Quit your YAPing: a new target for cancer therapy

  1. Ben Z. Stanger1
  1. Gastroenterology Division, Department of Medicine, Department of Cell and Developmental Biology, Abramson Family Cancer Research Institute, Perelman School of Medicine, University of Pennsylvania, Philadelphia, Pennsylvania 19104, USA

    Abstract

    The Hippo pathway is an evolutionarily conserved signaling module that plays multiple roles in embryonic development. Components of the pathway, which includes a kinase cascade and a downstream complex composed of YAP and TEAD transcription factors, are dysregulated in a significant fraction of human cancers. In this issue of Genes & Development, Liu-Chittenden and colleagues (pp. 1300–1305) use genetic and pharmacological means to disrupt the active YAP–TEAD complex. As this intervention impedes tumorigenesis in the liver with no apparent effect on normal liver homeostasis, the work paves the way for the development of new strategies to target this pervasive oncogenic pathway.

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    Related Article

    • RESEARCH COMMUNICATION: Genetic and pharmacological disruption of the TEAD–YAP complex suppresses the oncogenic activity of YAP
      • Yi Liu-Chittenden,
      • Bo Huang,
      • Joong Sup Shim,
      • Qian Chen,
      • Se-Jin Lee,
      • Robert A. Anders,
      • Jun O. Liu,
      • and Duojia Pan
      Genes Dev. June 15, 2012 26: 1300-1305; Published in Advance June 7, 2012, doi:10.1101/gad.192856.112
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    1. doi: 10.1101/gad.196501.112 Genes & Dev. 26: 1263-1267 Copyright © 2012 by Cold Spring Harbor Laboratory Press

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