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癌症细胞中依赖关系的全面临床信息图和目标优先级划分框架。

A comprehensive clinically informed map of dependencies in cancer cells and framework for target prioritization.

机构信息

Wellcome Sanger Institute, Wellcome Genome Campus, Hinxton, Cambridge CB10 1SA, UK; Open Targets, Wellcome Genome Campus, Hinxton, Cambridge CB10 1SA, UK.

Instituto Superior Técnico (IST), Universidade de Lisboa, 1049-001 Lisboa, Portugal; INESC-ID, 1000-029 Lisboa, Portugal.

出版信息

Cancer Cell. 2024 Feb 12;42(2):301-316.e9. doi: 10.1016/j.ccell.2023.12.016. Epub 2024 Jan 11.

Abstract

Genetic screens in cancer cell lines inform gene function and drug discovery. More comprehensive screen datasets with multi-omics data are needed to enhance opportunities to functionally map genetic vulnerabilities. Here, we construct a second-generation map of cancer dependencies by annotating 930 cancer cell lines with multi-omic data and analyze relationships between molecular markers and cancer dependencies derived from CRISPR-Cas9 screens. We identify dependency-associated gene expression markers beyond driver genes, and observe many gene addiction relationships driven by gain of function rather than synthetic lethal effects. By combining clinically informed dependency-marker associations with protein-protein interaction networks, we identify 370 anti-cancer priority targets for 27 cancer types, many of which have network-based evidence of a functional link with a marker in a cancer type. Mapping these targets to sequenced tumor cohorts identifies tractable targets in different cancer types. This target prioritization map enhances understanding of gene dependencies and identifies candidate anti-cancer targets for drug development.

摘要

癌症细胞系中的遗传筛选可提供基因功能和药物发现信息。需要更全面的多组学数据筛选数据集,以增加功能映射遗传缺陷的机会。在这里,我们通过注释 930 种癌症细胞系的多组学数据来构建第二代癌症依赖性图谱,并分析 CRISPR-Cas9 筛选得出的分子标记与癌症依赖性之间的关系。我们确定了除驱动基因之外与依赖性相关的基因表达标记,并观察到许多由功能获得而非合成致死效应驱动的基因成瘾关系。通过将临床相关的依赖性标记关联与蛋白质-蛋白质相互作用网络相结合,我们为 27 种癌症类型确定了 370 个抗癌优先靶点,其中许多靶点在网络上与癌症类型中的标记具有功能关联。将这些靶点映射到测序肿瘤队列中,可以确定不同癌症类型中可处理的靶点。这个目标优先级图谱增强了对基因依赖性的理解,并确定了候选抗癌药物靶点用于药物开发。

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