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ER Stress Signaling Promotes the Survival of Cancer “Persister Cells” Tolerant to EGFR Tyrosine Kinase Inhibitors

埃罗替尼 生物 癌症研究 信号转导 人口 癌症 医学 细胞生物学 表皮生长因子受体 遗传学 环境卫生
作者
Hideki Terai,Shunsuke Kitajima,Danielle S. Potter,Yusuke Matsui,Laura Gutierrez Quiceno,Ting Chen,Tae Jung Kim,Maria Rusan,Tran C. Thai,Federica Piccioni,Katherine A. Donovan,Nicholas Kwiatkowski,Kunihiko Hinohara,Guo Wei,Nathanael S. Gray,Eric S. Fischer,Kwok‐Kin Wong,Teppei Shimamura,Anthony Letai,Peter S. Hammerman,David A. Barbie
出处
期刊:Cancer Research [American Association for Cancer Research]
卷期号:78 (4): 1044-1057 被引量:79
标识
DOI:10.1158/0008-5472.can-17-1904
摘要

An increasingly recognized component of resistance to tyrosine kinase inhibitors (TKI) involves persistence of a drug-tolerant subpopulation of cancer cells that survive despite effective eradication of the majority of the cell population. Multiple groups have demonstrated that these drug-tolerant persister cells undergo transcriptional adaptation via an epigenetic state change that promotes cell survival. Because this mode of TKI drug tolerance appears to involve transcriptional addiction to specific genes and pathways, we hypothesized that systematic functional screening of EGFR TKI/transcriptional inhibitor combination therapy would yield important mechanistic insights and alternative drug escape pathways. We therefore performed a genome-wide CRISPR/Cas9 enhancer/suppressor screen in EGFR-dependent lung cancer PC9 cells treated with erlotinib + THZ1 (CDK7/12 inhibitor) combination therapy, a combination previously shown to suppress drug-tolerant cells in this setting. As expected, suppression of multiple genes associated with transcriptional complexes (EP300, CREBBP, and MED1) enhanced erlotinib/THZ1 synergy. Unexpectedly, we uncovered nearly every component of the recently described ufmylation pathway in the synergy suppressor group. Loss of ufmylation did not affect canonical downstream EGFR signaling. Instead, absence of this pathway triggered a protective unfolded protein response associated with STING upregulation, promoting protumorigenic inflammatory signaling but also unique dependence on Bcl-xL. These data reveal that dysregulation of ufmylation and ER stress comprise a previously unrecognized TKI drug tolerance pathway that engages survival signaling, with potentially important therapeutic implications.

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