Your search keyword '"Christopher Chevillard"' showing total 2 results

1. Adenovirus-Inspired Virus-Like-Particles Displaying Melanoma Tumor Antigen Specifically Target Human DC Subsets and Trigger Antigen-Specific Immune Responses.

Author

Besson, Solène, Laurin, David, Chauvière, Cyrielle, Thépaut, Michel, Kleman, Jean-Philippe, Pezet, Mylène, Manches, Olivier, Fieschi, Franck, Aspord, Caroline, and Fender, Pascal

Subjects

TUMOR antigens, IMMUNE response, VIRUS-like particles, VIRAL antigens, MELANOMA, EPITHELIAL cells

Abstract

Virus-like particles constitute versatile vectors that can be used as vaccine platforms in many fields from infectiology and more recently to oncology. We previously designed non-infectious adenovirus-inspired 60-mer dodecahedric virus-like particles named ADDomers displaying on their surface either a short epitope or a large tumor/viral antigen. In this work, we explored for the first time the immunogenicity of ADDomers exhibiting melanoma-derived tumor antigen/epitope and their impact on the features of human dendritic cell (DC) subsets. We first demonstrated that ADDomers displaying tumor epitope/antigen elicit a strong immune-stimulating potential of human DC subsets (cDC2s, cDC1s, pDCs), which were able to internalize and cross-present tumor antigen, and subsequently cross-prime antigen-specific T-cell responses. To further limit off-target effects and enhance DC targeting, we engineered specific motifs to de-target epithelial cells and improve DCs' addressing. The improved engineered platform making it possible to display large antigen represents a tool to overcome the barrier of immune allele restriction, broadening the immune response, and paving the way to its potential utilization in humans as an off-the-shelf vaccine. [ABSTRACT FROM AUTHOR]

Published

2022

2. Mechanical Control of Cell Migration by the Metastasis Suppressor Tetraspanin CD82/KAI1.

Author

Ordas, Laura, Costa, Luca, Lozano, Anthony, Chevillard, Christopher, Calovoulos, Alexia, Kantar, Diala, Fernandez, Laurent, Chauvin, Lucie, Dosset, Patrice, Doucet, Christine, Heron-Milhavet, Lisa, Odintsova, Elena, Berditchevski, Fedor, Milhiet, Pierre-Emmanuel, and Bénistant, Christine

Subjects

TUMOR suppressor proteins, TETRASPANIN, FOCAL adhesions, BREAST cancer, CELL migration, MEMBRANE proteins

Abstract

The plasma membrane is a key actor of cell migration. For instance, its tension controls persistent cell migration and cell surface caveolae integrity. Then, caveolae constituents such as caveolin-1 can initiate a mechanotransduction loop that involves actin- and focal adhesion-dependent control of the mechanosensor YAP to finely tune cell migration. Tetraspanin CD82 (also named KAI-1) is an integral membrane protein and a metastasis suppressor. Its expression is lost in many cancers including breast cancer. It is a strong inhibitor of cell migration by a little-known mechanism. We demonstrated here that CD82 controls persistent 2D migration of EGF-induced single cells, stress fibers and focal adhesion sizes and dynamics. Mechanistically, we found that CD82 regulates membrane tension, cell surface caveolae abundance and YAP nuclear translocation in a caveolin-1-dependent manner. Altogether, our data show that CD82 controls 2D cell migration using membrane-driven mechanics involving caveolin and the YAP pathway. [ABSTRACT FROM AUTHOR]

Published

2021