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IL-2 Regulates Expression of C-MAF in Human CD4 T Cells
Author(s) -
Aradhana Rani,
Behdad Afzali,
Audrey Kelly,
Lemlem Tewolde-Berhan,
Mark J. Hackett,
Aditi Kanhere,
Isabela PedrozaPacheco,
H. J. M. Bowen,
Stipo Jurčević,
Richard G. Jenner,
David J. Cousins,
Jack A. Ragheb,
Paul Lavender,
Susan John
Publication year - 2011
Publication title -
the journal of immunology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 2.737
H-Index - 372
eISSN - 1550-6606
pISSN - 0022-1767
DOI - 10.4049/jimmunol.1002354
Subject(s) - il 2 receptor , stat5 , chromatin immunoprecipitation , biology , microbiology and biotechnology , interleukin 4 , interleukin 3 , t cell , cytokine , immunology , signal transduction , gene expression , promoter , immune system , gene , genetics
Blockade of IL-2R with humanized anti-CD25 Abs, such as daclizumab, inhibits Th2 responses in human T cells. Recent murine studies have shown that IL-2 also plays a significant role in regulating Th2 cell differentiation by activated STAT5. To explore the role of activated STAT5 in the Th2 differentiation of primary human T cells, we studied the mechanisms underlying IL-2 regulation of C-MAF expression. Chromatin immunoprecipitation studies revealed that IL-2 induced STAT5 binding to specific sites in the C-MAF promoter. These sites corresponded to regions enriched for markers of chromatin architectural features in both resting CD4 and differentiated Th2 cells. Unlike IL-6, IL-2 induced C-MAF expression in CD4 T cells with or without prior TCR stimulation. TCR-induced C-MAF expression was significantly inhibited by treatment with daclizumab or a JAK3 inhibitor, R333. Furthermore, IL-2 and IL-6 synergistically induced C-MAF expression in TCR-activated T cells, suggesting functional cooperation between these cytokines. Finally, both TCR-induced early IL4 mRNA expression and IL-4 cytokine expression in differentiated Th2 cells were significantly inhibited by IL-2R blockade. Thus, our findings demonstrate the importance of IL-2 in Th2 differentiation in human T cells and support the notion that IL-2R-directed therapies may have utility in the treatment of allergic disorders.

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