Genetic and pharmacological disruption of the TEAD–YAP complex suppresses the oncogenic activity of YAP

Liu‐Chittenden, Yi; Huang, Bo; Shim, Joong Sup; Chen, Qian; Lee, Se-Jin; Anders, Robert A.; Liu, Jun O.; Pan, Duojia

doi:10.1101/gad.192856.112

articleGenes & DevelopmentJun 7, 2012DIAMOND OA

Genetic and pharmacological disruption of the TEAD–YAP complex suppresses the oncogenic activity of YAP

YLYi Liu‐Chittenden BHBo Huang JSJoong Sup Shim QCQian Chen SLSe-Jin Lee

Howard Hughes Medical Institute · Johns Hopkins University · +1 more institution

PubMed

Indexed incrossrefpubmed

Abstract

The Drosophila TEAD ortholog Scalloped is required for Yki-mediated overgrowth but is largely dispensable for normal tissue growth, suggesting that its mammalian counterpart may be exploited for selective inhibition of oncogenic growth driven by YAP hyperactivation. Here we test this hypothesis genetically and pharmacologically. We show that a dominant-negative TEAD molecule does not perturb normal liver growth but potently suppresses hepatomegaly/tumorigenesis resulting from YAP overexpression or Neurofibromin 2 (NF2)/Merlin inactivation. We further identify verteporfin as a small molecule that inhibits TEAD-YAP association and YAP-induced liver overgrowth. These findings provide proof of principle that…

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Topics & keywords

Topics

Keywords

Biology
Hippo signaling pathway
Carcinogenesis
Cancer research
Cell biology
Hyperactivation
Merlin (protein)
Mutation

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