4.7 Article

Targeting IRF3 as a YAP agonist therapy against gastric cancer

Journal

JOURNAL OF EXPERIMENTAL MEDICINE
Volume 215, Issue 2, Pages 699-718

Publisher

ROCKEFELLER UNIV PRESS
DOI: 10.1084/jem.20171116

Keywords

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Funding

  1. National Key R&D Program of China [2017YFA0504504]
  2. National Natural Science Foundation of China [91442125, 31470736, 31470868, 91542125, 81773212, 81725014]
  3. Strategic Priority Research Program [XDB19020202, XDA12020342]
  4. Science and Technology Commission of Shanghai Municipality [17YF1422200, 17ZR1435400]
  5. Youth Innovation Promotion Association of the Chinese Academy of Sciences
  6. SA-SIBS Scholarship Program
  7. Shanghai Institute of Biochemistry and Cell Biology

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The Hippo pathway plays a vital role in tissue homeostasis and tumorigenesis. The transcription factor IRF3 is essential for innate antiviral immunity. In this study, we discovered IRF3 as an agonist of Yes-associated protein (YAP). The expression of IRF3 is positively correlated with that of YAP and its target genes in gastric cancer; the expression of both IRF3 and YAP is up-regulated and prognosticates patient survival. IRF3 interacts with both YAP and TEAD4 in the nucleus to enhance their interaction, promoting nuclear translocation and activation of YAP. IRF3 and YAP-TEAD4 are associated genome-wide to cobind and coregulate many target genes of the Hippo pathway. Overexpression of active IRF3 increased, but depletion of IRF3 reduced, the occupancy of YAP on the target genes. Knockdown or pharmacological targeting of IRF3 by Amlexanox, a drug used clinically for antiinflammatory treatment, inhibits gastric tumor growth in a YAP-dependent manner. Collectively, our study identifies IRF3 as a positive regulator for YAP, highlighting a new therapeutic target against YAP-driven cancers.

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