Author:
Berger Michael F.,Levin Joshua Z.,Vijayendran Krishna,Sivachenko Andrey,Adiconis Xian,Maguire Jared,Johnson Laura A.,Robinson James,Verhaak Roel G.,Sougnez Carrie,Onofrio Robert C.,Ziaugra Liuda,Cibulskis Kristian,Laine Elisabeth,Barretina Jordi,Winckler Wendy,Fisher David E.,Getz Gad,Meyerson Matthew,Jaffe David B.,Gabriel Stacey B.,Lander Eric S.,Dummer Reinhard,Gnirke Andreas,Nusbaum Chad,Garraway Levi A.
Abstract
Global studies of transcript structure and abundance in cancer cells enable the systematic discovery of aberrations that contribute to carcinogenesis, including gene fusions, alternative splice isoforms, and somatic mutations. We developed a systematic approach to characterize the spectrum of cancer-associated mRNA alterations through integration of transcriptomic and structural genomic data, and we applied this approach to generate new insights into melanoma biology. Using paired-end massively parallel sequencing of cDNA (RNA-seq) together with analyses of high-resolution chromosomal copy number data, we identified 11 novel melanoma gene fusions produced by underlying genomic rearrangements, as well as 12 novel readthrough transcripts. We mapped these chimeric transcripts to base-pair resolution and traced them to their genomic origins using matched chromosomal copy number information. We also used these data to discover and validate base-pair mutations that accumulated in these melanomas, revealing a surprisingly high rate of somatic mutation and lending support to the notion that point mutations constitute the major driver of melanoma progression. Taken together, these results may indicate new avenues for target discovery in melanoma, while also providing a template for large-scale transcriptome studies across many tumor types.
Publisher
Cold Spring Harbor Laboratory
Subject
Genetics (clinical),Genetics
Cited by
235 articles.
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