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Genomic architecture and evolution of clear cell renal cell carcinomas defined by multiregion sequencing

Abstract: Clear cell renal carcinomas (ccRCCs) can display intratumor heterogeneity (ITH). We applied multiregion exome sequencing (M-seq) to resolve the genetic architecture and evolutionary histories of ten ccRCCs. Ultra-deep sequencing identified ITH in all cases. We found that 73–75% of identified ccRCC driver aberrations were subclonal, confounding estimates of driver mutation prevalence. ITH increased with the number of biopsies analyzed, without evidence of saturation in most tumors. Chromosome 3p loss and VHL aberrations were the only ubiquitous events. The proportion of C>T transitions at CpG sites increased during tumor progression. M-seq permits the temporal resolution of ccRCC evolution and refines mutational signatures occurring during tumor development.

Other publications of the same journal or congress with authors from the University of Cantabria

 Fuente: Nature Genetics, 2014, 46(3), 225-233

 Year of publication: 2014

 No. of pages: 24

 Publication type: Article

 DOI: 10.1038/ng.2891

 ISSN: 1061-4036,1546-1718

Authorship

GERLINGER, MARCO

HORSWELL, STUART

LARKIN, JAMES

ROWAN, ANDREW J

FISHER, ROSALIE

MCGRANAHAN, NICHOLAS

MATTHEWS, NICHOLAS

SANTOS, CLAUDIO R

MARTÍNEZ, PIERRE

PHILLIMORE, BENJAMIN

BEGUM, SHARMIN

RABINOWITZ, ADAM

SPENCER-DENE, BRADLEY

GULATI, SAKSHI

BATES, PAUL A

STAMP, GORDON

PICKERING, LISA

GORE, MARTÍN

NICOL, DAVID L

HAZELL, STEVEN

FUTREAL, P ANDREW

STEWART, AENGUS

SWANTON, CHARLES