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Rare BRAF mutations in melanoma patients: implications for molecular testing in clinical practice
Authors:L Heinzerling  S Kühnapfel  D Meckbach  M Baiter  E Kaempgen  P Keikavoussi  G Schuler  A Agaimy  J Bauer  A Hartmann  F Kiesewetter  R Schneider-Stock
Institution:1.Department of Dermatology, University Hospital Erlangen, 91052 Erlangen, Germany;2.Department of Pathology, University of Erlangen-Nürnberg, 91054 Erlangen, Germany;3.Experimental Tumor Pathology, Department of Pathology, University of Erlangen-Nürnberg, 91054 Erlangen, Germany;4.Department of Dermatology, University Hospital Tübingen, 72076 Tübingen, Germany
Abstract:

Background:

The detection of V600E BRAF mutation in melanoma is fundamental since here BRAF inhibitors represent an effective treatment. Non-V600E BRAF mutations that may also respond are not detected by certain screening methods. Thus, knowledge about detection of these mutations is needed.

Methods:

A total of 276 tumour samples from 174 melanoma patients were investigated for BRAF mutations by pyrosequencing. Rare mutations were confirmed by capillary sequencing and compared with findings from COBAS test and immunohistochemistry using a novel BRAF antibody. Melanoma type, localisation, and survival were summarised.

Results:

BRAF mutations were found in 43% of patients (124 tumours in 75 patients). Among those, 14 patients (18.7%) exhibited rare mutations. The V600EK601del and V600DK601del mutations have never been described before in melanoma. Furthermore, V600K, V600E2, and V600D, V600G, V600R, and L597S mutations were detected. Mutations were not detected by COBAS test in 7 out of these 14 patients and immunohistochemistry only reliably detected patients with the V600E2 and V600EK601del mutation.

Conclusion:

Accurate diagnosis of rare BRAF mutations is crucial. We show that pyrosequencing is accurate, highly sensitive, reliable, and time saving to detect rare BRAF mutations. Missing these rare variant mutations would exclude a subset of patients from available effective BRAF-targeting therapy.
Keywords:melanoma  pyrosequencing  Sanger  COBAS  survival  immunohistochemistry
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