Therapeutic synergy between microRNA and siRNA in ovarian cancer treatment.

نویسندگان

  • Masato Nishimura
  • Eun-Jung Jung
  • Maitri Y Shah
  • Chunhua Lu
  • Riccardo Spizzo
  • Masayoshi Shimizu
  • Hee Dong Han
  • Cristina Ivan
  • Simona Rossi
  • Xinna Zhang
  • Milena S Nicoloso
  • Sherry Y Wu
  • Maria Ines Almeida
  • Justin Bottsford-Miller
  • Chad V Pecot
  • Behrouz Zand
  • Koji Matsuo
  • Mian M Shahzad
  • Nicholas B Jennings
  • Cristian Rodriguez-Aguayo
  • Gabriel Lopez-Berestein
  • Anil K Sood
  • George A Calin
چکیده

UNLABELLED Development of improved RNA interference-based strategies is of utmost clinical importance. Although siRNA-mediated silencing of EphA2, an ovarian cancer oncogene, results in reduction of tumor growth, we present evidence that additional inhibition of EphA2 by a microRNA (miRNA) further "boosts" its antitumor effects. We identified miR-520d-3p as a tumor suppressor upstream of EphA2, whose expression correlated with favorable outcomes in two independent patient cohorts comprising 647 patients. Restoration of miR-520d-3p prominently decreased EphA2 protein levels, and suppressed tumor growth and migration/invasion both in vitro and in vivo. Dual inhibition of EphA2 in vivo using 1,2-dioleoyl-sn-glycero-3-phosphatidylcholine (DOPC) nanoliposomes loaded with miR-520d-3p and EphA2 siRNA showed synergistic antitumor efficiency and greater therapeutic efficacy than either monotherapy alone. This synergy is at least in part due to miR-520d-3p targeting EphB2, another Eph receptor. Our data emphasize the feasibility of combined miRNA-siRNA therapy, and will have broad implications for innovative gene silencing therapies for cancer and other diseases. SIGNIFICANCE This study addresses a new concept of RNA inhibition therapy by combining miRNA and siRNA in nanoliposomal particles to target oncogenic pathways altered in ovarian cancer. Combined targeting of the Eph pathway using EphA2-targeting siRNA and the tumor suppressor miR-520d-3p exhibits remarkable therapeutic synergy and enhanced tumor suppression in vitro and in vivo compared with either monotherapy alone.

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عنوان ژورنال:
  • Cancer discovery

دوره 3 11  شماره 

صفحات  -

تاریخ انتشار 2013