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抗肿瘤抗生素新制癌菌素和博来霉素对DNA的序列特异性切割。

Sequence specific cleavage of DNA by the antitumor antibiotics neocarzinostatin and bleomycin.

作者信息

D'Andrea A D, Haseltine W A

出版信息

Proc Natl Acad Sci U S A. 1978 Aug;75(8):3608-12. doi: 10.1073/pnas.75.8.3608.

Abstract

We have investigated the sites of DNA damage by the antitumor antibiotics neocarzinostatin and bleomycin by using a 5'-end-labeled DNA fragment of defined sequence as a substrate. At the high drug concentrations used here, neocarzinostatin creates single-strand breaks in DNA at positions of adenine and thymine in the presence of 2-mercaptoethanol, and bleomycin cleaves DNA at GC and GT sequences and to a lesser extent at TA sequences with its degradative activity enhanced by 2-mercaptoethanol. In the presence of ferrous ions, bleomycin cleaves DNA at TT, AT, and TA, as well as at GC and GT sequences. Both antibiotics make double-strand breaks in DNA at specific sites and it is likely that these result from two independent single-strand breaks at nearby sites on opposite strands of the DNA.

摘要

我们使用一段特定序列的5'-末端标记DNA片段作为底物,研究了抗肿瘤抗生素新制癌菌素和博来霉素造成DNA损伤的位点。在此处使用的高药物浓度下,新制癌菌素在2-巯基乙醇存在时会在腺嘌呤和胸腺嘧啶位置造成DNA单链断裂,而博来霉素在GC和GT序列处切割DNA,在TA序列处切割程度较小,其降解活性会被2-巯基乙醇增强。在亚铁离子存在时,博来霉素在TT、AT和TA以及GC和GT序列处切割DNA。两种抗生素都会在DNA的特定位点造成双链断裂,这些双链断裂很可能是由DNA相反链上附近位点的两个独立单链断裂导致的。

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