ATR 抑制增加了对 PARP 介导的 DNA 修复的依赖,揭示了一种更好的宫颈癌治疗策略。

IF 4.5 2区 医学 Q1 OBSTETRICS & GYNECOLOGY
Sugantha Priya Elayapillai , Samrita Dogra , James Lausen , Madison Parker , Amy Kennedy , Doris M. Benbrook , Katherine M. Moxley , Bethany N. Hannafon
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引用次数: 0

摘要

目的:宫颈癌源于高危人类乳头瘤病毒(HR-HPV)的持续感染以及 E6 和 E7 肿瘤蛋白的表达。E6 和 E7 会损害 p53 和 Rb、G1-S 细胞周期检查点以及 ATM 介导的 DNA 损伤修复(DDR)的活性,进而增加 G2 细胞周期检查点对 ATR 和 PARP 介导的 DDR 的依赖。本研究旨在确定ATR抑制剂(ATRi,AZD6738)和PARP抑制剂(PARPi,AZD2281)对HR-HPV+宫颈癌细胞系的影响:方法:在体外评估 ATRi 和 PARPi 单独或联合使用对宫颈癌细胞株代谢活力、细胞周期停滞、细胞凋亡和 DDR 通路的影响,并使用异种移植模型评估体内肿瘤反应:结果:宫颈癌细胞对 ATRi 和 PARPi 单药治疗敏感。结果表明:宫颈癌细胞对 ATRi 和 PARPi 单药治疗均敏感,但由于 ATRi 介导的 PARP 表达上调,联合治疗在降低代谢活力方面只有先暴露于 ATRi 后暴露于 PARPi 的协同作用。ATRi 和 PARPi 联合使用可诱导 G2 细胞周期停滞和细胞凋亡。PARPi 可诱导 DNA 损伤和 γH2AX 磷酸化,而 ATRi 可进一步提高这种磷酸化。然而,PARPi诱导的Rad51病灶形成在ATRi处理后减少,这表明同源重组修复受到了抑制。ATRi能明显降低宫颈癌异种移植瘤的生长,在研究剂量下,ATRi不受同时PARPi治疗的影响:我们的研究结果表明,ATRi 增加了对 PARP 代谢活力的依赖,ATRi 和 PARPi 的联合应用在体外诱导了宫颈癌的合成致死率,并减少了体内的肿瘤负荷。
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 increases reliance on PARP-mediated DNA repair revealing an improved therapeutic strategy for cervical cancer

ATR inhibition increases reliance on PARP-mediated DNA repair revealing an improved therapeutic strategy for cervical cancer

Objective

Cervical cancer results from persistent infection with high-risk human papillomavirus (HR-HPV) and the expression of E6 and E7 oncoproteins. E6 and E7 compromise the activity of p53 and Rb, the G1-S cell cycle checkpoint, and ATM-mediated DNA damage repair (DDR), which in turn increases reliance on ATR- and PARP-mediated DDR at the G2 cell cycle checkpoint. This study aimed to determine the effects of an ATR inhibitor (ATRi, AZD6738) and a PARP-inhibitor (PARPi, AZD2281) on HR-HPV+ cervical cancer cell lines.

Methods

The effects of ATRi and PARPi, alone and in combination, on metabolic viability, cell cycle arrest, apoptosis, and DDR pathways in cervical cancer cell lines were evaluated in vitro, and the in vivo tumor response was evaluated using a xenograft model.

Results

Cervical cancer cells were sensitive to ATRi and PARPi monotherapy. The combination therapy was only synergistic in reducing metabolic viability when exposed to ATRi first, followed by PARPi, owing to ATRi-mediated upregulation of PARP expression. Combination of ATRi and PARPi induced G2 cell cycle arrest and apoptosis. PARPi induced DNA damage and γH2AX phosphorylation, which was further increased by ATRi treatment. However, PARPi-induced Rad51 foci formation was reduced by ATRi treatment, suggesting the inhibition of homologous recombination repair. ATRi significantly reduced cervical cancer xenograft tumor growth and was not affected by simultaneous PARPi treatment at the doses studied.

Conclusions

Our findings show that ATRi increased reliance on PARP for metabolic viability, the combination of ATRi and PARPi induced synthetic lethality in cervical cancer in vitro, and reduced tumor burden in vivo.
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来源期刊
Gynecologic oncology
Gynecologic oncology 医学-妇产科学
CiteScore
8.60
自引率
6.40%
发文量
1062
审稿时长
37 days
期刊介绍: Gynecologic Oncology, an international journal, is devoted to the publication of clinical and investigative articles that concern tumors of the female reproductive tract. Investigations relating to the etiology, diagnosis, and treatment of female cancers, as well as research from any of the disciplines related to this field of interest, are published. Research Areas Include: • Cell and molecular biology • Chemotherapy • Cytology • Endocrinology • Epidemiology • Genetics • Gynecologic surgery • Immunology • Pathology • Radiotherapy
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