Journal ArticleDOI
Distinct Sets of Genetic Alterations in Melanoma
John A. Curtin,Jane Fridlyand,Toshiro Kageshita,Hetal N. Patel,Klaus J. Busam,Heinz Kutzner,Kwang Hyun Cho,Setsuya Aiba,Eva B. Bröcker,Philip E. LeBoit,Daniel Pinkel,Boris C. Bastian +11 more
TLDR
The genetic alterations identified in melanoma at different sites and with different levels of sun exposure indicate that there are distinct genetic pathways in the development of melanoma and implicate CDK4 and CCND1 as independent oncogenes in melanomas without mutations in BRAF or N-RAS.Abstract:
Background Exposure to ultraviolet light is a major causative factor in melanoma, although the relationship between risk and exposure is complex. We hypothesized that the clinical heterogeneity is explained by genetically distinct types of melanoma with different susceptibility to ultraviolet light. Methods We compared genome-wide alterations in the number of copies of DNA and mutational status of BRAF and N-RAS in 126 melanomas from four groups in which the degree of exposure to ultraviolet light differs: 30 melanomas from skin with chronic sun-induced damage and 40 melanomas from skin without such damage; 36 melanomas from palms, soles, and subungual (acral) sites; and 20 mucosal melanomas. Results We found significant differences in the frequencies of regional changes in the number of copies of DNA and mutation frequencies in BRAF among the four groups of melanomas. Samples could be correctly classified into the four groups with 70 percent accuracy on the basis of the changes in the number of copies of...read more
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The melanomas: a synthesis of epidemiological, clinical, histopathological, genetic, and biological aspects, supporting distinct subtypes, causal pathways, and cells of origin.
TL;DR: This review outlines the historical developments that underpin the understanding of melanoma heterogeneity from the perspectives of clinical presentation, histopathology, epidemiology, molecular genetics, and developmental biology and integrates the evidence from these separate trajectories to catalog the emerging major categories of melanomas.
Journal ArticleDOI
A distinct subset of atypical Spitz tumors is characterized by BRAF mutation and loss of BAP1 expression.
Thomas Wiesner,Rajmohan Murali,Isabella Fried,Lorenzo Cerroni,Klaus J. Busam,Heinz Kutzner,Boris C. Bastian +6 more
TL;DR: The combination of BRAF mutation and loss of nuclear BAP1 expression thus characterizes a subset of ASTs with distinct histologic features, and it is necessary to determine whether this subset has a predictable clinical behavior.
Journal ArticleDOI
Gene expression profiling-based identification of molecular subtypes in stage IV melanomas with different clinical outcome.
Göran Jönsson,Christian Busch,Stian Knappskog,Jürgen Geisler,Hrvoje Miletic,Markus Ringnér,Johan R. Lillehaug,Åke Borg,Per Eystein Lønning +8 more
TL;DR: The data reveal a biologically based taxonomy of malignant melanomas with prognostic effect and support an influence of the antitumoral immune response on outcome.
Journal ArticleDOI
MicroRNA Expression Profiles Associated with Mutational Status and Survival in Malignant Melanoma
Stefano Caramuta,Suzanne Egyhazi,Monica Rodolfo,Daniela Witten,Johan Hansson,Catharina Larsson,Weng-Onn Lui +6 more
TL;DR: Findings show miRNA dysregulation in malignant melanoma and its relation to established molecular backgrounds of BRAF and NRAS oncogenic mutations and the identification of an miRNA classifier for poor survival may lead to the development of miRNA detection as a complementary prognostic tool in clinical practice.
Journal ArticleDOI
Differential sensitivity of melanoma cell lines with BRAFV600E mutation to the specific Raf inhibitor PLX4032.
Jonas Nørskov Søndergaard,Jonas Nørskov Søndergaard,Ramin Nazarian,Qi Wang,Deliang Guo,Teli Hsueh,Stephen Mok,Hooman Sazegar,Laura E. MacConaill,Laura E. MacConaill,Jordi Barretina,Jordi Barretina,Sarah M. Kehoe,Sarah M. Kehoe,Narsis Attar,Erika von Euw,Jonathan E. Zuckerman,Bartosz Chmielowski,Begoña Comin-Anduix,Richard C. Koya,Paul S. Mischel,Roger S. Lo,Antoni Ribas +22 more
TL;DR: Testing the anti-tumor effects of a specific inhibitor of Raf protein kinases, PLX4032/RG7204, in melanoma cell lines showed a range of sensitivities to PLX 4032 and metabolic imaging using PET probes can be used to assess sensitivity.
References
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Mutations of the BRAF gene in human cancer
Helen Davies,Graham R. Bignell,Charles Cox,Philip J. Stephens,Sarah Edkins,S. M. Clegg,Jon W. Teague,Hayley Woffendin,Mathew J. Garnett,William Bottomley,Neil Davis,Ed Dicks,Rebecca Ewing,Yvonne Floyd,Kristian Gray,S. Hall,Rachel Hawes,Jaime Hughes,Vivian Kosmidou,Andrew Menzies,Catherine Mould,Adrian Parker,Claire Stevens,Stephen Watt,Steven Hooper,Rebecca Wilson,Hiran Jayatilake,Barry A. Gusterson,Colin Cooper,Janet Shipley,Darren Hargrave,Kathy Pritchard-Jones,Norman J. Maitland,Georgia Chenevix-Trench,Gregory J. Riggins,Darell D. Bigner,Giuseppe Palmieri,Antonio Cossu,Adrienne M. Flanagan,Andrew G. Nicholson,Judy W. C. Ho,Suet Yi Leung,Siu Tsan Yuen,Barbara L. Weber,Hilliard F. Seigler,Timothy L. Darrow,Hugh Paterson,Richard Marais,Christopher J. Marshall,Richard Wooster,Michael R. Stratton,P. Andrew Futreal +51 more
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Ross Ihaka,Robert Gentleman +1 more
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Journal ArticleDOI
A new regulatory motif in cell-cycle control causing specific inhibition of cyclin D/CDK4
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Comparison of discrimination methods for the classification of tumors using gene expression data
TL;DR: Different discrimination methods for the classification of tumors based on gene expression data include nearest-neighbor classifiers, linear discriminant analysis, and classification trees, which are applied to datasets from three recently published cancer gene expression studies.
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High resolution analysis of DNA copy number variation using comparative genomic hybridization to microarrays
Daniel Pinkel,Daniel Pinkel,Richard Segraves,Damir Sudar,Steven M. Clark,Ian Poole,David Kowbel,Colin Collins,Wen Lin Kuo,Chira Chen,Ye Zhai,Shanaz H. Dairkee,Britt-Marie Ljung,Joe W. Gray,Joe W. Gray,Donna G. Albertson,Donna G. Albertson,Donna G. Albertson +17 more
TL;DR: The implementation of array CGH is demonstrated to be able to measure copy number with high precision in the human genome, and to analyse clinical specimens by obtaining new information on chromosome 20 aberrations in breast cancer.
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