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在 216 种癌细胞系中进行平行的全基因组功能丧失筛选,以鉴定特定于上下文的遗传依赖性。

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

机构信息

Broad Institute of Harvard and MIT, 7 Cambridge Center , Cambridge, Massachusetts 02142, USA.

Broad Institute of Harvard and MIT, 7 Cambridge Center , Cambridge, Massachusetts 02142, USA ; Department of Medical, Dana-Farber Cancer Institute , 450 Brookline Avenue, Boston, Massachusetts 02215, USA.

出版信息

Sci Data. 2014 Sep 30;1:140035. doi: 10.1038/sdata.2014.35. eCollection 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.

摘要

利用一个基于基因组规模的慢病毒递送 shRNA 文库,我们在 216 种癌细胞系中进行了大规模平行的 pooled shRNA 筛选,以鉴定对细胞增殖和/或存活至关重要的基因。通过每个基因 5 个 shRNA 来检测 11000 个基因对细胞系的依赖性。通过将每个细胞系的 1100 万个细胞群体转导到每个细胞一个 shRNA 病毒中,并在经过 16 次群体倍增后使用下一代测序来确定 54000 个 shRNA 中的每一个的相对富集或耗尽,来评估每个 shRNA 在每个细胞系中的增殖效应。所有细胞系都使用标准化条件进行筛选,以最好地评估细胞系之间的差异遗传依赖性。当与这些细胞系的基因组特征相结合时,该数据集促进了遗传依赖性与特定细胞环境(例如基因突变或细胞谱系)的关联。为了实现这些比较,我们开发并提供了一种生物信息学工具,以识别这些特征之间的线性和非线性相关性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1b25/4432652/f3c23aeac5a5/sdata201435-f1.jpg

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