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  3. Comprehensive Characterization of Cancer Driver Genes and Mutations.
 

Comprehensive Characterization of Cancer Driver Genes and Mutations.

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BORIS DOI
10.7892/boris.126373
Date of Publication
April 5, 2018
Publication Type
Article
Contributor
Bailey, Matthew H
Tokheim, Collin
Porta-Pardo, Eduard
Sengupta, Sohini
Bertrand, Denis
Weerasinghe, Amila
Colaprico, Antonio
Wendl, Michael C
Kim, Jaegil
Reardon, Brendan
Ng, Patrick Kwok-Shing
Jeong, Kang Jin
Cao, Song
Wang, Zixing
Gao, Jianjiong
Gao, Qingsong
Wang, Fang
Liu, Eric Minwei
Mularoni, Loris
Rubio-Perez, Carlota
Nagarajan, Niranjan
Cortés-Ciriano, Isidro
Zhou, Daniel Cui
Liang, Wen-Wei
Hess, Julian M
Yellapantula, Venkata D
Tamborero, David
Gonzalez-Perez, Abel
Suphavilai, Chayaporn
Ko, Jia Yu
Khurana, Ekta
Park, Peter J
Van Allen, Eliezer M
Liang, Han
Lawrence, Michael S
Godzik, Adam
Lopez-Bigas, Nuria
Stuart, Josh
Wheeler, David
Getz, Gad
Chen, Ken
Lazar, Alexander J
Mills, Gordon B
Karchin, Rachel
Ding, Li
Subject(s)

600 - Technology::610...

Series
Cell
ISSN or ISBN (if monograph)
0092-8674
Publisher
Cell Press
Language
English
Publisher DOI
10.1016/j.cell.2018.02.060
PubMed ID
29625053
Uncontrolled Keywords

driver gene discovery...

Description
Identifying molecular cancer drivers is critical for precision oncology. Multiple advanced algorithms to identify drivers now exist, but systematic attempts to combine and optimize them on large datasets are few. We report a PanCancer and PanSoftware analysis spanning 9,423 tumor exomes (comprising all 33 of The Cancer Genome Atlas projects) and using 26 computational tools to catalog driver genes and mutations. We identify 299 driver genes with implications regarding their anatomical sites and cancer/cell types. Sequence- and structure-based analyses identified >3,400 putative missense driver mutations supported by multiple lines of evidence. Experimental validation confirmed 60%-85% of predicted mutations as likely drivers. We found that >300 MSI tumors are associated with high PD-1/PD-L1, and 57% of tumors analyzed harbor putative clinically actionable events. Our study represents the most comprehensive discovery of cancer genes and mutations to date and will serve as a blueprint for future biological and clinical endeavors.
Handle
https://boris-portal.unibe.ch/handle/20.500.12422/64157
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File(s)
FileFile TypeFormatSizeLicensePublisher/Copright statementContent
1-s2.0-S009286741830237X-main.pdftextAdobe PDF12.72 MBAttribution-NonCommercial-NoDerivatives (CC BY-NC-ND 4.0)publishedOpen
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