Direct regulation of TWIST by HIF-1α promotes metastasis

被引:0
|
作者
Muh-Hwa Yang
Min-Zu Wu
Shih-Hwa Chiou
Po-Min Chen
Shyue-Yih Chang
Chung-Ji Liu
Shu-Chun Teng
Kou-Juey Wu
机构
[1] Institutes of Biochemistry & Molecular Biology,Division of Hematology
[2] National Yang-Ming University,Oncology, Departments of Medicine
[3] No. 155,Department of Dentistry
[4] Sec. 2,undefined
[5] Clinical Medicine,undefined
[6] National Yang-Ming University,undefined
[7] No. 155,undefined
[8] Sec. 2,undefined
[9] Taipei Veterans General Hospital,undefined
[10] No. 201,undefined
[11] Sec. 2,undefined
[12] Medical Research & Education,undefined
[13] Taipei Veterans General Hospital,undefined
[14] No. 201,undefined
[15] Sec. 2,undefined
[16] Otolaryngology,undefined
[17] Taipei Veterans General Hospital,undefined
[18] No. 201,undefined
[19] Sec. 2,undefined
[20] Genomic Research Center,undefined
[21] Taipei Veterans General Hospital,undefined
[22] No. 201,undefined
[23] Sec. 2,undefined
[24] Taipei Mackay Memorial Hospital,undefined
[25] No. 92,undefined
[26] Sec. 2,undefined
[27] Graduate Institute of Microbiology,undefined
[28] College of Medicine,undefined
[29] National Taiwan University,undefined
[30] No. 1,undefined
[31] Sec,undefined
[32] 2,undefined
来源
Nature Cell Biology | 2008年 / 10卷
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摘要
Stabilization of the hypoxia-inducible factor-1α (HIF-1α) transcription complex, caused by intratumoural hypoxia, promotes tumour progression and metastasis, leading to treatment failure and mortality in different types of human cancers. The transcription factor TWIST is a master regulator of gastrulation and mesoderm-specification and was implicated recently as an essential mediator of cancer metastasis. Notably, HIF-1α- and TWIST-null mice show similarities in their phenotypes. Here, we have shown that hypoxia or overexpression of HIF-1α promotes epithelial–mesenchymal transition (EMT) and metastastic phenotypes. We also found that HIF-1 regulates the expression of TWIST by binding directly to the hypoxia-response element (HRE) in the TWIST proximal promoter. However, siRNA-mediated repression of TWIST in HIF-1α-overexpressing or hypoxic cells reversed EMT and metastastic phenotypes. Co-expression of HIF-1α, TWIST and Snail in primary tumours of patients with head and neck cancers correlated with metastasis and the worst prognosis. These results provide evidence of a key signalling pathway involving HIF-1α and TWIST that promotes metastasis in response to intratumoural hypoxia.
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页码:295 / 305
页数:10
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