Gilardini Montani Maria Saveria, Prodosmo Andrea, Stagni Venturina, Merli Dania, Monteonofrio Laura, Gatti Veronica, Gentileschi Maria Pia, Barilà Daniela, Soddu Silvia
Experimental Oncology, Regina Elena National Cancer Institute, Via Elio Chianesi, 53-00144 Rome, Italy.
J Exp Clin Cancer Res. 2013 Nov 19;32(1):95. doi: 10.1186/1756-9966-32-95.
Mutations in the DNA damage response (DDR) factors, breast cancer 1 (BRCA1) and BRCA2, sensitize tumor cells to poly(ADP-ribose) polymerase (PARP) inhibitors. The ataxia telangiectasia mutated (ATM) kinase is a key DDR protein whose heterozygous germline mutation is a moderate-risk factor for developing breast cancer. In this study, we examined whether ATM inactivation in breast cancer cell lines confers sensitivity to PARP inhibitors.
Wild-type BRCA1/2 breast cancer cells (i.e., MCF-7 and ZR-75-1 lines) were genetically manipulated to downregulate ATM expression then assayed for cytostaticity/cytotoxicity upon treatment with PARP inhibitors, olaparib and iniparib.
When ATM-depleted cells and their relative controls were treated with olaparib (a competitive PARP-1/2 inhibitor) and iniparib (a molecule originally described as a covalent PARP-1 inhibitor) a different response to the two compounds was observed. ATM-depletion sensitized both MCF-7 and ZR-75-1 cells to olaparib-treatment, as assessed by short and long survival assays and cell cycle profiles. In contrast, iniparib induced only a mild, ATM-dependent cytostatic effect in MCF-7 cells whereas ZR-75-1 cells were sensitive to this drug, independently of ATM inactivation. These latest results might be explained by recent observations indicating that iniparib acts with mechanisms other than PARP inhibition.
These data indicate that ATM-depletion can sensitize breast cancer cells to PARP inhibition, suggesting a potential in the treatment of breast cancers low in ATM protein expression/activity, such as those arising in mutant ATM heterozygous carriers.
DNA损伤反应(DDR)因子乳腺癌1(BRCA1)和BRCA2中的突变使肿瘤细胞对聚(ADP - 核糖)聚合酶(PARP)抑制剂敏感。共济失调毛细血管扩张症突变(ATM)激酶是一种关键的DDR蛋白,其杂合种系突变是患乳腺癌的中度风险因素。在本研究中,我们检测了乳腺癌细胞系中ATM失活是否会使其对PARP抑制剂敏感。
对野生型BRCA1/2乳腺癌细胞(即MCF - 7和ZR - 75 - 1细胞系)进行基因操作以下调ATM表达,然后在用PARP抑制剂奥拉帕利和英帕利布处理后检测细胞生长抑制/细胞毒性。
当用奥拉帕利(一种竞争性PARP - 1/2抑制剂)和英帕利布(一种最初被描述为共价PARP - 1抑制剂的分子)处理ATM缺失细胞及其相对对照时,观察到对这两种化合物的不同反应。通过短期和长期存活试验以及细胞周期分析评估,ATM缺失使MCF - 7和ZR - 75 - 1细胞对奥拉帕利治疗敏感。相比之下,英帕利布仅在MCF - 7细胞中诱导轻微的、依赖ATM的细胞生长抑制作用,而ZR - 75 - 1细胞对该药物敏感,与ATM失活无关。这些最新结果可能由最近的观察结果解释,即英帕利布的作用机制并非PARP抑制。
这些数据表明,ATM缺失可使乳腺癌细胞对PARP抑制敏感,这表明在治疗ATM蛋白表达/活性低的乳腺癌(如突变ATM杂合携带者中发生的乳腺癌)方面具有潜力。
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