作者
Diana M Munoz, Pamela J Cassiani, Li Li, Eric Billy, Joshua M Korn, Michael D Jones, Javad Golji, David A Ruddy, Kristine Yu, Gregory McAllister, Antoine DeWeck, Dorothee Abramowski, Jessica Wan, Matthew D Shirley, Sarah Y Neshat, Daniel Rakiec, Rosalie De Beaumont, Odile Weber, Audrey Kauffmann, E Robert McDonald III, Nicholas Keen, Francesco Hofmann, William R Sellers, Tobias Schmelzle, Frank Stegmeier, Michael R Schlabach
发表日期
2016/8/1
期刊
Cancer discovery
卷号
6
期号
8
页码范围
900-913
出版商
American Association for Cancer Research
简介
CRISPR/Cas9 has emerged as a powerful new tool to systematically probe gene function. We compared the performance of CRISPR to RNAi-based loss-of-function screens for the identification of cancer dependencies across multiple cancer cell lines. CRISPR dropout screens consistently identified more lethal genes than RNAi, implying that the identification of many cellular dependencies may require full gene inactivation. However, in two aneuploid cancer models, we found that all genes within highly amplified regions, including nonexpressed genes, scored as lethal by CRISPR, revealing an unanticipated class of false-positive hits. In addition, using a CRISPR tiling screen, we found that sgRNAs targeting essential domains generate the strongest lethality phenotypes and thus provide a strategy to rapidly define the protein domains required for cancer dependence. Collectively, these findings not only …
学术搜索中的文章
DM Munoz, PJ Cassiani, L Li, E Billy, JM Korn… - Cancer discovery, 2016