51. MHC class II signaling function is regulated during maturation of plasmacytoid dendritic cells
- Author
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Sophie Taque, Laurence Amiot, Nuala Mooney, Dominique Charron, Niclas Setterblad, Valérie Guilloux, Bernard Drenou, and Renée Fauchet
- Subjects
Immunology ,Plasma Cells ,Apoptosis ,Human leukocyte antigen ,Major histocompatibility complex ,Immune system ,Membrane Microdomains ,Interferon ,medicine ,Immunology and Allergy ,Humans ,Protein kinase C ,Cells, Cultured ,Protein Kinase C ,MHC class II ,CD40 ,biology ,hemic and immune systems ,Cell Biology ,Dendritic Cells ,HLA-DR Antigens ,Cell biology ,Enzyme Activation ,biology.protein ,medicine.drug ,Signal Transduction - Abstract
Dendritic cells (DC) play a central role in the immune response, linking innate and adaptative responses to pathogens. Myeloid DC (MDC) produce interleukin-12 in response to bacterial stimuli, whereas plasmacytoid DC (PDC) produce high levels of type I interferon upon viral infection. Human leukocyte antigen (HLA)-DR engagement has been shown to induce apoptosis in various antigen-presenting cells (APC). We now report the consequences of HLA-DR molecule engagement in human PDC, which had thus far not been studied as a result of the difficulty in isolating such cells. HLA-DR engagement on PDC, obtained using a two-step, immunomagnetic separation, led to recruitment of HLA-DR molecules at the site of engagement in mature but not immature PDC. In contrast, relocalization of protein kinase C (PKC) isoenzymes, indicating PKC activation, was observed at the site of HLA-DR engagement and was accompanied by relocalization of a lipid raft marker, the ganglioside M1 staining, in immature and mature PDC. Similar to MDC, HLA-DR-mediated apoptosis was regulated throughout PDC maturation. Freshly isolated PDC were resistant, whereas CD40 ligand-matured PDC were sensitive to HLA-DR-mediated apoptosis. Neither caspase activation nor PKC activation was required for HLA-DR-mediated apoptosis. However, the intrinsic pathway of apoptosis was implicated as mature PDC underwent mitochondrial depolarization in response to HLA-DR engagement. These data provide further arguments for considering HLA-DR-mediated apoptosis as a conserved mechanism of regulating survival of diverse APC and support the ongoing development of humanized ligands for HLA class II molecules as therapeutic tools for use in lymphoproliferative disease.
- Published
- 2005