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首页> 外文期刊>Bioorganic and medicinal chemistry >Novel DNA-directed alkylating agents: design, synthesis and potent antitumor effect of phenyl N-mustard-9-anilinoacridine conjugates via a carbamate or carbonate linker.
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Novel DNA-directed alkylating agents: design, synthesis and potent antitumor effect of phenyl N-mustard-9-anilinoacridine conjugates via a carbamate or carbonate linker.

机译:新型的DNA定向烷基化剂:通过氨基甲酸酯或碳酸盐连接基的苯基N-芥子9-苯胺基cr啶共轭物的设计,合成和有效的抗肿瘤作用。

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摘要

A series of phenyl N-mustard-9-anilinoacridine conjugates via a carbamate or carbonate linker was synthesized for antitumor evaluation. The carbamate or carbonate linker is able to lower the reactivity of the phenyl N-mustard pharmacophore and thus, these conjugates are rather chemically stable. The in vitro studies revealed that these derivatives possessed significant cytotoxicity with IC(50) in sub-micromolar range in inhibiting human lymphoblastic leukemia (CCRF-CEM), breast carcinoma (MX-1), colon carcinoma (HCT-116) and human non-small cell lung cancer (H1299) cell growth in vitro. Compounds 10a, 10b, 10e, 10i, and 15a were selected for evaluating their antitumor activity in nude mice bearing MX-1 and HCT-116 xenografts. Remarkably, total tumor remission was achieved by these agents with only one cycle of treatment. Interestingly, no tumor relapse was found in mice treated with 10a over 129 days. This agent is capable of inducing DNA interstrand cross-linking in human non-small lung cancer H1299 cells in a dose dependent manner by modified comet assay and has a long half-life in rat plasma.
机译:合成了一系列经由氨基甲酸酯或碳酸盐连接基的苯基N-芥子9-苯胺基cr啶共轭物,用于抗肿瘤评估。氨基甲酸酯或碳酸酯连接基能够降低苯基N-芥末药效基团的反应性,因此,这些结合物在化学上相当稳定。体外研究表明,这些衍生物在抑制人淋巴母细胞白血病(CCRF-CEM),乳腺癌(MX-1),结肠癌(HCT-116)和人非小细胞肺癌中具有亚微摩尔范围内的IC(50)的显着细胞毒性。 -小细胞肺癌(H1299)细胞的体外生长。选择化合物10a,10b,10e,10i和15a以评估其在携带MX-1和HCT-116异种移植物的裸鼠中的抗肿瘤活性。值得注意的是,仅用一个疗程,这些药物即可实现总的肿瘤缓解。有趣的是,在129天中用10a治疗的小鼠中未发现肿瘤复发。该试剂能够通过修饰的彗星试验以剂量依赖的方式诱导人非小肺癌H1299细胞中的DNA链交联,并且在大鼠血浆中具有长的半衰期。

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