MicroRNA-424 impairs ubiquitination to activate STAT3 and promote prostate tumor progression
Cecilia Dallavalle, … , Carlo V. Catapano, Giuseppina M. Carbone
Cecilia Dallavalle, … , Carlo V. Catapano, Giuseppina M. Carbone
Published November 7, 2016
Citation Information: J Clin Invest. 2016;126(12):4585-4602. https://doi.org/10.1172/JCI86505.
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Research Article Oncology

MicroRNA-424 impairs ubiquitination to activate STAT3 and promote prostate tumor progression

Abstract

Mutations and deletions in components of ubiquitin ligase complexes that lead to alterations in protein turnover are important mechanisms in driving tumorigenesis. Here we describe an alternative mechanism involving upregulation of the microRNA miR-424 that leads to impaired ubiquitination and degradation of oncogenic transcription factors in prostate cancers. We found that miR-424 targets the E3 ubiquitin ligase COP1 and identified STAT3 as a key substrate of COP1 in promoting tumorigenic and cancer stem-like properties in prostate epithelial cells. Altered protein turnover due to impaired COP1 function led to accumulation and enhanced basal and cytokine-induced activity of STAT3. We further determined that loss of the ETS factor ESE3/EHF is the initial event that triggers the deregulation of the miR-424/COP1/STAT3 axis. COP1 silencing and STAT3 activation were effectively reverted by blocking of miR-424, suggesting a possible strategy to attack this key node of tumorigenesis in ESE3/EHF–deficient tumors. These results establish miR-424 as an oncogenic effector linked to noncanonical activation of STAT3 and as a potential therapeutic target.

Authors

Cecilia Dallavalle, Domenico Albino, Gianluca Civenni, Jessica Merulla, Paola Ostano, Maurizia Mello-Grand, Simona Rossi, Marco Losa, Gioacchino D’Ambrosio, Fausto Sessa, George N. Thalmann, Ramon Garcia-Escudero, Andrea Zitella, Giovanna Chiorino, Carlo V. Catapano, Giuseppina M. Carbone

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Figure 2

ESE3/EHF occupies MIR424 promoter region and represses miR-424 transcription.

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ESE3/EHF occupies MIR424 promoter region and represses miR-424 transcrip...
(A) Schema of MIR424 promoter and position of the evaluated ETS binding site relative to the 5′ end of pri-miR-424 (RefSeq NR_029946). (B) ESE3/EHF occupancy on MIR424 promoter evaluated by ChIP and quantitative PCR in indicated cell lines. The results are represented relative to input. Bottom panels: Immunoblots of ESE3 in indicated cell lines. (C) miR-424 level in DU145 with stable ESE3/EHF (pESE3) expression compared with control cells (pcDNA). The results were normalized to RNU6 and are represented as miR-424 expression relative to pcDNA. Bottom panel: Immunoblot of ESE3. (D) miR-424 level evaluated by qRT-PCR in DU145 following transfection with pESE3 or pcDNA at the indicated time points (top), and immunoblot of ESE3/EHF (bottom). *P < 0.05; **P < 0.01.