Author:
Greenman Chris D.,Pleasance Erin D.,Newman Scott,Yang Fengtang,Fu Beiyuan,Nik-Zainal Serena,Jones David,Lau King Wai,Carter Nigel,Edwards Paul A.W.,Futreal P. Andrew,Stratton Michael R.,Campbell Peter J.
Abstract
Cancer genomes are complex, carrying thousands of somatic mutations including base substitutions, insertions and deletions, rearrangements, and copy number changes that have been acquired over decades. Recently, technologies have been introduced that allow generation of high-resolution, comprehensive catalogs of somatic alterations in cancer genomes. However, analyses of these data sets generally do not indicate the order in which mutations have occurred, or the resulting karyotype. Here, we introduce a mathematical framework that begins to address this problem. By using samples with accurate data sets, we can reconstruct relatively complex temporal sequences of rearrangements and provide an assembly of genomic segments into digital karyotypes. For cancer genes mutated in rearranged regions, this information can provide a chronological examination of the selective events that have taken place.
Publisher
Cold Spring Harbor Laboratory
Subject
Genetics (clinical),Genetics
Cited by
109 articles.
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