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Derek C. Radisky
J Clin Invest. 2009;
119(9):2528
doi:10.1172/JCI40555
Abstract |
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H
omeobox (Hox) genes encode transcription factors that act as critical regulators of growth and differentiation during embryogenesis. While many studies have identified increased expression of Hox genes in tumors, much less is known about the mechanistic basis by which Hox genes facilitate tumor development. In this issue of the JCI, McCoy and colleagues show that transgenic mice that express the homeoprotein Six1 in mammary epithelial cells show increases in stem/progenitor cell populations and subsequent tumor development, while in a separate study Micalizzi and colleagues show that overexpression of Six1 facilitates breast cancer cell metastasis by inducing epithelial-mesenchymal transition (EMT) (see the related articles beginning on pages 2663 and 2678, respectively). Their findings implicate Six1 as a central mediator of breast cancer development.
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(4)
| Title and authors |
Publication |
Year |
Cancer stem cell subsets and their relationships.
Hai-Guang Liu, Chong Chen, Han Yang, Yi-Fei Pan, Xiao-Hua Zhang
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J Transl Med
|
2011 |
Functional analysis of HOXD9 in human gliomas and glioma cancer stem cells.
Masanao Tabuse, Shigeki Ohta, Yohei Ohashi, Raita Fukaya, Aya Misawa, Kazunari Yoshida, Takeshi Kawase, Hideyuki Saya, Cécile Thirant, Hérve Chneiweiss, Yumi Matsuzaki, Hideyuki Okano, Yutaka Kawakami, Masahiro Toda
|
Mol Cancer
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2011 |
SIX1 protein expression selectively identifies blastemal elements in Wilms tumor
Daniel Sehic, Jenny Karlsson, Bengt Sandstedt, David Gisselsson
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Pediatr. Blood Cancer
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2011 |
MicroRNA-185 suppresses tumor growth and progression by targeting the Six1 oncogene in human cancers
J S Imam, K Buddavarapu, J S Lee-Chang, S Ganapathy, C Camosy, Y Chen, M K Rao
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Oncogene
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2010 |
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