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Expression and activity of eIF6 trigger Malignant Pleural Mesothelioma growth in vivo

Miluzio, A; Oliveto, S; Pesce, E; Mutti, L; Murer, B; Grosso, S; Ricciardi, S; Brina, D; Biffo, S

Expression and activity of eIF6 trigger Malignant Pleural Mesothelioma growth in vivo Thumbnail


Authors

A Miluzio

S Oliveto

E Pesce

L Mutti

B Murer

S Grosso

S Ricciardi

D Brina

S Biffo



Abstract

eIF6 is an antiassociation factor that regulates the availability of active 80S. Its activation is driven by the RACK1/PKCβ axis, in a mTORc1 independent manner. We previously described that eIF6 haploinsufficiency causes a striking survival in the Eμ-Myc mouse lymphoma model, with lifespans extended up to 18 months. Here we screen for eIF6 expression in human cancers. We show that Malignant Pleural Mesothelioma tumors (MPM) and a MPM cell line (REN cells) contain high levels of hyperphosphorylated eIF6. Enzastaurin is a PKC beta inhibitor used in clinical trials. We prove that Enzastaurin treatment decreases eIF6 phosphorylation rate, but not eIF6 protein stability. The growth of REN, in vivo, and metastasis are reduced by either Enzastaurin treatment or eIF6 shRNA. Molecular analysis reveals that eIF6 manipulation affects the metabolic status of malignant mesothelioma cells. Less glycolysis and less ATP content are evident in REN cells depleted for eIF6 or treated with Enzastaurin (Anti-Warburg effect). We propose that eIF6 is necessary for malignant mesothelioma growth, in vivo, and can be targeted by kinase inhibitors.

Citation

Miluzio, A., Oliveto, S., Pesce, E., Mutti, L., Murer, B., Grosso, S., …Biffo, S. (2015). Expression and activity of eIF6 trigger Malignant Pleural Mesothelioma growth in vivo. Oncotarget, 2015(6), 37471-37485. https://doi.org/10.18632/oncotarget.5462

Journal Article Type Article
Acceptance Date Sep 24, 2015
Online Publication Date Oct 6, 2015
Publication Date Oct 6, 2015
Deposit Date Nov 8, 2016
Publicly Available Date Nov 19, 2018
Journal Oncotarget
Publisher Impact Journals
Volume 2015
Issue 6
Pages 37471-37485
DOI https://doi.org/10.18632/oncotarget.5462
Publisher URL http://dx.doi.org/10.18632/oncotarget.5462

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