FOXP3 and FOXP3-regulated microRNAs suppress SATB1 in breast cancer cells

被引:0
|
作者
N McInnes
T J Sadlon
C Y Brown
S Pederson
M Beyer
J L Schultze
S McColl
G J Goodall
S C Barry
机构
[1] Women's and Children's Health Research Institute,Department of Paediatrics
[2] Molecular Immunology Laboratory,Department of Immunology
[3] Women's and Children's Hospital,Department of Medicine
[4] The University of Adelaide,Department of Gastroenterology
[5] LIMES-Institute,undefined
[6] Laboratory for Genomics and Immunoregulation,undefined
[7] University of Bonn,undefined
[8] The University of Adelaide,undefined
[9] Centre for Cancer Biology,undefined
[10] SA Pathology,undefined
[11] University of Adelaide,undefined
[12] Women's and Children's Hospital,undefined
来源
Oncogene | 2012年 / 31卷
关键词
SATB1; FOXP3; microRNA; gene regulation networks; breast cancer; tumour suppressor;
D O I
暂无
中图分类号
学科分类号
摘要
The transcription factor FOXP3 has been identified as a tumour suppressor in the breast and prostate epithelia, but little is known about its specific mechanism of action. We have identified a feed-forward regulatory loop in which FOXP3 suppresses the expression of the oncogene SATB1. In particular, we demonstrate that SATB1 is not only a direct target of FOXP3 repression, but that FOXP3 also induces two miRs, miR-7 and miR-155, which specifically target the 3′-UTR of SATB1 to further regulate its expression. We conclude that FOXP3-regulated miRs form part of the mechanism by which FOXP3 prevents the transformation of the healthy breast epithelium to a cancerous phenotype. Approaches aimed at restoring FOXP3 function and the miRs it regulates could help provide new approaches to target breast cancer.
引用
收藏
页码:1045 / 1054
页数:9
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