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Absence of BRAF mutations in UV-protected mucosal melanomas

Background: Mutations in BRAF have recently been identified in a significant percentage of primary and metastatic cutaneous malignant melanomas. As ultraviolet (UV) exposure may play a role in the development of cutaneous melanoma lesions with BRAF mutations, BRAF mutation frequency in melanomas ari... Full description

Journal Title: Journal of medical genetics 2004, Vol.41 (4), p.270-272
Main Author: Edwards, R H
Other Authors: Ward, M R , Wu, H , Medina, C A , Brose, M S , Volpe, P , Nussen-Lee, S , Haupt, H M , Martin, A M , Herlyn, M , Lessin, S R , Weber, B L
Format: Electronic Article Electronic Article
Language: English
Subjects:
Biological and medical sciences
BRAF
Cancer
connective tissue diseases
CPD
cyclobutane pyrimidine dimers
Dermatology
digestive system diseases
DNA Mutational Analysis
endocrine system diseases
Environmental Exposure
Gene Frequency
Genes
Health aspects
Humans
Kinases
Medical sciences
melanoma
Melanoma - genetics
Mucous Membrane
Mutation
neoplasms
Oncology, Experimental
Polymorphism, Restriction Fragment Length
Proto-Oncogene Proteins B-raf
Proto-Oncogene Proteins c-raf - genetics
restriction fragment length polymorphism
RFLP
Risk factors
Short Report
skin
Skin cancer
Skin Neoplasms - etiology
Skin Neoplasms - genetics
Tumors of the skin and soft tissue. Premalignant lesions
ultraviolet
ultraviolet exposure
Ultraviolet radiation
Ultraviolet Rays
Quelle: Alma/SFX Local Collection
Publisher: London: BMJ Publishing Group Ltd
ID: ISSN: 0022-2593
Zum Text:
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recordid: cdi_pubmedcentral_primary_oai_pubmedcentral_nih_gov_1735752
title: Absence of BRAF mutations in UV-protected mucosal melanomas
format: Article
creator:
  • Edwards, R H
  • Ward, M R
  • Wu, H
  • Medina, C A
  • Brose, M S
  • Volpe, P
  • Nussen-Lee, S
  • Haupt, H M
  • Martin, A M
  • Herlyn, M
  • Lessin, S R
  • Weber, B L
subjects:
  • Biological and medical sciences
  • BRAF
  • Cancer
  • connective tissue diseases
  • CPD
  • cyclobutane pyrimidine dimers
  • Dermatology
  • digestive system diseases
  • DNA Mutational Analysis
  • endocrine system diseases
  • Environmental Exposure
  • Gene Frequency
  • Genes
  • Health aspects
  • Humans
  • Kinases
  • Medical sciences
  • melanoma
  • Melanoma - genetics
  • Mucous Membrane
  • Mutation
  • neoplasms
  • Oncology, Experimental
  • Polymorphism, Restriction Fragment Length
  • Proto-Oncogene Proteins B-raf
  • Proto-Oncogene Proteins c-raf - genetics
  • restriction fragment length polymorphism
  • RFLP
  • Risk factors
  • Short Report
  • skin
  • Skin cancer
  • Skin Neoplasms - etiology
  • Skin Neoplasms - genetics
  • Tumors of the skin and soft tissue. Premalignant lesions
  • ultraviolet
  • ultraviolet exposure
  • Ultraviolet radiation
  • Ultraviolet Rays
ispartof: Journal of medical genetics, 2004, Vol.41 (4), p.270-272
description: Background: Mutations in BRAF have recently been identified in a significant percentage of primary and metastatic cutaneous malignant melanomas. As ultraviolet (UV) exposure may play a role in the development of cutaneous melanoma lesions with BRAF mutations, BRAF mutation frequency in melanomas arising in sites protected from sun exposure may be lower than those from sun-exposed areas. Thus, we determined the BRAF mutation frequency in a panel of 13 mucosal melanomas and compared those data with data from all currently published series of cutaneous melanomas. Methods:BRAF exon 15 DNA from 13 archival primary mucosal melanomas (eight vulvar, four anorectal, and one laryngeal) was sequenced using intron-based primers. As archival DNA occasionally produces poor-quality template, results were confirmed with a TspRI restriction fragment length polymorphism (RFLP) that distinguishes wild-type BRAF from the common mutant form V599E. A binomial test was used to compare the mutation frequency in the mucosal melanomas with the published mutation frequency in cutaneous melanomas. Results: None of the 13 mucosal melanomas in this series had an exon 15 BRAF mutation, as compared to 54/165 (33%) primary cutaneous melanomas with BRAF mutations in a compilation of all current published studies (p = 0.006). Discussion: These data suggest that UV exposure, plays a role in the genesis of BRAF mutations in cutaneous melanoma, despite the absence of the characteristic C>T or CC>TT mutation signature associated with UV exposure, and suggests mechanisms other than pyrimidine dimer formation are important in UV-induced mutagenesis.
language: eng
source: Alma/SFX Local Collection
identifier: ISSN: 0022-2593
fulltext: fulltext
issn:
  • 0022-2593
  • 1468-6244
  • 1468-6244
url: Link


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titleAbsence of BRAF mutations in UV-protected mucosal melanomas
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creatorEdwards, R H ; Ward, M R ; Wu, H ; Medina, C A ; Brose, M S ; Volpe, P ; Nussen-Lee, S ; Haupt, H M ; Martin, A M ; Herlyn, M ; Lessin, S R ; Weber, B L
creatorcontribEdwards, R H ; Ward, M R ; Wu, H ; Medina, C A ; Brose, M S ; Volpe, P ; Nussen-Lee, S ; Haupt, H M ; Martin, A M ; Herlyn, M ; Lessin, S R ; Weber, B L
descriptionBackground: Mutations in BRAF have recently been identified in a significant percentage of primary and metastatic cutaneous malignant melanomas. As ultraviolet (UV) exposure may play a role in the development of cutaneous melanoma lesions with BRAF mutations, BRAF mutation frequency in melanomas arising in sites protected from sun exposure may be lower than those from sun-exposed areas. Thus, we determined the BRAF mutation frequency in a panel of 13 mucosal melanomas and compared those data with data from all currently published series of cutaneous melanomas. Methods:BRAF exon 15 DNA from 13 archival primary mucosal melanomas (eight vulvar, four anorectal, and one laryngeal) was sequenced using intron-based primers. As archival DNA occasionally produces poor-quality template, results were confirmed with a TspRI restriction fragment length polymorphism (RFLP) that distinguishes wild-type BRAF from the common mutant form V599E. A binomial test was used to compare the mutation frequency in the mucosal melanomas with the published mutation frequency in cutaneous melanomas. Results: None of the 13 mucosal melanomas in this series had an exon 15 BRAF mutation, as compared to 54/165 (33%) primary cutaneous melanomas with BRAF mutations in a compilation of all current published studies (p = 0.006). Discussion: These data suggest that UV exposure, plays a role in the genesis of BRAF mutations in cutaneous melanoma, despite the absence of the characteristic C>T or CC>TT mutation signature associated with UV exposure, and suggests mechanisms other than pyrimidine dimer formation are important in UV-induced mutagenesis.
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subjectBiological and medical sciences ; BRAF ; Cancer ; connective tissue diseases ; CPD ; cyclobutane pyrimidine dimers ; Dermatology ; digestive system diseases ; DNA Mutational Analysis ; endocrine system diseases ; Environmental Exposure ; Gene Frequency ; Genes ; Health aspects ; Humans ; Kinases ; Medical sciences ; melanoma ; Melanoma - genetics ; Mucous Membrane ; Mutation ; neoplasms ; Oncology, Experimental ; Polymorphism, Restriction Fragment Length ; Proto-Oncogene Proteins B-raf ; Proto-Oncogene Proteins c-raf - genetics ; restriction fragment length polymorphism ; RFLP ; Risk factors ; Short Report ; skin ; Skin cancer ; Skin Neoplasms - etiology ; Skin Neoplasms - genetics ; Tumors of the skin and soft tissue. Premalignant lesions ; ultraviolet ; ultraviolet exposure ; Ultraviolet radiation ; Ultraviolet Rays
ispartofJournal of medical genetics, 2004, Vol.41 (4), p.270-272
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8Martin, A M
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0Absence of BRAF mutations in UV-protected mucosal melanomas
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descriptionBackground: Mutations in BRAF have recently been identified in a significant percentage of primary and metastatic cutaneous malignant melanomas. As ultraviolet (UV) exposure may play a role in the development of cutaneous melanoma lesions with BRAF mutations, BRAF mutation frequency in melanomas arising in sites protected from sun exposure may be lower than those from sun-exposed areas. Thus, we determined the BRAF mutation frequency in a panel of 13 mucosal melanomas and compared those data with data from all currently published series of cutaneous melanomas. Methods:BRAF exon 15 DNA from 13 archival primary mucosal melanomas (eight vulvar, four anorectal, and one laryngeal) was sequenced using intron-based primers. As archival DNA occasionally produces poor-quality template, results were confirmed with a TspRI restriction fragment length polymorphism (RFLP) that distinguishes wild-type BRAF from the common mutant form V599E. A binomial test was used to compare the mutation frequency in the mucosal melanomas with the published mutation frequency in cutaneous melanomas. Results: None of the 13 mucosal melanomas in this series had an exon 15 BRAF mutation, as compared to 54/165 (33%) primary cutaneous melanomas with BRAF mutations in a compilation of all current published studies (p = 0.006). Discussion: These data suggest that UV exposure, plays a role in the genesis of BRAF mutations in cutaneous melanoma, despite the absence of the characteristic C>T or CC>TT mutation signature associated with UV exposure, and suggests mechanisms other than pyrimidine dimer formation are important in UV-induced mutagenesis.
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2Cancer
3connective tissue diseases
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5cyclobutane pyrimidine dimers
6Dermatology
7digestive system diseases
8DNA Mutational Analysis
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10Environmental Exposure
11Gene Frequency
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15Kinases
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18Melanoma - genetics
19Mucous Membrane
20Mutation
21neoplasms
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23Polymorphism, Restriction Fragment Length
24Proto-Oncogene Proteins B-raf
25Proto-Oncogene Proteins c-raf - genetics
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27RFLP
28Risk factors
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32Skin Neoplasms - etiology
33Skin Neoplasms - genetics
34Tumors of the skin and soft tissue. Premalignant lesions
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37Ultraviolet radiation
38Ultraviolet Rays
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titleAbsence of BRAF mutations in UV-protected mucosal melanomas
authorEdwards, R H ; Ward, M R ; Wu, H ; Medina, C A ; Brose, M S ; Volpe, P ; Nussen-Lee, S ; Haupt, H M ; Martin, A M ; Herlyn, M ; Lessin, S R ; Weber, B L
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8DNA Mutational Analysis
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0Edwards, R H
1Ward, M R
2Wu, H
3Medina, C A
4Brose, M S
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7Haupt, H M
8Martin, A M
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atitleAbsence of BRAF mutations in UV-protected mucosal melanomas
jtitleJournal of medical genetics
addtitleJ Med Genet
date2004-04
risdate2004
volume41
issue4
spage270
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pages270-272
issn
00022-2593
11468-6244
eissn1468-6244
codenJMDGAE
notesCorrespondence to:
 B L Weber
 MD, Abramson Family Cancer Research Institute, University of Pennsylvania Medical Center, 514 BRB II/III, 421 Curie Boulevard, Philadelphia, PA 19104, USA; weberb@mail.med.upenn.edu
abstractBackground: Mutations in BRAF have recently been identified in a significant percentage of primary and metastatic cutaneous malignant melanomas. As ultraviolet (UV) exposure may play a role in the development of cutaneous melanoma lesions with BRAF mutations, BRAF mutation frequency in melanomas arising in sites protected from sun exposure may be lower than those from sun-exposed areas. Thus, we determined the BRAF mutation frequency in a panel of 13 mucosal melanomas and compared those data with data from all currently published series of cutaneous melanomas. Methods:BRAF exon 15 DNA from 13 archival primary mucosal melanomas (eight vulvar, four anorectal, and one laryngeal) was sequenced using intron-based primers. As archival DNA occasionally produces poor-quality template, results were confirmed with a TspRI restriction fragment length polymorphism (RFLP) that distinguishes wild-type BRAF from the common mutant form V599E. A binomial test was used to compare the mutation frequency in the mucosal melanomas with the published mutation frequency in cutaneous melanomas. Results: None of the 13 mucosal melanomas in this series had an exon 15 BRAF mutation, as compared to 54/165 (33%) primary cutaneous melanomas with BRAF mutations in a compilation of all current published studies (p = 0.006). Discussion: These data suggest that UV exposure, plays a role in the genesis of BRAF mutations in cutaneous melanoma, despite the absence of the characteristic C>T or CC>TT mutation signature associated with UV exposure, and suggests mechanisms other than pyrimidine dimer formation are important in UV-induced mutagenesis.
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