Article ID Journal Published Year Pages File Type
2041244 Cell Reports 2016 15 Pages PDF
Abstract

•The MYCN-regulated miR-17∼92 cluster targets nuclear hormone receptors•An NHR signature is associated with neural differentiation and patient survival•The induction of MYCN or miR-17∼92 attenuates glucocorticoid receptor signaling•Combined MYCN inhibition and GR activation drive differentiation and ease tumor burden

SummaryMYCN amplification and MYC signaling are associated with high-risk neuroblastoma with poor prognosis. Treating these tumors remains challenging, although therapeutic approaches stimulating differentiation have generated considerable interest. We have previously shown that the MYCN-regulated miR-17∼92 cluster inhibits neuroblastoma differentiation by repressing estrogen receptor alpha. Here, we demonstrate that this microRNA (miRNA) cluster selectively targets several members of the nuclear hormone receptor (NHR) superfamily, and we present a unique NHR signature associated with the survival of neuroblastoma patients. We found that suppressing glucocorticoid receptor (GR) expression in MYCN-driven patient and mouse tumors was associated with an undifferentiated phenotype and decreased survival. Importantly, MYCN inhibition and subsequent reactivation of GR signaling promotes neural differentiation and reduces tumor burden. Our findings reveal a key role for the miR-17∼92-regulated NHRs in neuroblastoma biology, thereby providing a potential differentiation approach for treating neuroblastoma patients.

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