Ozturk Kivilcim, Panwala Rebecca, Sheen Jeanna, Ford Kyle, Payne Nathan, Zhang Dong-Er, Hutter Stephan, Haferlach Torsten, Ideker Trey, Mali Prashant, Carter Hannah
bioRxiv. 2023 Aug 4:2023.08.03.551876. doi: 10.1101/2023.08.03.551876.
Understanding the consequences of single amino acid substitutions in cancer driver genes remains an unmet need. Perturb-seq provides a tool to investigate the effects of individual mutations on cellular programs. Here we deploy SEUSS, a Perturb-seq like approach, to generate and assay mutations at physical interfaces of the RUNX1 Runt domain. We measured the impact of 115 mutations on RNA profiles in single myelogenous leukemia cells and used the profiles to categorize mutations into three functionally distinct groups: wild-type (WT)-like, loss-of-function (LOF)-like and hypomorphic. Notably, the largest concentration of functional mutations (non-WT-like) clustered at the DNA binding site and contained many of the more frequently observed mutations in human cancers. Hypomorphic variants shared characteristics with loss of function variants but had gene expression profiles indicative of response to neural growth factor and cytokine recruitment of neutrophils. Additionally, DNA accessibility changes upon perturbations were enriched for RUNX1 binding motifs, particularly near differentially expressed genes. Overall, our work demonstrates the potential of targeting protein interaction interfaces to better define the landscape of prospective phenotypes reachable by amino acid substitutions.
了解癌症驱动基因中单个氨基酸取代的后果仍是一项尚未满足的需求。Perturb-seq提供了一种工具,用于研究单个突变对细胞程序的影响。在这里,我们采用了一种类似Perturb-seq的方法SEUSS,在RUNX1 Runt结构域的物理界面处生成并检测突变。我们测量了115个突变对单核细胞白血病细胞RNA谱的影响,并利用这些谱将突变分为三个功能上不同的组:野生型(WT)样、功能丧失(LOF)样和亚效型。值得注意的是,功能突变(非WT样)的最大集中区域聚集在DNA结合位点,并且包含许多在人类癌症中更频繁观察到的突变。亚效型变体与功能丧失变体具有共同特征,但具有指示对神经生长因子和中性粒细胞细胞因子募集反应的基因表达谱。此外,扰动后DNA可及性的变化富含RUNX1结合基序,特别是在差异表达基因附近。总体而言,我们的工作证明了靶向蛋白质相互作用界面以更好地定义氨基酸取代可达到的预期表型格局的潜力。
