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Cell Cycle Volume 14, 2015 - Issue 13
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Editorials: Cell Cycle Features

Energy crisis and the Hippo pathway

Wenqi WangDepartment of Experimental Radiation Oncology; The University of Texas MD Anderson Cancer Center; Houston, TXUSA
,
Xu LiDepartment of Experimental Radiation Oncology; The University of Texas MD Anderson Cancer Center; Houston, TXUSA
&
Junjie ChenDepartment of Experimental Radiation Oncology; The University of Texas MD Anderson Cancer Center; Houston, TXUSACorrespondence[email protected]
Pages 1995-1996 | Received 04 Apr 2015, Accepted 10 Apr 2015, Published online: 09 Jun 2015

Figures & data

Figure 1. Energy stress regulates the Hippo-YAP pathway. Both AMPK and LATS kinases are activated under energy stress, and once activated phosphorylate YAP at several residues, contributing to the inhibition of YAP transactivation activity. Release from energy stress leads to translocation of YAP into the nucleus, where it forms a complex with TEAD to initiate downstream gene transcription. In addition, a glycolysis enzyme PFK1 has recently been shown to interact with TEAD and maintain the YAP-TEAD complex in the nucleus. The active YAP-TEAD complex promotes cell proliferation, anti-apoptosis, and glycolysis, in part by upregulating GLUT3 and possibly also HK2.

Figure 1. Energy stress regulates the Hippo-YAP pathway. Both AMPK and LATS kinases are activated under energy stress, and once activated phosphorylate YAP at several residues, contributing to the inhibition of YAP transactivation activity. Release from energy stress leads to translocation of YAP into the nucleus, where it forms a complex with TEAD to initiate downstream gene transcription. In addition, a glycolysis enzyme PFK1 has recently been shown to interact with TEAD and maintain the YAP-TEAD complex in the nucleus. The active YAP-TEAD complex promotes cell proliferation, anti-apoptosis, and glycolysis, in part by upregulating GLUT3 and possibly also HK2.

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