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Treatment with inhibitors of polyamine biosynthesis which selectively lower intracellular spermine does not affect the activity of alkylating agents but antagonizes the cytotoxicity of DNA topoisomerase II inhibitors.

机译：用多胺生物合成抑制剂（选择性降低细胞内精胺）的处理不会影响烷基化剂的活性但会拮抗DNA拓扑异构酶II抑制剂的细胞毒性。

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Inhibitors of ornithine decarboxylase (ODC), such as alpha-difluoromethylornithine (DFMO), may influence the cytotoxicity of anti-tumour agents that interact with DNA. Intracellular levels of putrescine and spermidine were markedly reduced by ODC inhibitors while the level of spermine, which is the main polyamine in nuclei, was unchanged. By combining a novel inhibitor of ODC, such as (2R, 5R)-6-heptyne-2,5-diamine (MDL 72.175, MAP), with an inhibitor of S-adenosylmethionine decarboxylase (SAMDC), such as 5'-[[(Z)-4-aminobut-2-enyl]methylamino]-5'-deoxyadenosine (MDL 73.811, AbeAdo), spermine was selectively depleted in a human ovarian cancer cell line OVCAR-3 (i.e. spermine became almost undetectable whereas the levels of spermidine and putrescine were not affected). The depletion of spermine blocked DNA synthesis with a consequent accumulation of cells in the G1 phase of the cell cycle. Pretreatment with MAP plus AbeAdo did not change the cytotoxicity of alkylating agents, such as L-phenylalanine mustard (L-PAM), 1,4-bis(2'-chloroethyl)-1,4-diazabicyclo-[2.2.1] heptane diperchlorate (DABIS), 1,3-bis(2-chloroethyl)-1-nitrosourea (BCNU), cis-diamminedichloroplatinum (II) (cis-DDP), N-deformyl-N-[4-N-N,N-bis (2-chloroethylamino)benzoyl] (tallimustine) or CC-1065, whereas it markedly reduced the cytotoxicity of DNA topoisomerase II inhibitors, such as doxorubicin (DX) and 4'-demethylepipodophyllotoxin-5-(4,6-O)-ethylidene- beta-D-glycopyranoside (VP-16). The addition of spermine before drug treatment restored the sensitivity to the DNA topoisomerase II inhibitors, thus indicating that the reduced effect was related to the intracellular spermine level. The reason for the reduction in cytotoxicity is unclear, but it does not appear to be related to a cell cycle effect or to a decrease in the intracellular level of DNA topoisomerase II. Drugs that modify polyamine biosynthesis are under early clinical development as potential new anti-tumour agents. These findings illustrate the need for caution in combining such drugs with DNA topoisomerase II inhibitors.

机译：鸟氨酸脱羧酶（ODC）的抑制剂，例如α-二氟甲基鸟氨酸（DFMO），可能会影响与DNA相互作用的抗肿瘤剂的细胞毒性。 ODC抑制剂可显着降低细胞内腐胺和亚精胺的含量，而作为细胞核中主要多胺的精胺的含量则没有变化。通过将新型ODC抑制剂（例如（2R，5R）-6-庚炔2,5-二胺（MDL 72.175，MAP））与S-腺苷甲硫氨酸脱羧酶（SAMDC）抑制剂（例如5'-[ [（Z）-4-氨基丁-2-烯基甲基氨基] -5'-脱氧腺苷（MDL 73.811，AbeAdo），在人类卵巢癌细胞系OVCAR-3中选择性地消耗了精胺（即精胺几乎无法检测，而水平亚精胺和腐胺不受影响）。精胺的耗竭阻止了DNA的合成，从而导致细胞在细胞周期的G1期积累。 MAP加AbeAdo预处理不会改变烷基化剂的细胞毒性，例如L-苯丙氨酸芥末（L-PAM），1,4-双（2'-氯乙基）-1,4-二氮杂双环-[2.2.1]庚烷二氯二乙酸（DABIS），1,3-双（2-氯乙基）-1-亚硝基脲（BCNU），顺式二氨二氯铂（II）（顺式DDP），N-去甲酰基-N- [4-NN，N-bis（ 2-氯乙基氨基）苯甲酰基]]（tallimustine）或CC-1065，而它显着降低了DNA拓扑异构酶II抑制剂的细胞毒性，例如阿霉素（DX）和4'-去甲基表鬼臼毒素5-（4,6-O）-亚乙基- β-D-吡喃葡萄糖苷（VP-16）。药物治疗前添加精胺可恢复对DNA拓扑异构酶II抑制剂的敏感性，因此表明降低的作用与细胞内精胺水平有关。细胞毒性降低的原因尚不清楚，但似乎与细胞周期效应或DNA拓扑异构酶II的细胞内水平降低无关。修饰多胺生物合成的药物作为潜在的新抗肿瘤剂正在临床早期开发。这些发现说明将此类药物与DNA拓扑异构酶II抑制剂联合使用时需要谨慎。

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期刊名称 British Journal of Cancer
作者
M. A. Desiderio; D. Bergamaschi; E. Mascellani; P. De Feudis; E. Erba; M. DIncalci;
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作者单位

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年(卷),期 1997(75),7
年度 1997
页码 1028–1034
总页数 7
原文格式 PDF
正文语种
中图分类肿瘤学;
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专利

1. Treatment with inhibitors of polyamine biosynthesis, which selectively lower intracellular spermine, does not affect the activity of alkylating agents but antagonizes the cytotoxicity of DNA topoisomerase II inhibitors [J] . MA Desiderio, D Bergamaschi, E Mascellani, British Journal of Cancer . 1997,第7期

机译：用多胺生物合成抑制剂处理（选择性降低细胞内精胺）不会影响烷基化剂的活性，但会拮抗DNA拓扑异构酶II抑制剂的细胞毒性。
2. Antitumor agents. Part 230: C4'-esters of GL-331 as cytotoxic agents and DNA topoisomerase II inhibitors. [J] . Han S, Xiao Z, Bastow KF, Bioorganic and Medicinal Chemistry Letters . 2004,第11期

机译：抗肿瘤药。第230部分：GL-331的C4'-酯作为细胞毒剂和DNA拓扑异构酶II抑制剂。
3. Antitumor agents. Part 186: Synthesis and biological evaluation of demethylcolchiceinamide analogues as cytotoxic DNA topoisomerase II inhibitors. [J] . Guan J, Zhu XK, Tachibana Y, Bioorganic and medicinal chemistry . 1998,第11期

机译：抗肿瘤药。第186部分：作为细胞毒性DNA拓扑异构酶II抑制剂的去甲基colchiceinamide类似物的合成和生物学评估。
4. Part I. The synthesis and structure-activity relationship study of azo dye related HIV replication inhibitors. Part II. Plant isolation of signalling pathways inhibitors as anti-cancer agents. [D] . Lu, Hang. 1994

机译：第一部分：偶氮染料相关的HIV复制抑制剂的合成及其构效关系研究。第二部分植物分离的信号通路抑制剂为抗癌剂。
5. Exploring the activity of polyamine analogues on polyamine and spermine oxidase: methoctramine a potent and selective inhibitor of polyamine oxidase [O] . Maria Luisa Di Paolo, Manuela Cervelli, Paolo Mariottini, 2019

机译：探索多胺类似物对多胺和精胺氧化酶的活性：甲辛胺一种有效的多胺氧化酶的选择性抑制剂
6. Treatment with inhibitors of polyamine biosynthesis, which selectively lower intracellular spermine, does not affect the activity of alkylating agents but antagonizes the cytotoxicity of DNA topoisomerase II inhibitors. [O] . Desiderio, M. A., Bergamaschi, D., Mascellani, E., 1997

机译：用多胺生物合成抑制剂（选择性降低细胞内精胺）的处理不会影响烷基化剂的活性，但会拮抗DNA拓扑异构酶II抑制剂的细胞毒性。

Treatment with inhibitors of polyamine biosynthesis which selectively lower intracellular spermine does not affect the activity of alkylating agents but antagonizes the cytotoxicity of DNA topoisomerase II inhibitors.

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