The whole-genome panorama of cancer drivers

Author:

Sabarinathan RadhakrishnanORCID,Pich OriolORCID,Martincorena IñigoORCID,Rubio-Perez CarlotaORCID,Juul MaleneORCID,Wala JeremiahORCID,Schumacher StevenORCID,Shapira Ofer,Sidiropoulos NikosORCID,Waszak Sebastian M.ORCID,Tamborero DavidORCID,Mularoni LorisORCID,Rheinbay EstherORCID,Hornshøj HenrikORCID,Deu-Pons JordiORCID,Muiños Ferran,Bertl JohannaORCID,Guo QianyunORCID,Creighton Chad J.,Weischenfeldt JoachimORCID,Korbel Jan O.ORCID,Getz GadORCID,Campbell Peter J.,Pedersen Jakob S.ORCID,Beroukhim Rameen,Gonzalez-Perez AbelORCID,López-Bigas NúriaORCID,

Abstract

SUMMARYThe advance of personalized cancer medicine requires the accurate identification of the mutations driving each patient’s tumor. However, to date, we have only been able to obtain partial insights into the contribution of genomic events to tumor development. Here, we design a comprehensive approach to identify the driver mutations in each patient’s tumor and obtain a whole-genome panorama of driver events across more than 2,500 tumors from 37 types of cancer. This panorama includes coding and non-coding point mutations, copy number alterations and other genomic rearrangements of somatic origin, and potentially predisposing germline variants. We demonstrate that genomic events are at the root of virtually all tumors, with each carrying on average 4.6 driver events. Most individual tumors harbor a unique combination of drivers, and we uncover the most frequent co-occurring driver events. Half of all cancer genes are affected by several types of driver mutations. In summary, the panorama described here provides answers to fundamental questions in cancer genomics and bridges the gap between cancer genomics and personalized cancer medicine.

Publisher

Cold Spring Harbor Laboratory

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