Regulation of Tumor Angiogenesis by Ezh2

Göster/
Tarih
2010
Yazar
Lu, Chunhua
Han, Hee Dong
Mangala, Lingegowda S.
Ali-Fehmi, Rouba
Newton, Christopher S.
Ozbun, Laurent
Armaiz-Pena, Guillermo N.
Hu, Wei
Stone, Rebecca L.
Munkarah, Adnan
Ravoori, Murali K.
Shahzad, Mian M. K.
Lee, Jeong-Won
Mora, Edna
Langley, Robert R.
Carroll, Amy R.
Matsuo, Koji
Spannuth, Whitney A.
Schmandt, Rosemarie
Jennings, Nicholas B.
Goodman, Blake W.
Jaffe, Robert B.
Nick, Alpa M.
Kim, Hye Sun
Guven, Eylem Ozturk
Chen, Ya-Huey
Li, Long-Yuan
Hsu, Ming-Chuan
Coleman, Robert L.
Calin, George A.
Denkbas, Emir B.
Lim, Jae Yun
Lee, Ju-Seog
Kundra, Vikas
Birrer, Michael J.
Hung, Mien-Chie
Lopez-Berestein, Gabriel
Sood, Anil K.
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Özet
Although VEGF-targeted therapies are showing promise, new angiogenesis targets are needed to make additional gains. Here, we show that increased Zeste homolog 2 (EZH2) expression in either tumor cells or in tumor vasculature is predictive of poor clinical outcome. The increase in endothelial EZH2 is a direct result of VEGF stimulation by a paracrine circuit that promotes angiogenesis by methylating and silencing vasohibin1 (vash1). Ezh2 silencing in the tumor-associated endothelial cells inhibited angiogenesis mediated by reactivation of VASH1, and reduced ovarian cancer growth, which is further enhanced in combination with ezh2 silencing in tumor cells. Collectively, these data support the potential for targeting ezh2 as an important therapeutic approach.
Bağlantı
https://doi.org/10.1016/j.ccr.2010.06.016
http://hdl.handle.net/11655/19857
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