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Oncofetal H19 RNA promotes tumor metastasis
Authors:Imad J Matouk  Eli Raveh  Rasha Abu-lail  Shaul Mezan  Michal Gilon  Eitan Gershtain  Tatiana Birman  Jennifer Gallula  Tamar Schneider  Moshe Barkali  Carmelit Richler  Yakov Fellig  Vladimir Sorin  Ayala Hubert  Abraham Hochberg  Abraham Czerniak
Institution:1. Department of Biological Chemistry, Institute of Life Sciences, The Hebrew University of Jerusalem, Jerusalem 91904, Israel;2. Department of Pathology, Hadassah Hebrew University Medical Center, Jerusalem 91240, Israel;3. Department of Oncology, Hadassah University Hospital, Jerusalem 91000, Israel;4. Department of HPB Surgery “A”, Sheba Medical Center, Tel Hashomer, Tel Aviv 52621, Israel
Abstract:The oncofetal H19 gene transcribes a long non-coding RNA(lncRNA) that is essential for tumor growth. Here we found that numerous established inducers of epithelial to mesenchymal transition(EMT) also induced H19/miR-675 expression. Both TGF-β and hypoxia concomitantly induced H19 and miR-675 with the induction of EMT markers. We identified the PI3K/AKT pathway mediating the inductions of Slug, H19 RNA and miR-675 in response to TGF-β treatment, while Slug induction depended on H19 RNA. In the EMT induced multidrug resistance model, H19 level was also induced. In a mouse breast cancer model, H19 expression was tightly correlated with metastatic potential. In patients, we detected high H19 expression in all common metastatic sites tested, regardless of tumor primary origin. H19 RNA suppressed the expression of E-cadherin protein. H19 up-regulated Slug expression concomitant with the suppression of E-cadherin protein through a mechanism that involved miR-675. Slug also up-regulated H19 expression and activated its promoter. Altogether, these results may support the existence of a positive feedback loop between Slug and H19/miR-675, that regulates E-cadherin expression. H19 RNA enhanced the invasive potential of cancer cells in vitro and enhanced tumor metastasis in vivo. Additionally, H19 knockdown attenuated the scattering and tumorigenic effects of HGF/SF. Our results present novel mechanistic insights into a critical role for H19 RNA in tumor progression and indicate a previously unknown link between H19/miR-675, Slug and E-cadherin in the regulation of cancer cell EMT programs.
Keywords:Epithelial to mesenchymal transition  E-cadherin  Slug  Positive loop  H19  miR-675
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