| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 2107112 | Cancer Cell | 2012 | 18 Pages |
SummaryWe investigated the transcriptional and epigenetic repression of miR-29 by MYC, HDAC3, and EZH2 in mantle cell lymphoma and other MYC-associated lymphomas. We demonstrate that miR-29 is repressed by MYC through a corepressor complex with HDAC3 and EZH2. MYC contributes to EZH2 upregulation via repression of the EZH2 targeting miR-26a, and EZH2 induces MYC via inhibition of the MYC targeting miR-494 to create positive feedback. Combined inhibition of HDAC3 and EZH2 cooperatively disrupted the MYC-EZH2-miR-29 axis, resulting in restoration of miR-29 expression, downregulation of miR-29-targeted genes, and lymphoma growth suppression in vitro and in vivo. These findings define a MYC-mediated miRNA repression mechanism, shed light on MYC lymphomagenesis mechanisms, and reveal promising therapeutic targets for aggressive B-cell malignancies.
► Interplay between MYC, HDAC3, and EZH2 defines a mechanism of miRNA repression ► MYC-miRNA-EZH2 positive feedback loop underlies MYC activity and tumor aggressiveness ► miR-29 is required for MYC oncogenesis and cooperatively regulated by HDAC3 and EZH2 ► Targeting HDAC and EZH2 inhibits aggressive lymphomagenicity in vitro and in vivo
