Direct Transcriptional Consequences of Somatic Mutation in Breast Cancer

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Disordered transcriptomes of cancer encompass direct effects of somatic mutation on transcription, coordinated secondary pathway alterations, and increased transcriptional noise. To catalog the rules governing how somatic mutation exerts direct transcriptional effects, we developed an exhaustive pipeline for analyzing RNA sequencing data, which we integrated with whole genomes from 23 breast cancers. Using X-inactivation analyses, we found that cancer cells are more transcriptionally active than intermixed stromal cells. This is especially true in estrogen receptor (ER)-negative tumors. Overall, 59% of substitutions were expressed. Nonsense mutations showed lower expression levels than expected, with patterns characteristic of nonsense-mediated decay. 14% of 4,234 rearrangements caused transcriptional abnormalities, including exon skips, exon reusage, fusions, and premature polyadenylation. We found productive, stable transcription from sense-to-antisense gene fusions and gene-to-intergenic rearrangements, suggesting that these mutation classes drive more transcriptional disruption than previously suspected. Systematic integration of transcriptome with genome data reveals the rules by which transcriptional machinery interprets somatic mutation.
Publisher
CELL PRESS
Issue Date
2016-08
Language
English
Article Type
Article
Keywords

ACUTE MYELOID-LEUKEMIA; GENOMIC CHARACTERIZATION; GENE-EXPRESSION; FUSION TRANSCRIPTS; SEQUENCING DATA; CELL; REARRANGEMENT; IDENTIFICATION; LANDSCAPE; DISCOVERY

Citation

CELL REPORTS, v.16, no.7, pp.2032 - 2046

ISSN
2211-1247
DOI
10.1016/j.celrep.2016.07.028
URI
http://hdl.handle.net/10203/219673
Appears in Collection
MSE-Journal Papers(저널논문)
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