| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 2107250 | Cancer Cell | 2010 | 15 Pages |
SummaryIn multiple myeloma (MM), an incurable B cell neoplasm, mutation or deletion of p53 is rarely detected at diagnosis. Using small-molecule inhibitors of MDM2, we provide evidence that miR-192, 194, and 215, which are downregulated in a subset of newly diagnosed MMs, can be transcriptionally activated by p53 and then modulate MDM2 expression. Furthermore, ectopic re-expression of these miRNAs in MM cells increases the therapeutic action of MDM2 inhibitors in vitro and in vivo by enhancing their p53-activating effects. In addition, miR-192 and 215 target the IGF pathway, preventing enhanced migration of plasma cells into bone marrow. The results suggest that these miRNAs are positive regulators of p53 and that their downregulation plays a key role in MM development.
► microRNA 192, 194, and 215 genes are silent in newly diagnosed MMs ► WT p53 is a transcriptional activator of miR-192, 194, and 215 ► Human MDM2 mRNA is directly downmodulated by miR-192, 194, and 215 ► miR-192, 194, and 215 enhance the pharmacological activity of MDM2 inhibitors
