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Enhancing transcription–replication conflict targets ecDNA-positive cancers

抄写(语言学) 癌基因 转录因子 DNA DNA复制 生物 癌症研究 遗传学 医学 基因 细胞周期 语言学 哲学
作者
Jun Tang,Natasha E. Weiser,Guiping Wang,Sudhir Chowdhry,Ellis J. Curtis,Yanding Zhao,Ivy Tsz-Lo Wong,Georgi K. Marinov,Rui Li,Philip Hanoian,Edison Tse,Salvador Garcia Mojica,Ryan J. Hansen,Joshua Plum,Auzon Steffy,Snezana Milutinovic,S. Todd Meyer,Jens Luebeck,Yanbo Wang,Shu Zhang
出处
期刊:Nature [Nature Portfolio]
卷期号:635 (8037): 210-218 被引量:59
标识
DOI:10.1038/s41586-024-07802-5
摘要

Abstract Extrachromosomal DNA (ecDNA) presents a major challenge for cancer patients. ecDNA renders tumours treatment resistant by facilitating massive oncogene transcription and rapid genome evolution, contributing to poor patient survival 1–7 . At present, there are no ecDNA-specific treatments. Here we show that enhancing transcription–replication conflict enables targeted elimination of ecDNA-containing cancers. Stepwise analyses of ecDNA transcription reveal pervasive RNA transcription and associated single-stranded DNA, leading to excessive transcription–replication conflicts and replication stress compared with chromosomal loci. Nucleotide incorporation on ecDNA is markedly slower, and replication stress is significantly higher in ecDNA-containing tumours regardless of cancer type or oncogene cargo. pRPA2-S33, a mediator of DNA damage repair that binds single-stranded DNA, shows elevated localization on ecDNA in a transcription-dependent manner, along with increased DNA double strand breaks, and activation of the S-phase checkpoint kinase, CHK1. Genetic or pharmacological CHK1 inhibition causes extensive and preferential tumour cell death in ecDNA-containing tumours. We advance a highly selective, potent and bioavailable oral CHK1 inhibitor, BBI-2779, that preferentially kills ecDNA-containing tumour cells. In a gastric cancer model containing FGFR2 amplified on ecDNA, BBI-2779 suppresses tumour growth and prevents ecDNA-mediated acquired resistance to the pan-FGFR inhibitor infigratinib, resulting in potent and sustained tumour regression in mice. Transcription–replication conflict emerges as a target for ecDNA-directed therapy, exploiting a synthetic lethality of excess to treat cancer.
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