Sequence specificity, reactivity, and antitumor activity of DNA-alkylating pyrrole-imidazole diamides

被引:49
|
作者
Bando, T
Iida, H
Tao, ZF
Narita, A
Fukuda, N
Yamori, T
Sugiyama, H
机构
[1] Tokyo Med & Dent Univ, Inst Biomat & Bioengn, Div Biofunct Mol, Chiyoda Ku, Tokyo 1010062, Japan
[2] Nihon Univ, Sch Med, Dept Internal Med 2, Itabashi Ku, Tokyo 1738610, Japan
[3] Japanese Fdn Canc Res, Ctr Canc Chemotherapy, Div Mol Pharmacol, Toshima Ku, Tokyo 1708455, Japan
来源
CHEMISTRY & BIOLOGY | 2003年 / 10卷 / 08期
关键词
D O I
10.1016/S1074-5521(03)00160-1
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Three conjugates of imidazole (Im)-pyrrole (Py) diamide and a DNA-alkylating moiety derived from the antibiotic duocarmycin A were synthesized, and their sequence specificity, reactivity, and antitumor activity comparatively examined. Sequencing gel analysis indicated that ImPyDu (1) alkylates DNA at the 3' end of AT-rich sequences at micromolar concentration. ImPyDu86 (2) reacts with DNA at AT-rich sites together with dialkylation sites at micromolar concentration. ImPyLDu86 (3) efficiently alkylates dialkylation sites at nanomolar concentration. Average values of log IC50 against a 39 cancer cell line panel of 1-3 were - 4.59, -5.95, and -8.25, respectively. The differential growth inhibition pattern of 1-3 varied with relatively low correlation coefficients. Array-based gene expression monitoring was performed for 3 in a human lung cancer cell line. Substantial downregulation of expression was seen for genes involved in DNA damage response, transcription, and signal transduction.
引用
收藏
页码:751 / 758
页数:8
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