Lack of association between BRAF mutation and MAPK ERK activation in melanocytic nevi

Uribe, Pablo; Andrade, Leonardo; Gonzalez, Sergio

Lack of association between BRAF mutation and MAPK ERK activation in melanocytic nevi

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Lack of Association between BRAF Mutation and MAPK ERK Activation in Melanocytic Nevi.pdf(286.31 KB)

Date

2006

Authors

Uribe, Pablo

Andrade, Leonardo

Gonzalez, Sergio

Publisher

NATURE PUBLISHING GROUP

Abstract

The mitogen-activated protein kinase (MAPK) extracellular signal-regulated kinase signaling pathway can be activated through mutations of V-RAF murine sarcoma viral oncogene homolog B1 (BRAF) oncogene, frequently found in melanoma (60%), common nevi (CN) (73-82%), and atypical nevi (AN) (52-80%). MAPK activation has been reported between 0 and 22% in nevi, and 86% of primary melanoma, without any knowledge of BRAF mutational status. We studied the correlation of MAPK activation status, BRAF mutation, and B-Raf expression in CN, AN, and melanoma. Using immunohistochemistry, phosphorylated (active) MAPK and B-Raf expression was studied in 24 CN, 21 AN, and 26 primary cutaneous melanomas (PM). BRAF mutations at codon 600 were assessed by PCR-RFLP. Active MAPK was detected in 29% of CN, 48% of AN, and 85% of PM. BRAF mutation was found in 67% of CN, 62% of AN, and 58% of PM. In all, 23% of CN, 54% of AN, and 93% of PM with BRAF mutation have activated MAPK. All lesions expressed B-Raf. BRAF mutation does not seem to be sufficient to produce MAPK activation in melanocytic nevi, and it is suggested that other events are needed to induce MAPK activation, that is, B-Raf overexpression, inhibition of MAPK phosphatases, or suppression of RAF kinase inhibitors.

Keywords

PROTEIN-KINASE ACTIVATION, SIGNAL-REGULATED KINASES, B-RAF, CUTANEOUS MELANOMAS, TUMOR PROGRESSION, EXPRESSION, CANCER, INHIBITOR, NEOPLASMS, FREQUENCY

URI

https://doi.org/10.1038/sj.jid.5700011
https://repositorio.uc.cl/handle/11534/78386

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