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DOI: 10.1016/j.ccr.2011.11.024
¤ OpenAccess: Hybrid
This work has “Hybrid” OA status. This means it is free under an open license in a toll-access journal.

Pericyte Depletion Results in Hypoxia-Associated Epithelial-to-Mesenchymal Transition and Metastasis Mediated by Met Signaling Pathway

Vesselina G. Cooke,Valerie S. LeBleu,Doruk Keskin,Zainab Khan,Joyce T. O’Connell,Yingqi Teng,Michael B. Duncan,Liang Xie,Genta Maeda,Sylvia Vong,Hikaru Sugimoto,Rafael Malagoli Rocha,Aline Santos Damascena,Ricardo R. Brentani,Raghu Kalluri

Pericyte
Epithelial–mesenchymal transition
Metastasis
2012
The functional role of pericytes in cancer progression remains unknown. Clinical studies suggest that low numbers of vessel-associated pericytes correlated with a drop in overall survival of patients with invasive breast cancer. Using genetic mouse models or pharmacological inhibitors, pericyte depletion suppressed tumor growth but enhanced metastasis. Pericyte depletion was further associated with increased hypoxia, epithelial-to-mesenchymal transition (EMT), and Met receptor activation. Silencing of Twist or use of a Met inhibitor suppressed hypoxia and EMT/Met-driven metastasis. In addition, poor pericyte coverage coupled with high Met expression in cancer cells speculates the worst prognosis for patients with invasive breast cancer. Collectively, our study suggests that pericytes within the primary tumor microenvironment likely serve as important gatekeepers against cancer progression and metastasis.
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    Pericyte Depletion Results in Hypoxia-Associated Epithelial-to-Mesenchymal Transition and Metastasis Mediated by Met Signaling Pathway” is a paper by Vesselina G. Cooke Valerie S. LeBleu Doruk Keskin Zainab Khan Joyce T. O’Connell Yingqi Teng Michael B. Duncan Liang Xie Genta Maeda Sylvia Vong Hikaru Sugimoto Rafael Malagoli Rocha Aline Santos Damascena Ricardo R. Brentani Raghu Kalluri published in 2012. It has an Open Access status of “hybrid”. You can read and download a PDF Full Text of this paper here.