Hypusination of Eukaryotic Initiation Factor 5A (eIF5A): a Novel Therapeutic Target in BCR-ABL-positive Leukemias Identified by a Proteomics Approach

Overview

Journal Blood

Publisher Elsevier

Specialty Hematology

Date 2006 Sep 30

PMID 17008552

Citations 46

Authors

Stefan Balabanov

Artur Gontarewicz

Patrick Ziegler

Ulrike Hartmann

Winfried Kammer

Mhairi Copland

Ute Brassat

Martin Priemer

Ilona Hauber

Thomas Wilhelm

Gerold Schwarz

Lothar Kanz

Carsten Bokemeyer

Joachim Hauber

Tessa L Holyoake

Alfred Nordheim

Tim H Brummendorf

Affiliations

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Abstract

Inhibition of BCR-ABL tyrosine kinase with imatinib represents a major breakthrough in the treatment of patients with chronic myeloid leukemia (CML). However, resistance to imatinib develops frequently, particularly in late-stage disease. To identify new cellular BCR-ABL downstream targets, we analyzed differences in global protein expression in BCR-ABL-positive K562 cells treated with or without imatinib in vitro. Among the 19 proteins found to be differentially expressed, we detected the down-regulation of eukaryotic initiation factor 5A (eIF5A), a protein essential for cell proliferation. eIF5A represents the only known eukaryotic protein activated by posttranslational hypusination. Hypusination inhibitors (HIs) alone exerted an antiproliferative effect on BCR-ABL-positive and -negative leukemia cell lines in vitro. However, the synergistic dose-response relationship found for the combination of imatinib and HI was restricted to Bcr-Abl-positive cells. Furthermore, this synergistic effect was confirmed by cytotoxicity assays, cell-cycle analysis, and CFSE labeling of primary CD34+ CML cells. Specificity of this effect could be demonstrated by cotreatment of K562 cells with imatinib and siRNA against eIF5. In conclusion, through a comparative proteomics approach and further functional analysis, we identified the inhibition of eIF5A hypusination as a promising new approach for combination therapy in BCR-ABL-positive leukemias.

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