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The role of eIF4E in response and acquired resistance to vemurafenib in melanoma.

The Journal of investigative dermatology (2015-01-24)
Yao Zhan, Michael S Dahabieh, Arjuna Rajakumar, Monica C Dobocan, Marie-Noël M'Boutchou, Christophe Goncalves, Shiru L Lucy, Filippa Pettersson, Ivan Topisirovic, Léon van Kempen, Sonia V Del Rincón, Wilson H Miller
RÉSUMÉ

In eukaryotic cells, the rate-limiting component for cap-dependent mRNA translation is the translation initiation factor eIF4E. eIF4E is overexpressed in a variety of human malignancies, but whether it has a role in melanoma remains obscure. We hypothesized that eIF4E promotes melanoma cell proliferation and facilitates the development of acquired resistance to the BRAF inhibitor vemurafenib. We show that eIF4E is overexpressed in a panel of melanoma cell lines, compared with immortalized melanocytes. Knockdown of eIF4E significantly repressed the proliferation of a subset of melanoma cell lines. Moreover, in BRAF(V600E) melanoma cell lines, vemurafenib inhibits 4E-BP1 phosphorylation, thus promoting its binding to eIF4E. Cap-binding and polysome profiling analysis confirmed that vemurafenib stabilizes the eIF4E-4E-BP1 association and blocks mRNA translation, respectively. Conversely, in cells with acquired resistance to vemurafenib, there is an increased dependence on eIF4E for survival; 4E-BP1 is highly phosphorylated and thus eIF4E-4E-BP1 associations are impeded. Moreover, increasing eIF4E activity by silencing 4E-BP1/2 renders vemurafenib-responsive cells more resistant to BRAF inhibition. In conclusion, these data suggest that therapeutically targeting eIF4E may be a viable means of inhibiting melanoma cell proliferation and overcoming vemurafenib resistance.

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Tris(tert-butoxy)silanol, 99.999%
Sigma-Aldrich
eIF4E Active human, N-terminal GST-tag, recombinant, expressed in E. coli, ≥70% (SDS-PAGE)