Targeting ERK Beyond the Boundaries of the Kinase Active Site in Melanoma

Overview

Journal Mol Carcinog

Specialties Molecular Biology
Oncology

Date 2019 Jun 14

PMID 31190430

Citations 18

Authors

Rachel M Sammons

Ranajeet Ghose

Kenneth Y Tsai

Kevin N Dalby

Affiliations

Soon will be listed here.

Abstract

Extracellular signal-regulated kinase 1/2 (ERK1/2) constitute a point of convergence for complex signaling events that regulate essential cellular processes, including proliferation and survival. As such, dysregulation of the ERK signaling pathway is prevalent in many cancers. In the case of BRAF-V600E mutant melanoma, ERK inhibition has emerged as a viable clinical approach to abrogate signaling through the ERK pathway, even in cases where MEK and Raf inhibitor treatments fail to induce tumor regression due to resistance mechanisms. Several ERK inhibitors that target the active site of ERK have reached clinical trials, however, many critical ERK interactions occur at other potentially druggable sites on the protein. Here we discuss the role of ERK signaling in cell fate, in driving melanoma, and in resistance mechanisms to current BRAF-V600E melanoma treatments. We explore targeting ERK via a distinct site of protein-protein interaction, known as the D-recruitment site (DRS), as an alternative or supplementary mode of ERK pathway inhibition in BRAF-V600E melanoma. Targeting the DRS with inhibitors in melanoma has the potential to not only disrupt the catalytic apparatus of ERK but also its noncatalytic functions, which have significant impacts on spatiotemporal signaling dynamics and cell fate.

Citing Articles

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Identification and biochemical characterization of small molecule inhibitors of ERK2 that target the D-recruitment site.

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