Monocyte Surface-Bound IL-15 Can Function as an Activating Receptor and Participate in Reverse Signaling

IL-15 is a short chain, four-alpha helix cytokine that shares some biological function with IL-2. One striking difference between IL-2 and IL-15 is the ability of monocytes to express IL-15 on their cell surface after activation. In the current study we have investigated the ability of human monocyt...

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Veröffentlicht in:The Journal of immunology (1950) 2004-04, Vol.172 (7), p.4225-4234
Hauptverfasser: Neely, Graham G, Epelman, Slava, Ma, Ling Ling, Colarusso, Pina, Howlett, Christopher J, Amankwah, Ernest K, McIntyre, Amanda C, Robbins, Stephen M, Mody, Christopher H
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Sprache:eng
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Zusammenfassung:IL-15 is a short chain, four-alpha helix cytokine that shares some biological function with IL-2. One striking difference between IL-2 and IL-15 is the ability of monocytes to express IL-15 on their cell surface after activation. In the current study we have investigated the ability of human monocyte cell surface IL-15 to participate in reverse signaling. Cross-linking anti-IL-15 Abs were used as a surrogate ligand for surface IL-15 engagement. Ligation of cell surface-expressed IL-15 induced monocyte adhesion that required the activity of small m.w. GTPases. Reverse signals through surface IL-15 activated the Rho-GTPase Rac3. In addition, engagement of cell surface IL-15 was found to activate a number of signaling pathways, including both extracellular signal-regulated kinase 1/2 and p38, and resulted in the secretion of IL-8. IL-8 production required mitogen-activated protein kinase activity. Thus, the current study has established that cell surface IL-15 is more than just a ligand; it can function as a receptor and participate in reverse signaling that results in cellular adhesion and production of inflammatory cytokines.
ISSN:0022-1767
1550-6606
DOI:10.4049/jimmunol.172.7.4225