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Influence of the Expression Level of O6-Alkylguanine-DNA Alkyltransferase on the Formation of DNA Interstrand Crosslinks Induced by Chloroethylnitrosoureas in Cells: A Quantitation Using High-Performance Liquid Chromatography-Mass Spectrometry

机译:O6-烷基鸟嘌呤-DNA烷基转移酶的表达水平对氯乙基亚硝基脲诱导细胞DNA链间交联形成的影响:高效液相色谱-质谱法定量

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摘要

Chloroethylnitrosoureas (CENUs), which are bifunctional alkylating agents widely used in the clinical treatment of cancer, exert anticancer activity by inducing crosslink within a guanine-cytosine DNA base pair. However, the formation of dG-dC crosslinks can be prevented by O6-alkylguanine-DNA alkyltransferase (AGT), ultimately leading to drug resistance. Therefore, the level of AGT expression is related to the formation of dG-dC crosslinks and the sensitivity of cells to CENUs. In this work, we determined the CENU-induced dG-dC crosslink in mouse L1210 leukemia cells and in human glioblastoma cells (SF-763, SF-767 and SF-126) containing different levels of AGT using high-performance liquid chromatography coupled with electrospray ionization tandem mass spectrometry. The results indicate that nimustine (ACNU) induced more dG-dC crosslinks in L1210 leukemia cells than those induced by carmustine (BCNU), lomustine (CCNU) and fotemustine (FTMS). This result was consistent with a previously reported cohort study, which demonstrated that ACNU had a better survival gain than BCNU, CCNU and FTMS for patients with high-grade glioma. Moreover, we compared the crosslinking levels and the cytotoxicity in SF-763, SF-767 and SF-126 cells with different AGT expression levels after exposure to ACNU. The levels of dG-dC crosslink in SF-126 cells (low AGT expression) were significantly higher than those in SF-767 (medium AGT expression) and SF-763 (high AGT expression) cells at each time point. Correspondingly, the cytotoxicity of SF-126 was the highest followed by SF-767 and SF-763. The results obtained in this work provided unequivocal evidence for drug resistance to CENUs induced by AGT-mediated repair of DNA ICLs. We postulate that the level of dG-dC crosslink has the potential to be employed as a biomarker for estimating drug resistance and anticancer efficiencies of novel CENU chemotherapies.
机译:氯乙基亚硝基脲(CENU)是广泛用于癌症临床治疗的双功能烷基化剂,可通过诱导鸟嘌呤-胞嘧啶DNA碱基对内的交联来发挥抗癌活性。然而,O 6 -烷基鸟嘌呤-DNA烷基转移酶(AGT)可以阻止dG-dC交联的形成,最终导致耐药性。因此,AGT表达水平与dG-dC交联的形成以及细胞对CENU的敏感性有关。在这项工作中,我们使用高效液相色谱与质谱联用,测定了包含不同水平AGT的小鼠L1210白血病细胞和人胶质母细胞瘤细胞(SF-763,SF-767和SF-126)中CENU诱导的dG-dC交联。电喷雾电离串联质谱。结果表明,尼莫斯汀(ACNU)在L1210白血病细胞中诱导的dG-dC交联比卡莫司汀(BCNU),洛莫斯汀(CCNU)和铁莫司汀(FTMS)诱导的交联更多。该结果与先前报道的一项队列研究一致,该研究表明,对于高度神经胶质瘤患者,ACNU的生存率优于BCNU,CCNU和FTMS。此外,我们比较了暴露于ACNU后具有不同AGT表达水平的SF-763,SF-767和SF-126细胞的交联水平和细胞毒性。在每个时间点,SF-126细胞(低AGT表达)中的dG-dC交联水平显着高于SF-767(中AGT表达)和SF-763(高AGT表达)细胞。相应地,SF-126的细胞毒性最高,其次是SF-767和SF-763。这项工作中获得的结果为AGT介导的DNA ICL修复诱导的对CENU的耐药性提供了明确的证据。我们假设dG-dC交联的水平有可能被用作生物标记物,以评估新型CENU化疗药物的耐药性和抗癌效率。

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