NAD-dependent ADP-ribosylation is one of the posttranslational protein modifications, best known as the pathogenic mechanism of bacterial toxins. ART2 is a toxin-related argininespecific ADP-ribosyltransferase that is expressed by murine T cells as an ecto-enzyme in association with lipid rafts. Inflammation leads to the release of the ART2 substrate NAD from damaged cells. ART2 then catalyzes ADP-ribosylation of raft-associated signalling proteins. ART2 is shed from the T cell surface as an active enzyme upon T cell activation. Shed ART2 ADP-ribosylates secretory proteins including certain cytokines. ADP-riboslyation of membrane and secretory proteins can profoundly influence the function, intercellular communication, and interaction of inflammatory cells. We recently discovered that CD25, the alpha chain of the interleukin-2 receptor, which is constirutively expressed by regulatroy T cells, is a prominent target for ADP-ribosylation. The goal of the proposed project is to identify the arginine residue in CD25 that serves as the acceptor for ADP-ribosylation and to determine the consequences of this modification for the function of CD25. Moreover we will evaluate the effects of CD25-ADP-ribosylation on the function of regulatory T cells.

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Internationaler Bezug Frankreich

Beteiligte Personen Professor Dr. Olivier Boyer; Professor Dr. Michel Seman