confocal analysis and ELISA done on subcellular fractions of iDCs showed that the Tn-MUC1 glycopeptides colocalized with HLA class I and II compartments after internalization. Importantly, although Tn-MUC1 recombinant protein was bound and internalized by MGL, the glycoprotein entered the HLA class II compartment, but not the HLA class I pathway. These data indicate that MGL expressed on iDCs is an optimal receptor for the internalization of short GalNAcs carrying immunogens to be delivered into HLA class I and II compartments. Such glycopeptides therefore represent a new way of targeting the HLA class I and II pathways of DCs. These results have possible implications in designing cancer vaccines.Entities:
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Year: 2007 PMID: 17804752 DOI: 10.1158/0008-5472.CAN-07-1035
Source DB: PubMed Journal: Cancer Res ISSN: 0008-5472 Impact factor: 12.701