The Skp2-SCF E3 Ligase Regulates Akt Ubiquitination, Glycolysis, Herceptin Sensitivity, and Tumorigenesis

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作者：Chia-Hsin Chan1sup> ; Chien-Feng Li5sup> ; sup>6sup> ; sup>11sup> ; Wei-Lei Yang1sup> ; sup>4sup> ; Yuan Gao1sup> ; sup>4sup> ; Szu-Wei Lee1sup> ; sup>4sup> ; Zizhen Feng1sup> ; Hsuan-Ying Huang7sup> ; Kelvin ; K.C. Tsai6sup> ; Leo ; G. Flores2sup> ; Yiping Shao3sup> ; John ; D. Hazle3sup> ; Dihua Yu1sup> ; sup>4sup> ; Wenyi Wei8sup> ; Dos Sarbassov1sup> ; sup>4sup> ; Mien-Chie Hung1sup> ; sup>4sup> ; sup>10sup> ; Keiichi ; I. Nakayama9sup> ; Hui-Kuan Lin1sup> ; sup>4sup> ; sup>hklin@mdanderson.orgsup>
刊名：Cell
出版年：2012
期刊代码：50_00928674
类别：med
出版时间：25 May, 2012
卷：149
期：5
页码：1098-1111
文件大小：2129 K

摘要

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ss="h3">Summary

Akt kinase plays a central role in cell growth, metabolism, and tumorigenesis. The TRAF6 E3 ligase orchestrates IGF-1-mediated Akt ubiquitination and activation. Here, we show that Akt ubiquitination is also induced by activation of ErbB receptors; unexpectedly, and in contrast to IGF-1 induced activation, the Skp2 SCF complex, not TRAF6, is a critical E3 ligase for ErbB-receptor-mediated Akt ubiquitination and membrane recruitment in response to EGF. Skp2 deficiency impairs Akt activation, Glut1 expression, glucose uptake and glycolysis, and breast cancer progression in various tumor models. Moreover, Skp2 overexpression correlates with Akt activation and breast cancer metastasis and serves as a marker for poor prognosis in Her2-positive patients. Finally, Skp2 silencing sensitizes Her2-overexpressing tumors to Herceptin treatment. Our study suggests that distinct E3 ligases are utilized by diverse growth factors for Akt activation and that targeting glycolysis sensitizes Her2-positive tumors to Herceptin treatment.

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