ATR抑制诱导错配修复缺陷细胞的合成致死性,并增强免疫疗法。

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.351084.123
Mingchao Wang, Xiaojuan Ran, Wendy Leung, Ajinkya Kawale, Sneha Saxena, Jian Ouyang, Parasvi S Patel, Yuting Dong, Tao Yin, Jian Shu, Robert T Manguso, Li Lan, Xiao-Fan Wang, Michael S Lawrence, Lee Zou
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引用次数: 0

摘要

癌症细胞的错配修复(MMR)缺乏驱动突变,并为免疫疗法提供了有用的生物标志物。然而,许多MMR-d缺乏(MMR-d)肿瘤对免疫疗法没有反应,这突出了靶向MMR-d癌症细胞的替代方法的必要性。在此,我们发现抑制ATR激酶优先杀死MMR-d癌症细胞。从机制上讲,ATR抑制剂(ATRi)通过以复制和MUS81核酸酶依赖的方式诱导DNA损伤,对MMR-d细胞施加合成致死性。ATRi诱导的DNA损伤与MSH2和PCNA共定位,表明它是由复制过程中MMR蛋白识别的DNA结构引起的。在同基因小鼠模型中,ATRi有效地减少了MMR-d肿瘤的生长。有趣的是,ATRi的抗肿瘤作用部分是由于CD8+T细胞。在MMR-d细胞中,ATRi刺激细胞质中新生DNA片段的积累,激活cGAS介导的干扰素反应。ATRi和抗PD-1抗体的组合比单独的ATRi或抗PD-1更有效地减少MMR-d肿瘤的生长,显示出ATRi增强MMR-d瘤的免疫治疗的能力。因此,ATRi通过诱导合成致死性和增强抗肿瘤免疫来选择性靶向MMR-d肿瘤细胞,为补充和增强MMR缺乏指导的免疫疗法提供了一种有前途的策略。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
ATR inhibition induces synthetic lethality in mismatch repair-deficient cells and augments immunotherapy.

The mismatch repair (MMR) deficiency of cancer cells drives mutagenesis and offers a useful biomarker for immunotherapy. However, many MMR-deficient (MMR-d) tumors do not respond to immunotherapy, highlighting the need for alternative approaches to target MMR-d cancer cells. Here, we show that inhibition of the ATR kinase preferentially kills MMR-d cancer cells. Mechanistically, ATR inhibitor (ATRi) imposes synthetic lethality on MMR-d cells by inducing DNA damage in a replication- and MUS81 nuclease-dependent manner. The DNA damage induced by ATRi is colocalized with both MSH2 and PCNA, suggesting that it arises from DNA structures recognized by MMR proteins during replication. In syngeneic mouse models, ATRi effectively reduces the growth of MMR-d tumors. Interestingly, the antitumor effects of ATRi are partially due to CD8+ T cells. In MMR-d cells, ATRi stimulates the accumulation of nascent DNA fragments in the cytoplasm, activating the cGAS-mediated interferon response. The combination of ATRi and anti-PD-1 antibody reduces the growth of MMR-d tumors more efficiently than ATRi or anti-PD-1 alone, showing the ability of ATRi to augment the immunotherapy of MMR-d tumors. Thus, ATRi selectively targets MMR-d tumor cells by inducing synthetic lethality and enhancing antitumor immunity, providing a promising strategy to complement and augment MMR deficiency-guided immunotherapy.

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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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