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Parallel genome-scale loss of function screens in 216 cancer cell lines for the identification of context-specific genetic dependencies.

Authors :
Cowley GS
Weir BA
Vazquez F
Tamayo P
Scott JA
Rusin S
East-Seletsky A
Ali LD
Gerath WF
Pantel SE
Lizotte PH
Jiang G
Hsiao J
Tsherniak A
Dwinell E
Aoyama S
Okamoto M
Harrington W
Gelfand E
Green TM
Tomko MJ
Gopal S
Wong TC
Li H
Howell S
Stransky N
Liefeld T
Jang D
Bistline J
Hill Meyers B
Armstrong SA
Anderson KC
Stegmaier K
Reich M
Pellman D
Boehm JS
Mesirov JP
Golub TR
Root DE
Hahn WC
Source :
Scientific data [Sci Data] 2014 Sep 30; Vol. 1, pp. 140035. Date of Electronic Publication: 2014 Sep 30 (Print Publication: 2014).
Publication Year :
2014

Abstract

Using a genome-scale, lentivirally delivered shRNA library, we performed massively parallel pooled shRNA screens in 216 cancer cell lines to identify genes that are required for cell proliferation and/or viability. Cell line dependencies on 11,000 genes were interrogated by 5 shRNAs per gene. The proliferation effect of each shRNA in each cell line was assessed by transducing a population of 11M cells with one shRNA-virus per cell and determining the relative enrichment or depletion of each of the 54,000 shRNAs after 16 population doublings using Next Generation Sequencing. All the cell lines were screened using standardized conditions to best assess differential genetic dependencies across cell lines. When combined with genomic characterization of these cell lines, this dataset facilitates the linkage of genetic dependencies with specific cellular contexts (e.g., gene mutations or cell lineage). To enable such comparisons, we developed and provided a bioinformatics tool to identify linear and nonlinear correlations between these features.

Details

Language :
English
ISSN :
2052-4463
Volume :
1
Database :
MEDLINE
Journal :
Scientific data
Publication Type :
Academic Journal
Accession number :
25984343
Full Text :
https://doi.org/10.1038/sdata.2014.35