Elevated Expression of Transmembrane IL-15 in Immune Cells Correlates with the Development of Murine Lupus: a Potential Target for Immunotherapy Against SLE |
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| Authors: | H. Bo,&dagger ,,X.-Q. Wei&Dagger ,,H. Dong,,Y. Zhang,P. Lv,W. Liu,A. Koutoulaki&Dagger ,& X.-M. Gao,&dagger |
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| Affiliation: | Department of Immunology, Peking University Health Science Center, Peking University, Beijing, China;;Key Laboratory of Immunology, Ministry for Public Health, China;;and Department of Dental Health and Biological Sciences, Dental School of University of Cardiff, Wales, UK |
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| Abstract: | Presentation in trans by the Interleukin-15 receptor α chain (IL-15Rα) has been suggested as the main mechanism for IL-15 anchoring to the cell surface, but it is also evident that IL-15 can exist as a transmembrane protein. We herein demonstrate that replacement of the first 41 residues of human IL-15 (hIL-15) with Ig κ chain leader sequence resulted in secretion of most of the recombinant hIL-15 expressed in transfectant cells, thus identifying the transmembrane region of IL-15. A fusion protein (hIL-15Rα-Fc) between the extracellular domain of hIL-15Rα and the Fc fragment of IgG1 was prepared and shown to be able to bind with transmembrane IL-15 (tmIL-15). The level of tmIL-15 expression in macrophages, activated T cells and B cells from 6-month-old BXSB male mice, an animal model for systemic lupus erythematosus (SLE), was significantly increased compared with that from BXSB females or young males. In addition, hIL-15Rα-Fc was able to block the T cell stimulating and anti-apoptotic effect of the tmIL-15-positive BXSB macrophages in vitro . Intravenous administration of hIL-15Rα-Fc reduced the titre of autoantibodies against dsDNA and also proteinuria in aged BXSB males, implying that neutralization of IL-15 activity in vivo may be an effective way of treating SLE. |
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