首页> 外文期刊>Mutation Research: International Journal on Mutagenesis, Chromosome Breakage and Related Subjects >The DNA topoisomerase II catalytic inhibitor merbarone is genotoxic and induces endoreduplication.
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The DNA topoisomerase II catalytic inhibitor merbarone is genotoxic and induces endoreduplication.

机译:DNA拓扑异构酶II催化抑制剂Merbarone具有遗传毒性,并诱导内复制。

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In the last years a number of reports have shown that the so-called topoisomerase II (topo II) catalytic inhibitors are able to induce DNA and chromosome damage, an unexpected result taking into account that they do not stabilize topo II-DNA cleavable complexes, a feature of topo II poisons such as etoposide and amsacrine. Merbarone inhibits the catalytic activity of topo II by blocking DNA cleavage by the enzyme. While it was first reported that merbarone does not induce genotoxic effects in mammalian cells, this has been challenged by reports showing that the topo II inhibitor induces efficiently chromosome and DNA damage, and the question as to a possible behavior as a topo II poison has been put forward. Given these contradictory results, and the as yet incomplete knowledge of the molecular mechanism of action of merbarone, in the present study we have tried to further characterize the mechanism of action of merbarone on cell proliferation, cell cycle, as well as chromosome and DNA damage in cultured CHO cells. Merbarone was cytotoxic as well as genotoxic, inhibited topo II catalytic activity, and induced endoreduplication. We have also shown that merbarone-induced DNA damage depends upon ongoing DNA synthesis. Supporting this, inhibition of DNA synthesis causes reduction of DNA damage and increased cell survival.
机译:近年来,许多报告表明所谓的拓扑异构酶II(topo II)催化抑制剂能够诱导DNA和染色体损伤,这是出乎意料的结果,因为它们不能稳定topo II-DNA可裂解的复合物, topo II毒物的特征,如依托泊苷和氨苯磺酸。 Merbarone通过阻止酶切割DNA来抑制topo II的催化活性。尽管首次报道美宝龙不会在哺乳动物细胞中诱导遗传毒性作用,但有报道称topo II抑制剂能有效诱导染色体和DNA损伤,对此提出了挑战,关于topo II毒物的可能行为的问题一直存在。提出。鉴于这些矛盾的结果,以及对美宝龙的分子作用机理的认识尚不完全,在本研究中,我们试图进一步表征美宝龙对细胞增殖,细胞周期以及染色体和DNA损伤的作用机理。在培养的CHO细胞中。 Merbarone具有细胞毒性和遗传毒性,抑制了topo II的催化活性,并诱导了核内复制。我们还表明,美巴龙诱导的DNA损伤取决于正在进行的DNA合成。支持这一点的是,DNA合成的抑制导致DNA损伤的减少和细胞存活的增加。

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