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KMID : 0620920030350050350
Experimental & Molecular Medicine
2003 Volume.35 No. 5 p.350 ~ p.357
Hypoxia activates signal transducers and activators oftranscription 5 (STAT5) and increases its binding activityto the GAS element in mammary epithelial cells
Joung Youn-Hee

Park Jong-Hwan
Park Tae-Kyu
Lee Chang-Soo
Kim Oun-Hyun
Ye Sang-Kyu
Yang Un-Mok
Lee Kwang-Jeon
Yang Young-Mok
Abstract
STATs (signal transducers and activators of transcription) are proteins with dual functions: signal transducers in the cytoplasm and transcriptional activators in the nucleus. STAT proteins act as transcription factors activated by phosphorylation on its tyrosine residues upon stimulation by various cytokines. The phosphorylated STAT molecules then form homo- or heterodimers through SH2-mediated interaction and translocate into the nucleus to activate the transcription of various target genes. STAT5 recognizes the interferon-¥ã activated site TTCNNNGAA (GAS sequence) in the promoter region of the ¥â-casein gene. Except for prolactin-dependent ¥â-casein production in mammary gland cells, the biological consequences of STAT5a activation in various systems are not clear. Here we showed that STAT5a was phosphorylated 10 min after desferrioxamine (DFO) treatment, and reached a maximum induction at 4 h in mammary epithelial cells (HC11) and transfected COS-7 cells. Under hypoxic conditions (2% O2), a maximal phosphorylation of STAT5a was observed within 6 h. EMSA (electrophoretic mobility shift assay) showed that DFO or hypoxia enhanced the binding activities of STAT5a DNA to ¥â-casein gene promoter in mammary epithelial cells (HC11) and transfected COS-7 cells. These results showed that DFO or hypoxia induces tyrosine phosphorylation of STAT5a and also increases the binding activity of STAT5a DNA in mammary epithelial cells. Our data suggest that the STAT5 may act as a mediator in hypoxia-mediated gene expression.
KEYWORD
binding activity, desferrioxamine, hypoxia, interferon-¥ã activated site, STAT5a, tyrosine phosphorylation
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