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C1027生色团,一种强效的新型烯二炔类抗肿瘤抗生素,可诱导序列特异性双链DNA切割。

C1027 chromophore, a potent new enediyne antitumor antibiotic, induces sequence-specific double-strand DNA cleavage.

作者信息

Xu Y J, Zhen Y S, Goldberg I H

机构信息

Department of Biological Chemistry and Molecular Pharmacology, Harvard Medical School, Boston, Massachusetts 02115.

出版信息

Biochemistry. 1994 May 17;33(19):5947-54. doi: 10.1021/bi00185a036.

DOI:10.1021/bi00185a036
PMID:8180224
Abstract

C1027, a new macromolecular antitumor antibiotic produced by a Streptomyces strain, shows highly potent cytotoxicity to cultured cancer cells and marked DNA cleaving ability. The structure of its chromophore, responsible for most of the biological activities of the antibiotic, was recently determined and found to contain a nine-membered enediyne. In contrast to other enediyne antibiotics, such as neocarzinostatin, calicheamicin, esperamicin, and recently found kedarcidin, C1027 damages duplex DNA even in the absence of thiols. The DNA damage caused by C1027 includes double-strand breaks, single-strand breaks, and abasic sites. Experiments with plasmid DNA and 32P-end-labeled restriction fragments demonstrated that the chromophore, extracted from the protein-containing holoantibiotic, interacts in the DNA minor groove and cleaves double-helical DNA with a remarkable sequence-selectivity causing direct double-strand breaks. The double-strand cleavage sites, occurring predominantly at CTTTT/AAAAG, ATAAT/ATTAT, CTTTA/TAAAG, CTCTT/AAGAG, and especially GTTAT/ATAAC, consist of five nucleotide sequences with a two-nucleotide 3'-stagger of the cleaved residues (cutting sites are underlined). The chemical structures of the damaged residues at the GTTAT/ATAAC cleavage site suggest a model in which a C1027-induced double-strand break results from abstraction, by a single molecule of the diradical form of the chromophore, of a C4' hydrogen atom from the A residue of GTTAT and a C5' hydrogen atom from the A of ATAAC on the opposite strand. Single-strand breaks, which are mainly produced at adenylate and thymidylate residues, appear to be separate events presumably resulting from different binding modes of the drug to DNA.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

C1027是一种由链霉菌菌株产生的新型大分子抗肿瘤抗生素,对培养的癌细胞显示出高效的细胞毒性和显著的DNA切割能力。其发色团的结构负责抗生素的大部分生物活性,最近已被确定,发现其中含有一个九元烯二炔。与其他烯二炔抗生素,如新制癌菌素、刺孢霉素、埃斯帕霉素以及最近发现的克达霉素不同,C1027即使在没有硫醇的情况下也会损伤双链DNA。C1027引起的DNA损伤包括双链断裂、单链断裂和无碱基位点。用质粒DNA和32P末端标记的限制性片段进行的实验表明,从含蛋白质的全抗生素中提取的发色团在DNA小沟中相互作用,并以显著的序列选择性切割双螺旋DNA,导致直接双链断裂。双链切割位点主要出现在CTTTT/AAAAG、ATAAT/ATTAT、CTTTA/TAAAG、CTCTT/AAGAG,尤其是GTTAT/ATAAC处,由五个核苷酸序列组成,切割后的残基有两个核苷酸的3'交错(切割位点下划线)。GTTAT/ATAAC切割位点处受损残基的化学结构表明了一种模型,即C1027诱导的双链断裂是由发色团的单分子双自由基形式从GTTAT的A残基中提取一个C4'氢原子,并从相反链上的ATAAC的A中提取一个C5'氢原子所致。主要在腺苷酸和胸苷酸残基处产生的单链断裂似乎是独立事件,可能是由于药物与DNA的不同结合模式导致的。(摘要截短至250字)

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