The Prognostic Significance of Eukaryotic Translation Initiation Factors (eIFs) in Endometrial Cancer

Overview

Journal Int J Mol Sci

Publisher MDPI

Specialties Biochemistry
Chemistry
Molecular Biology

Date 2019 Dec 11

PMID 31817792

Citations 8

Authors

Maria Anna Smolle

Piotr Czapiewski

Sylwia Lapinska-Szumczyk

Hanna Majewska

Anna Supernat

Anna Zaczek

Wojciech Biernat

Nicole Golob-Schwarzl

Johannes Haybaeck

Affiliations

Soon will be listed here.

Abstract

Whilst the role of eukaryotic translation initiation factors (eIFs) has already been investigated in several human cancers, their role in endometrial cancer (EC) is relatively unknown. In the present retrospective study, 279 patients with EC (1180 samples) were included (mean age: 63.0 years, mean follow-up: 6.1 years). Samples were analysed for expression of 7 eIFs subunits (eIF2α, eIF3c, eIF3h, eIF4e, eIF4g, eIF5, eIF6) through immunohistochemistry and western blotting. Fifteen samples of healthy endometrium served as controls. Density and intensity were assessed and mean combined scores (CS) calculated for each patient. Upon immunohistochemistry, median eIF5 CS were significantly higher in EC as compared with non-neoplastic tissue (NNT, < 0.001), whilst median eIF6 CS were significantly lower in EC ( < 0.001). Moreover, eIF5 ( = 0.002), eIF6 ( = 0.032) and eIF4g CS ( = 0.014) were significantly different when comparing NNT with EC grading types. Median eIF4g CS was higher in type II EC ( = 0.034). Upon western blot analysis, eIF4g ( < 0.001), peIF2α ( < 0.001) and eIF3h ( < 0.05) were significantly overexpressed in EC, while expression of eIF3c was significantly reduced in EC as compared with NNT ( < 0.001). The remaining eIFs were non-significant. Besides tumour stage ( < 0.001) and patient's age ( < 0.001), high eIF4g CS-levels were independently associated with poor prognosis (HR: 1.604, 95%CI: 1.037-2.483, = 0.034). The other eIFs had no prognostic significance. Notably, the independent prognostic significance of eIF4g was lost when adding tumour type. Considering the difficulties in differentiating EC type I and II, eIF4g may serve as a novel prognostic marker indicating patient outcome.

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