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A pyrimido16-abenzimidazole that enhances DNA cleavage mediated by eukaryotic topoisomerase II: a novel class of topoisomerase II-targeted drugs with cytotoxic potential.

机译：嘧啶并16-a苯并咪唑增强了由真核拓扑异构酶II介导的DNA切割：一种新型的靶向拓扑异构酶II的具有细胞毒性的药物。

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Recently, a number of novel quinolones with potent activity against topoisomerase II and eukaryotic cells have been described. Many of these compounds contain aromatic substituents in their C-7 ring positions. To determine whether pyrimido[1,6-a]benzimidazoles, a class of drugs modeled on quinolones, also display activity toward eukaryotic systems, the effects of Ro 46-7864 and Ro 47-3359 on Drosophila melanogaster topoisomerase II and Kc cells were characterized. While the former drug contains an aliphatic group (4-N-methylpiperazine) at the ring position equivalent to C-7 in quinolones, the latter compound contains an aromatic substituent (2,6-dimethylpyridine). Both pyrimido[1,6-a]benzimidazoles inhibited DNA relaxation catalyzed by the type II enzyme. However, only Ro 47-3359 enhanced topoisomerase II-mediated DNA cleavage and was toxic to Kc cells. At a concentration of 100 microM, this drug approximately doubled the levels of DNA breakage in vitro and killed > 50% of the initial cell population of cultures. These results strongly suggest that selected pyrimido[1,6-a]benzimidazoles may function as topoisomerase II-targeted drugs with cytotoxic potential.

机译：近来，已经描述了许多对拓扑异构酶II和真核细胞具有有效活性的新型喹诺酮。这些化合物中有许多在其C-7环位置含有芳族取代基。为了确定吡喹啉[1,6-a]苯并咪唑类药物是否对喹诺酮类药物也表现出活性，对Ro 46-7864和Ro 47-3359对果蝇果蝇拓扑异构酶II和Kc细胞的作用进行了表征。前一种药物在与喹诺酮类中的C-7等效的环位置上含有一个脂族基团（4-N-甲基哌嗪），而后一种化合物则含有一个芳族取代基（2,6-二甲基吡啶）。两种嘧啶并[1,6-a]苯并咪唑均抑制II型酶催化的DNA松弛。但是，只有Ro 47-3359增强了拓扑异构酶II介导的DNA裂解，并且对Kc细胞具有毒性。在100 microM的浓度下，该药物在体外的DNA破坏水平大约增加了一倍，并杀死了培养物中初始细胞群的50％以上。这些结果有力地表明，选定的嘧啶并[1,6-a]苯并咪唑类可能作为拓扑异构酶II靶向药物，具有细胞毒性。

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期刊名称 Antimicrobial Agents and Chemotherapy
作者
A H Corbett; P Guerry; P Pflieger; N Osheroff;
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作者单位

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年(卷),期 1993(37),12
年度 1993
页码 2599–2605
总页数 7
原文格式 PDF
正文语种
中图分类药学;微生物学;
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专利

1. Incomplete reversion of double stranded DNA cleavage mediated by Drosophila topoisomerase II: formation of single stranded DNA cleavage complex in the presence of an anti-tumor drug VM26 [J] . Maxwell P. Lee, Tao-shih Hsieh Nucleic acids research . 1992,第19期

机译：果蝇拓扑异构酶II介导的双链DNA裂解的不完全还原：在抗肿瘤药物VM26存在下形成单链DNA裂解复合物
2. Covalent attachment of ethidium to DNA results in enhanced topoisomerase II-mediated DNA cleavage [J] . Marx G, Zhou H, Graves DE, Biochemistry . 1997,第50期

机译：乙锭与DNA的共价结合导致拓扑异构酶II介导的DNA裂解增强
3. Coupling the core of the anticancer drug etoposide to an oligonucleotide induces topoisomerase II-mediated cleavage at specific DNA sequences [J] . Lara Lorena Infante, Fenner Sabine, Ratcliffe Steven, Nucleic Acids Research . 2018,第5期

机译：将抗癌药物的核苷酸偶联到寡核苷酸，诱导特定DNA序列的拓扑异构酶II介导的切割
4. DNA topoisomerases II: Evolution of their ATP bining site and design of new inhibitors [C] . L.Assairi Chinese peptide symposium . 1998

机译：DNA Topoisomerases II：其ATP啤酒网站的演变和新抑制剂的设计
5. Mechanistic studies of eukaryotic type II DNA topoisomerase and its interaction with topo II-targeting drugs. [D] . Hu, Tao. 2001

机译：真核II型DNA拓扑异构酶及其与topo II靶向药物相互作用的机理研究。
6. Drug features that contribute to the activity of quinolones against mammalian topoisomerase II and cultured cells: correlation between enhancement of enzyme-mediated DNA cleavage in vitro and cytotoxic potential. [O] . S H Elsea, P R McGuirk, T D Gootz, 1993

机译：有助于喹诺酮类抗哺乳动物拓扑异构酶II和培养细胞活性的药物特性：体外酶介导的DNA切割增强与细胞毒性潜力之间的相关性。
7. A pyrimido[1,6-a]benzimidazole that enhances DNA cleavage mediated by eukaryotic topoisomerase II: a novel class of topoisomerase II-targeted drugs with cytotoxic potential. [O] . Corbett, A H, Guerry, P, Pflieger, P, 1993

机译：嘧啶并[1,6-a]苯并咪唑增强了由真核拓扑异构酶II介导的DNA切割：一种新型的靶向拓扑异构酶II的具有细胞毒性的药物。
8. Short Communication: Enhancement of Topoisomerase I-Mediated Unwinding ofSupercoiled DNA by the Radioprotector WR-33278 [R] . Holwitt, E. A., Koda, E., Swenberg, C. E. 1990

机译：短沟通：放射防护剂WR-33278增强拓扑异构酶I介导的超螺旋DNa解旋

A pyrimido16-abenzimidazole that enhances DNA cleavage mediated by eukaryotic topoisomerase II: a novel class of topoisomerase II-targeted drugs with cytotoxic potential.

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