SPRY2 is an Inhibitor of the Ras/extracellular Signal-regulated Kinase Pathway in Melanocytes and Melanoma Cells with Wild-type BRAF but Not with the V599E Mutant

Overview

Journal Cancer Res

Specialty Oncology

Date 2004 Aug 18

PMID 15313890

Citations 56

Authors

Dimitra Tsavachidou

Mathew L Coleman

Galene Athanasiadis

Shuixing Li

Jonathan D Licht

Michael F Olson

Barbara L Weber

Affiliations

Soon will be listed here.

Abstract

BRAF mutations result in constitutively active BRAF kinase activity and increased extracellular signal-regulated kinase (ERK) signaling and cell proliferation. Initial studies have shown that BRAF mutations occur at a high frequency in melanocytic nevi and metastatic lesions, but recent data have revealed much lower incidence of these mutations in early-stage melanoma, implying that other factors may contribute to melanoma pathogenesis in a wild-type (WT) BRAF context. To identify such contributing factors, we used microarray gene expression profiling to screen for differences in gene expression between a panel of melanocytic and melanoma cell lines with WT BRAF and a group of melanoma cell lines with the V599E BRAF mutation. We found that SPRY2, an inhibitor homologous to SPRY4, which was previously shown to suppress Ras/ERK signaling via direct binding to Raf-1, had reduced expression in WT BRAF cells. Using small interfering RNA-mediated SPRY2 knockdown, we showed that SPRY2 acts as an inhibitor of ERK signaling in melanocytes and WT BRAF melanoma cells, but not in cell lines with the V599E mutation. We also show that SPRY2 and SPRY4 directly bind WT BRAF but not the V599E and other exon 15 BRAF mutants. These data suggest that SPRY2, an inhibitor of ERK signaling, may be bypassed in melanoma cells either by down-regulation of its expression in WT BRAF cells, or by the presence of the BRAF mutation.

Citing Articles

Model ensembling as a tool to form interpretable multi-omic predictors of cancer pharmacosensitivity.

De Landtsheer S, Badkas A, Kulms D, Sauter T Brief Bioinform. 2024; 25(6).

PMID: 39494610 PMC: 11532660. DOI: 10.1093/bib/bbae567.

Therapeutic effect and transcriptome-methylome characteristics of METTL3 inhibition in liver hepatocellular carcinoma.

Liu Q, Qi J, Li W, Tian X, Zhang J, Liu F Cancer Cell Int. 2023; 23(1):298.

PMID: 38012755 PMC: 10683134. DOI: 10.1186/s12935-023-03096-1.

TRAF7-targeted HOXA5 acts as a tumor suppressor in prostate cancer progression and stemness via transcriptionally activating SPRY2 and regulating MEK/ERK signaling.

Ye J, Liu W, Yu X, Wu L, Chen Z, Yu Y Cell Death Discov. 2023; 9(1):378.

PMID: 37845209 PMC: 10579307. DOI: 10.1038/s41420-023-01675-9.

Examining the Effects of Gestational Physical Activity and Hofbauer Cell Polarization on Angiogenic Factors.

Goudreau A, Tanara L, Tzaneva V, Adamo K Int J Environ Res Public Health. 2023; 20(13).

PMID: 37444145 PMC: 10342061. DOI: 10.3390/ijerph20136298.

ABL1/2 and DDR1 Drive MEKi Resistance in NRAS-Mutant Melanomas by Stabilizing RAF/MYC/ETS1 and Promoting RAF Homodimerization.

Lyon A, Tripathi R, Meeks C, He D, Wu Y, Liu J Cancers (Basel). 2023; 15(3).

PMID: 36765910 PMC: 9913232. DOI: 10.3390/cancers15030954.