Low PPP2R2A expression promotes sensitivity to CHK1 inhibition in high-grade serous ovarian cancer.

IF 12.4 1区医学 Q1 MEDICINE, RESEARCH & EXPERIMENTAL

Theranostics Pub Date : 2024-11-04 eCollection Date: 2024-01-01 DOI:10.7150/thno.96879

Zhaojun Qiu, Deepika Sigh, Yujie Liu, Chandra B Prasad, Nichalos Bean, Chunhong Yan, Zaibo Li, Xiaoli Zhang, Goutham Narla, Analisa DiFeo, Qi-En Wang, Junran Zhang

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引用次数: 0

Abstract

Rationale: High-grade serous ovarian cancer (HGSOC), the most lethal epithelial ovarian cancer subtype, faces persistent challenges despite advances in the therapeutic use of PARP inhibitors. Thus, innovative strategies are urgently needed to improve survival rates for this deadly disease. Checkpoint kinase 1 (CHK1) is pivotal in regulating cell survival during oncogene-induced replication stress (RS). While CHK1 inhibitors (CHK1i's) show promise as monotherapy for ovarian cancer, a crucial biomarker for effective stratification in clinical trials is lacking, hindering efficacy improvement and toxicity reduction. PP2A B55α, encoded by PPP2R2A, is a regulatory subunit of the serine/threonine protein phosphatase 2 (PP2A) that influences CHK1 sensitivity in non-small cell lung cancer (NSCLC). Given the complexity of PP2A B55α function in different types of cancer, here we sought to identify whether PPP2R2A deficiency enhances the sensitivity of HGSOC to CHK1 inhibition. Methods: To determine whether PPP2R2A deficiency affects the sensitivity of HGSOC to CHK1 inhibition, we treated PPP2R2A knockdown (KD) HGSOC cells or HGSOC cells with naturally low PPP2R2A expression with a CHK1 inhibitor, then assessed cell growth in in vitro and in vivo assays. Additionally, we investigated the mechanisms contributing to the increased RS and the enhanced sensitivity to the CHK1 inhibitor in PPP2R2A-KD or deficient cells using various molecular biology assays, including western blotting, immunofluorescence, and DNA fiber assays. Results: Our study suggests that PPP2R2A-KD elevates c-Myc-induced RS via upregulation of replication initiation, rendering HGSOC cells reliant on CHK1 for survival, including those resistant to PARP inhibitors. Conclusion: Combined, these results identify PPP2R2A/PP2A B55α as a potential predictive biomarker for CHK1i sensitivity in HGSOC, as well as suggesting it as a therapeutic target to overcome PARP resistance.

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PPP2R2A低表达促进高级别浆液性卵巢癌对CHK1抑制的敏感性。

理由：高级别浆液性卵巢癌（HGSOC）是最致命的上皮性卵巢癌亚型，尽管PARP抑制剂的治疗应用取得了进展，但仍面临着持续的挑战。因此，迫切需要创新战略来提高这一致命疾病的存活率。检查点激酶1 （CHK1）在癌基因诱导的复制应激（RS）期间调节细胞存活中起关键作用。虽然CHK1抑制剂（CHK1i’s）有望作为卵巢癌的单一疗法，但在临床试验中缺乏有效分层的关键生物标志物，阻碍了疗效的提高和毒性的降低。PP2A B55α由PPP2R2A编码，是丝氨酸/苏氨酸蛋白磷酸酶2 （PP2A）的一个调控亚基，影响非小细胞肺癌（NSCLC）中CHK1的敏感性。鉴于PP2A B55α在不同类型癌症中的功能复杂性，本研究旨在确定PPP2R2A缺乏是否会增强HGSOC对CHK1抑制的敏感性。方法：为了确定PPP2R2A缺乏是否会影响HGSOC对CHK1抑制的敏感性，我们用CHK1抑制剂处理PPP2R2A敲低（KD）的HGSOC细胞或PPP2R2A自然低表达的HGSOC细胞，然后通过体外和体内实验评估细胞生长情况。此外，我们研究了PPP2R2A-KD或缺陷细胞中RS增加和对CHK1抑制剂敏感性增强的机制，使用了各种分子生物学分析，包括western blotting、免疫荧光和DNA纤维分析。结果：我们的研究表明PPP2R2A-KD通过上调复制起始来升高c- myc诱导的RS，使HGSOC细胞依赖CHK1存活，包括那些对PARP抑制剂有抗性的细胞。结论：综合上述结果，PPP2R2A/PP2A B55α可作为HGSOC中CHK1i敏感性的潜在预测生物标志物，并提示其可作为克服PARP耐药的治疗靶点。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Theranostics MEDICINE, RESEARCH & EXPERIMENTAL-

CiteScore

25.40

自引率

1.60%

发文量

433

审稿时长

1 months

期刊介绍： Theranostics serves as a pivotal platform for the exchange of clinical and scientific insights within the diagnostic and therapeutic molecular and nanomedicine community, along with allied professions engaged in integrating molecular imaging and therapy. As a multidisciplinary journal, Theranostics showcases innovative research articles spanning fields such as in vitro diagnostics and prognostics, in vivo molecular imaging, molecular therapeutics, image-guided therapy, biosensor technology, nanobiosensors, bioelectronics, system biology, translational medicine, point-of-care applications, and personalized medicine. Encouraging a broad spectrum of biomedical research with potential theranostic applications, the journal rigorously peer-reviews primary research, alongside publishing reviews, news, and commentary that aim to bridge the gap between the laboratory, clinic, and biotechnology industries.