The interleukin-4 receptor activates STAT5 by a mechanism that relies upon common γ-chain

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Abstract

Interleukin (IL)-4 signaling proceeds via cytoplasmic activation of the Janus kinases JAK1 and JAK3 and the signal transducer and activator of transcription STAT6. We show that the IL-4 receptor, like other cytokine receptor systems utilizing the common receptor γ-chain (γc), is also connected to a signaling pathway that involves STAT5. Both STAT5a and STAT5b become tyrosine-phosphorylated and acquire specific DNA-binding properties in response to IL-4 receptor stimulation in the murine pro-B cell line Ba/F3. In preactivated human T cells, STAT5 became activated in an IL-4-dependent fashion as assayed by IL-4-induced STAT5 translocation from the cytoplasm to the cell nucleus and by binding to cognate DNA. Moreover, stimulation of preactivated human T cells by IL-4 led to specific transcriptional upregulation of STAT5 target genes. IL-4 receptor-mediated STAT5 activation is dependent on the presence of γc and JAK3 within the receptor complex. In COS-7 cells, the JAK/STAT pathway leading from the IL-4 receptor to STAT5- dependent regulation of a reporter gene relied largely on coexpression of JAK3. In Ba/F3 cells, studies on signal transduction evoked by directed specific receptor homo- or heterodimerization revealed that STAT5 activation can be triggered exclusively by IL-4R heterodimers containing γc.

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Lischke, A., Moriggl, R., Brändlein, S., Berchtold, S., Kammer, W., Sebald, W., … Friedrich, K. (1998). The interleukin-4 receptor activates STAT5 by a mechanism that relies upon common γ-chain. Journal of Biological Chemistry, 273(47), 31222–31229. https://doi.org/10.1074/jbc.273.47.31222

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