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NRAS and BRAF Mutations in Melanoma-Associated Nevi and Uninvolved Nevi
Authors:Philipp Tschandl  Anna Sophie Berghoff  Matthias Preusser  Sebastian Burgstaller-Muehlbacher  Hubert Pehamberger  Ichiro Okamoto  Harald Kittler
Institution:1. Department of Dermatology, Medical University of Vienna, Vienna, Austria.; 2. Institute of Neurology and Comprehensive Cancer Center, Medical University of Vienna, Vienna, Austria.; 3. Department of Medicine I and Comprehensive Cancer Center, Medical University of Vienna, Vienna, Austria,
Abstract:According to the prevailing multistep model of melanoma development, oncogenic BRAF or NRAS mutations are crucial initial events in melanoma development. It is not known whether melanocytic nevi that are found in association with a melanoma are more likely to carry BRAF or NRAS mutations than uninvolved nevi. By laser microdissection we were able to selectively dissect and genotype cells either from the nevus or from the melanoma part of 46 melanomas that developed in association with a nevus. In 25 cases we also genotyped a control nevus of the same patients. Available tissue was also immunostained using the BRAFV600E-mutation specific antibody VE1. The BRAFV600E mutation was found in 63.0% of melanomas, 65.2% of associated nevi and 50.0% of control nevi. No significant differences in the distribution of BRAF or NRAS mutations could be found between melanoma and associated nevi or between melanoma associated nevi and control nevi. In concordant cases immunohistochemistry showed a higher expression (intensity of immunohistochemistry) of the mutated BRAFV600E-protein in melanomas compared to their associated nevi. In this series the presence of a BRAF- or NRAS mutation in a nevus was not associated with the risk of malignant transformation. Our findings do not support the current traditional model of stepwise tumor progression.
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