miR-221 affects multiple cancer pathways by modulating the level of hundreds messenger RNAs

نویسندگان

  • Laura Lupini
  • Cristian Bassi
  • Manuela Ferracin
  • Nenad Bartonicek
  • Lucilla D'Abundo
  • Barbara Zagatti
  • Elisa Callegari
  • Gentian Musa
  • Farzaneh Moshiri
  • Laura Gramantieri
  • Fernando J. Corrales
  • Anton J. Enright
  • Silvia Sabbioni
  • Massimo Negrini
چکیده

microRNA miR-221 is frequently over-expressed in a variety of human neoplasms. Aim of this study was to identify new miR-221 gene targets to improve our understanding on the molecular tumor-promoting mechanisms affected by miR-221. Gene expression profiling of miR-221-transfected-SNU-398 cells was analyzed by the Sylamer algorithm to verify the enrichment of miR-221 targets among down-modulated genes. This analysis revealed that enforced expression of miR-221 in SNU-398 cells caused the down-regulation of 602 mRNAs carrying sequences homologous to miR-221 seed sequence within their 3'UTRs. Pathways analysis performed on these genes revealed their prominent involvement in cell proliferation and apoptosis. Activation of E2F, MYC, NFkB, and β-catenin pathways was experimentally proven. Some of the new miR-221 target genes, including RB1, WEE1 (cell cycle inhibitors), APAF1 (pro-apoptotic), ANXA1, CTCF (transcriptional repressor), were individually validated as miR-221 targets in SNU-398, HepG2, and HEK293 cell lines. By identifying a large set of miR-221 gene targets, this study improves our knowledge about miR-221 molecular mechanisms involved in tumorigenesis. The modulation of mRNA level of 602 genes confirms the ability of miR-221 to promote cancer by affecting multiple oncogenic pathways.

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عنوان ژورنال:

دوره 4  شماره 

صفحات  -

تاریخ انتشار 2013