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A genetic screen implicates miRNA-372 and miRNA-373 as oncogenes in testicular germ cell tumors.

P Mathijs Voorhoeve ,
Carlos le Sage ,
Mariette Schrier ,
Ad J M Gillis ,
Hans Stoop ,
Remco Nagel ,
Ying-Poi Liu ,
Josyanne van Duijse ,
Jarno Drost ,
Alexander Griekspoor ,
Eitan Zlotorynski ,
Norikazu Yabuta ,
Gabriella De Vita ,
Hiroshi Nojima ,
Leendert H J Looijenga ,
Reuven Agami

Abstract

Endogenous small RNAs (miRNAs) regulate gene expression by mechanisms conserved across metazoans. While the number of verified human miRNAs is still expanding, only few have been functionally annotated. To perform genetic screens for novel functions of miRNAs, we developed a library of vectors expressing the majority of cloned human miRNAs and created corresponding DNA barcode arrays. In a screen for miRNAs that cooperate with oncogenes in cellular transformation, we identified miR-372 and miR-373, each permitting proliferation and tumorigenesis of primary human cells that harbor both oncogenic RAS and active wild-type p53. These miRNAs neutralize p53-mediated CDK inhibition, possibly through direct inhibition of the expression of the tumor-suppressor LATS2. We provide evidence that these miRNAs are potential novel oncogenes participating in the development of human testicular germ cell tumors by numbing the p53 pathway, thus allowing tumorigenic growth in the presence of wild-type p53.

More about this publication

Cell

Volume 124
Issue nr. 6
Pages 1169-81
Publication date 24-03-2006

Full text links

Publisher website (DOI) 10.1016/j.cell.2006.02.037
Europe PubMed Central 16564011
Pubmed 16564011

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