Phosphorylation of EIF4E by MNKs Supports Protein Synthesis, Cell Cycle Progression and Proliferation in Prostate Cancer Cells

Overview

Journal Carcinogenesis

Specialty Oncology

Date 2008 Sep 24

PMID 18809972

Citations 70

Authors

Andrea Bianchini

Maria Loiarro

Pamela Bielli

Roberta Busa

Maria Paola Paronetto

Fabrizio Loreni

Raffaele Geremia

Claudio Sette

Affiliations

Soon will be listed here.

Abstract

Deregulation of the phosphatidyl inositol trisphosphate kinase/AKT/mammalian target of rapamycin (mTOR) and RAS/mitogen-activated protein kinase (MAPK)/MNK pathways frequently occurs in human prostate carcinomas (PCas) and leads to aberrant modulation of messenger RNA (mRNA) translation. We have investigated the relative contribution of these pathways to translational regulation and proliferation of PCa cells. MNK-dependent phosphorylation of eIF4E is elevated in DU145 cells, which have low basal levels of AKT/mTOR activity due to the expression of the tumor suppressor PTEN. In contrast, eIF4E phosphorylation is low in PC3 and LNCaP cells with mutated PTEN and constitutively active AKT/mTOR pathway, but it can be strongly induced through inhibition of mTOR activity by rapamycin or serum depletion. Remarkably, we found that inhibition of MNKs strongly reduced the polysomal recruitment of terminal oligopyrimidine messenger RNAs (TOP mRNAs), which are known targets of mTOR-dependent translational control. Pull-down assays of the eIF4F complex indicated that translation initiation was differently affected by inhibition of MNKs and mTOR. In addition, concomitant treatment with MNK inhibitor and rapamycin exerted additive effects on polysomal recruitment of TOP mRNAs and protein synthesis. The MNK inhibitor was more effective than rapamycin in blocking proliferation of PTEN-expressing cells, whereas combination of the two inhibitors suppressed cell cycle progression in both cell lines. Microarray analysis showed that MNK affected translation of mRNAs involved in cell cycle progression. Thus, our results indicate that a balance between the activity of the AKT/mTOR and the MAPK/MNK pathway in PCa cells maintains a defined translational level of specific mRNAs required for ribosome biogenesis, cell proliferation and stress response and might confer to these cells the ability to overcome negative insults.

Citing Articles

Splicing targeting drugs highlight intron retention as an actionable vulnerability in advanced prostate cancer.

Naro C, Antonioni A, Medici V, Caggiano C, Jolly A, De La Grange P J Exp Clin Cancer Res. 2024; 43(1):58.

PMID: 38413979 PMC: 10898177. DOI: 10.1186/s13046-024-02986-0.

In Vivo Investigation of the Effect of Dietary Acrylamide and Evaluation of Its Clinical Relevance in Colon Cancer.

Neophytou C, Katsonouri A, Christodoulou M, Papageorgis P Toxics. 2023; 11(10).

PMID: 37888706 PMC: 10610724. DOI: 10.3390/toxics11100856.

Master Transcription Factor Reprogramming Unleashes Selective Translation Promoting Castration Resistance and Immune Evasion in Lethal Prostate Cancer.

Santasusagna S, Zhu S, Jawalagatti V, Carceles-Cordon M, Ertel A, Garcia-Longarte S Cancer Discov. 2023; 13(12):2584-2609.

PMID: 37676710 PMC: 10714140. DOI: 10.1158/2159-8290.CD-23-0306.

Baicalin Inhibits Airway Smooth Muscle Cells Proliferation through the RAS Signaling Pathway in Murine Asthmatic Airway Remodeling Model.

Hu L, Li L, Yan C, Cao Y, Duan X, Sun J Oxid Med Cell Longev. 2023; 2023:4144138.

PMID: 36814956 PMC: 9940961. DOI: 10.1155/2023/4144138.

Design, Synthesis and Evaluation of Novel Phorbazole C Derivatives as MNK Inhibitors through Virtual High-Throughput Screening.

Jin X, Li M, Qiu T, Yu R, Jiang T Mar Drugs. 2022; 20(7).

PMID: 35877722 PMC: 9319845. DOI: 10.3390/md20070429.