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A novel epigenetic CREB-miR-373 axis mediates ZIP4-induced pancreatic cancer growth

  • Yuqing Zhang
  • , Jingxuan Yang
  • , Xiaobo Cui
  • , Yong Chen
  • , Vivian F. Zhu
  • , John P. Hagan
  • , Huamin Wang
  • , Xianjun Yu
  • , Sally E. Hodges
  • , Jing Fang
  • , Paul J. Chiao
  • , Craig D. Logsdon
  • , William E. Fisher
  • , F. Charles Brunicardi
  • , Changyi Chen
  • , Qizhi Yao
  • , Martin E. Fernandez-Zapico
  • , Min Li

Research output: Contribution to journalArticlepeer-review

96 Scopus citations

Abstract

Changes in the intracellular levels of the essential micronutrient zinc have been implicated in multiple diseases including pancreatic cancer; however, the molecular mechanism is poorly understood. Here, we report a novel mechanism where increased zinc mediated by the zinc importer ZIP4 transcriptionally induces miR-373 in pancreatic cancer to promote tumour growth. Reporter, expression and chromatin immunoprecipitation assays demonstrate that ZIP4 activates the zinc-dependent transcription factor CREB and requires this transcription factor to increase miR-373 expression through the regulation of its promoter. miR-373 induction is necessary for efficient ZIP4-dependent enhancement of cell proliferation, invasion, and tumour growth. Further analysis of miR-373 in vivo oncogenic function reveals that it is mediated through its negative regulation of TP53INP1, LATS2 and CD44. These results define a novel ZIP4-CREB-miR-373 signalling axis promoting pancreatic cancer growth, providing mechanistic insights explaining in part how a zinc transporter functions in cancer cells and may have broader implications as inappropriate regulation of intracellular zinc levels plays an important role in many other diseases.

Original languageEnglish
Pages (from-to)1322-1334
Number of pages13
JournalEMBO Molecular Medicine
Volume5
Issue number9
DOIs
StatePublished - Sep 2013

Keywords

  • MicroRNA-373
  • Pancreatic cancer
  • ZIP4
  • Zinc

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