微卫星不稳定癌症细胞中细胞命运的综合图谱支持WRN和ATR的双重靶向。

IF 7.5 1区 生物学 Q1 CELL BIOLOGY Genes & development Pub Date : 2023-10-01 Epub Date: 2023-11-06 DOI:10.1101/gad.351085.123
Dali Zong, Natasha C Koussa, James A Cornwell, Ajith V Pankajam, Michael J Kruhlak, Nancy Wong, Raj Chari, Steven D Cappell, André Nussenzweig
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引用次数: 0

摘要

WRN解旋酶成瘾是具有高水平微卫星不稳定性(MSI-H)的人类癌症的一个独特脆弱性。然而,尽管WRN的长期缺失最终导致细胞死亡,但对MSI-H癌症最初如何对WRN知识的急性缺失做出反应知之甚少,这将有助于为WRN靶向治疗的临床开发提供信息,预测可能的耐药性机制,并确定成功抑制WRN的有用生物标志物。在这里,我们报道了一种诱导型配体介导的降解系统的构建,在该系统中,内源性WRN蛋白的稳定性可以快速而特异性地调节,使我们能够跟踪WRN功能急性丧失引起的细胞事件的完整序列。我们发现,WRN降解以复制依赖的方式导致DNA损伤的立即增加,奇怪的是,这种方式并没有有力地参与检查点机制来阻止DNA合成。结果,WRN降解的MSI-H癌症细胞在多个复制周期中积累DNA损伤,并经历连续几轮越来越异常的有丝分裂,最终触发细胞死亡。对于潜在的治疗重要性,我们没有发现任何证据表明MSI-H癌症可以适应WRN几乎完全丧失的普遍机制。然而,在WRN部分降解的条件下,添加低剂量ATR抑制剂显著提高了它们的综合疗效,达到接近WRN完全失活的水平。总的来说,我们的研究结果首次全面了解了将WRN的上游抑制与随后的细胞死亡联系起来的分子事件,并表明WRN和ATR的双重靶向可能是治疗MSI-H癌症的有用策略。
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Comprehensive mapping of cell fates in microsatellite unstable cancer cells supports dual targeting of WRN and ATR.

Addiction to the WRN helicase is a unique vulnerability of human cancers with high levels of microsatellite instability (MSI-H). However, while prolonged loss of WRN ultimately leads to cell death, little is known about how MSI-H cancers initially respond to acute loss of WRN-knowledge that would be helpful for informing clinical development of WRN targeting therapy, predicting possible resistance mechanisms, and identifying useful biomarkers of successful WRN inhibition. Here, we report the construction of an inducible ligand-mediated degradation system in which the stability of endogenous WRN protein can be rapidly and specifically tuned, enabling us to track the complete sequence of cellular events elicited by acute loss of WRN function. We found that WRN degradation leads to immediate accrual of DNA damage in a replication-dependent manner that curiously did not robustly engage checkpoint mechanisms to halt DNA synthesis. As a result, WRN-degraded MSI-H cancer cells accumulate DNA damage across multiple replicative cycles and undergo successive rounds of increasingly aberrant mitoses, ultimately triggering cell death. Of potential therapeutic importance, we found no evidence of any generalized mechanism by which MSI-H cancers could adapt to near-complete loss of WRN. However, under conditions of partial WRN degradation, addition of low-dose ATR inhibitor significantly increased their combined efficacy to levels approaching full inactivation of WRN. Overall, our results provide the first comprehensive view of molecular events linking upstream inhibition of WRN to subsequent cell death and suggest that dual targeting of WRN and ATR might be a useful strategy for treating MSI-H cancers.

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来源期刊
Genes & development
Genes & development 生物-发育生物学
CiteScore
17.50
自引率
1.90%
发文量
71
审稿时长
3-6 weeks
期刊介绍: Genes & Development is a research journal published in association with The Genetics Society. It publishes high-quality research papers in the areas of molecular biology, molecular genetics, and related fields. The journal features various research formats including Research papers, short Research Communications, and Resource/Methodology papers. Genes & Development has gained recognition and is considered as one of the Top Five Research Journals in the field of Molecular Biology and Genetics. It has an impressive Impact Factor of 12.89. The journal is ranked #2 among Developmental Biology research journals, #5 in Genetics and Heredity, and is among the Top 20 in Cell Biology (according to ISI Journal Citation Reports®, 2021).
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