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Hippo signaling regulates microprocessor and links cell-density-dependent miRNA biogenesis to cancer.


ABSTRACT: Global downregulation of microRNAs (miRNAs) is commonly observed in human cancers and can have a causative role in tumorigenesis. The mechanisms responsible for this phenomenon remain poorly understood. Here, we show that YAP, the downstream target of the tumor-suppressive Hippo-signaling pathway regulates miRNA biogenesis in a cell-density-dependent manner. At low cell density, nuclear YAP binds and sequesters p72 (DDX17), a regulatory component of the miRNA-processing machinery. At high cell density, Hippo-mediated cytoplasmic retention of YAP facilitates p72 association with Microprocessor and binding to a specific sequence motif in pri-miRNAs. Inactivation of the Hippo pathway or expression of constitutively active YAP causes widespread miRNA suppression in cells and tumors and a corresponding posttranscriptional induction of MYC expression. Thus, the Hippo pathway links contact-inhibition regulation to miRNA biogenesis and may be responsible for the widespread miRNA repression observed in cancer.

SUBMITTER: Mori M 

PROVIDER: S-EPMC3982296 | biostudies-literature | 2014 Feb

REPOSITORIES: biostudies-literature

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Hippo signaling regulates microprocessor and links cell-density-dependent miRNA biogenesis to cancer.

Mori Masaki M   Triboulet Robinson R   Mohseni Morvarid M   Schlegelmilch Karin K   Shrestha Kriti K   Camargo Fernando D FD   Gregory Richard I RI  

Cell 20140201 5


Global downregulation of microRNAs (miRNAs) is commonly observed in human cancers and can have a causative role in tumorigenesis. The mechanisms responsible for this phenomenon remain poorly understood. Here, we show that YAP, the downstream target of the tumor-suppressive Hippo-signaling pathway regulates miRNA biogenesis in a cell-density-dependent manner. At low cell density, nuclear YAP binds and sequesters p72 (DDX17), a regulatory component of the miRNA-processing machinery. At high cell d  ...[more]

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