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首页> 美国卫生研究院文献>International Journal of Oncology >Inhibition of poly(ADP-ribose) polymerase-1 or poly(ADP-ribose) glycohydrolase individually but not in combination leads to improved chemotherapeutic efficacy in HeLa cells
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Inhibition of poly(ADP-ribose) polymerase-1 or poly(ADP-ribose) glycohydrolase individually but not in combination leads to improved chemotherapeutic efficacy in HeLa cells

机译:单独(而非同时)抑制聚(ADP-核糖)聚合酶-1或聚(ADP-核糖)糖水解酶可提高HeLa细胞的化学治疗功效

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The genome-protecting role of poly(ADP-ribose) (PAR) has identified PAR polymerase-1 (PARP-1) and PAR glycohydrolase (PARG), two enzymes responsible for the synthesis and hydrolysis of PAR, as chemotherapeutic targets. Each has been previously individually evaluated in chemotherapy, but the effects of combination PARP-1 and PARG inhibition in cancer cells are not known. Here we determined the effects of the inhibition of PARP-1 and the absence or RNAi knockdown of PARG on PAR synthesis, cell death after chemotherapy and long-term viability. Using three experimental/clinical PARP-1 inhibitors in PARG-null cells, we show decreased levels of PAR and increased short-term and long-term viability with each inhibitor, with the exception of DPQ. Treatment with the experimental chemotherapeutic agent, N-methyl-N’-nitro-N-nitrosoguanidine (MNNG), led to increased cell death in PARG-null cells, but decreased cell death when pretreated with each PARP-1 inhibitor. Similar results were observed in MNNG-treated HeLa cells, where RNAi knockdown of PARG or pretreatment with ABT-888 led to increased HeLa cell death, whereas combination PARG RNAi knockdown + ABT-888 failed to produce increased cell death. The results demonstrate the ability of the PARP-1 inhibitors to decrease PAR levels, maintain viability and decrease PAR-mediated cell death after chemotherapeutic treatment in the absence of PARG. Further, the results demonstrate that the combination of PARP-1 and PARG inhibition in chemotherapy does not produce increased HeLa cell death. Thus, the results indicate that inhibiting both PARP-1 and PARG, which both are chemotherapeutic targets that increase cancer cell death, does not lead to synergistic cell death in HeLa cells. Therefore, strategies that target PAR metabolism for the improved treatment of cancer may be required to target PARP-1 and PARG individually in order to optimize cancer cell death.
机译:聚(ADP-核糖)(PAR)的基因组保护作用已确定PAR聚合酶-1(PARP-1)和PAR糖水解酶(PARG),这两种酶负责PAR的合成和水解,是化学治疗的靶标。每种药物先前均已在化疗中进行了单独评估,但未知PARP-1和PARG联合抑制在癌细胞中的作用。在这里,我们确定了PARP-1的抑制作用以及PARG的缺失或RNAi抑制对PAR合成,化疗后细胞死亡和长期生存力的影响。在PARG-null细胞中使用三种实验/临床PARP-1抑制剂,除DPQ以外,我们显示每种抑制剂的PAR水平降低,短期和长期生存能力增强。用实验性化学治疗剂N-甲基-N'-硝基-N-亚硝基胍(MNNG)处理可导致PARG空细胞的细胞死亡增加,但经每种PARP-1抑制剂预处理后细胞死亡减少。在MNNG处理的HeLa细胞中观察到了相似的结果,其中PARG的RNAi敲除或ABT-888预处理导致HeLa细胞死亡增加,而PARG RNAi的敲除+ ABT-888组合未能导致细胞死亡增加。结果表明,在不存在PARG的情况下,进行化学治疗后,PARP-1抑制剂具有降低PAR水平,维持活力和减少PAR介导的细胞死亡的能力。进一步地,结果表明在化学疗法中PARP-1和PARG抑制的组合不会产生增加的HeLa细胞死亡。因此,结果表明抑制PARP-1和PARG这两者都是增加癌细胞死亡的化学治疗靶标,不会导致HeLa细胞中的协同细胞死亡。因此,可能需要针对PAR代谢以改善癌症治疗的策略分别针对PARP-1和PARG,以优化癌细胞死亡。

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