Title of article
A MicroRNA Targeting Dicer for Metastasis Control
Author/Authors
Graziano Martello، نويسنده , , Antonio Rosato، نويسنده , , Francesco Ferrari، نويسنده , , Andrea Manfrin، نويسنده , , Michelangelo Cordenonsi، نويسنده , , Sirio Dupont، نويسنده , , Elena Enzo، نويسنده , , Vincenza Guzzardo، نويسنده , , Maria Rondina، نويسنده , , Thomas Spruce، نويسنده , , Anna R. Parenti، نويسنده , , Maria Grazia Daidone، نويسنده , , Silvio Bicciato، نويسنده , , Stefano Piccolo، نويسنده ,
Issue Information
هفته نامه با شماره پیاپی سال 2010
Pages
13
From page
1195
To page
1207
Abstract
Although specific microRNAs (miRNAs) can be upregulated in cancer, global miRNA downregulation is a common trait of human malignancies. The mechanisms of this phenomenon and the advantages it affords remain poorly understood. Here we identify a microRNA family, miR-103/107, that attenuates miRNA biosynthesis by targeting Dicer, a key component of the miRNA processing machinery. In human breast cancer, high levels of miR-103/107 are associated with metastasis and poor outcome. Functionally, miR-103/107 confer migratory capacities in vitro and empower metastatic dissemination of otherwise nonaggressive cells in vivo. Inhibition of miR-103/107 opposes migration and metastasis of malignant cells. At the cellular level, a key event fostered by miR-103/107 is induction of epithelial-to-mesenchymal transition (EMT), attained by downregulating miR-200 levels. These findings suggest a new pathway by which Dicer inhibition drifts epithelial cancer toward a less-differentiated, mesenchymal fate to foster metastasis.
Journal title
CELL
Serial Year
2010
Journal title
CELL
Record number
1020325
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