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埃斯帕霉素对DNA切割特异性的测定

Determination of DNA cleavage specificity by esperamicins.

作者信息

Lu M, Guo Q, Krishnan B, Golik J, Rosenberg I E, Doyle T W, Kallenbach N R

机构信息

Department of Chemistry, New York University, New York 10003.

出版信息

J Biomol Struct Dyn. 1991 Oct;9(2):285-98. doi: 10.1080/07391102.1991.10507913.

Abstract

The esperamicins are members of a class of potent antitumor antibiotics that contain stained diacetylenic ring systems capable of forming DNA-cleaving diradicals upon reaction with thiols. Here we show that the diacetylenic ring core itself determines the sequence specificity for scission of duplex DNA): esperamicin A1, and three products of hydrolysis of the glycon, esperamicins C, D, and E, are found to retain a common sequence preference. The sugar residues exert a strong influence on the cleavage efficiency, presumably by interacting nonspecifically with DNA. The presence of a branch in the DNA is found locally to inhibit scission by esperamicins, and this effect is shown to be due to the core also.

摘要

埃斯佩拉霉素是一类强效抗肿瘤抗生素,其含有经染色的二炔环系统,该系统在与硫醇反应时能够形成可切割DNA的双自由基。在此我们表明,二炔环核心本身决定了双链DNA断裂的序列特异性:埃斯佩拉霉素A1以及糖苷水解的三种产物,即埃斯佩拉霉素C、D和E,被发现保留了共同的序列偏好性。糖残基对切割效率有很大影响,推测是通过与DNA非特异性相互作用实现的。发现DNA中的一个分支会局部抑制埃斯佩拉霉素的切割作用,并且这种效应也被证明是由核心引起的。

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