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博来霉素:作用机制的新观点

Bleomycin: new perspectives on the mechanism of action.

作者信息

Hecht S M

机构信息

Departments of Chemistry and Biology, University of Virginia, Charlottesville, Virginia 22901, USA.

出版信息

J Nat Prod. 2000 Jan;63(1):158-68. doi: 10.1021/np990549f.

Abstract

The bleomycin group antitumor antibiotics have long been of interest as a consequence of their efficacy in the treatment of certain tumors, not to mention their unique structures and properties in mediating dioxygen activation and sequence selective degradation of DNA. At a chemical level, the structure originally assigned to bleomycin was subsequently reassigned and the new structure has been confirmed by total synthesis. Through the elaboration of structurally modified bleomycin congeners and fragments, synthetic efforts have also facilitated an understanding of the contribution of individual structural domains in bleomycin to sequence selective DNA binding and cleavage, and have also provided insights into the nature of the chemical processes by which DNA degradation takes place. Within the last several years, it has also become apparent that bleomycin can mediate the oxidative degradation of all major classes of cellular RNAs; it seems entirely plausible that RNA may also represent an important locus of action for this class of antitumor agent. In parallel with ongoing synthetic and mechanistic efforts using classical methods, the study of bleomycins attached to solid supports has been shown to provide important mechanistic insights, and the actual elaboration of modified bleomycins by solid phase synthesis constitutes a logical extension of such efforts.

摘要

博来霉素类抗肿瘤抗生素长期以来备受关注,这是因为它们在治疗某些肿瘤方面具有疗效,更不用说它们在介导双氧激活和DNA序列选择性降解方面具有独特的结构和性质。在化学层面上,最初赋予博来霉素的结构后来被重新确定,并且新结构已通过全合成得到证实。通过对结构修饰的博来霉素类似物和片段的精心研究,合成工作也有助于理解博来霉素中各个结构域对序列选择性DNA结合和切割的贡献,并且还为DNA降解发生的化学过程的本质提供了见解。在过去几年中,也已明显看出博来霉素可介导所有主要类别的细胞RNA的氧化降解;RNA似乎也完全有可能代表这类抗肿瘤剂的一个重要作用位点。与使用经典方法进行的正在进行的合成和机理研究并行,已表明对连接到固体支持物上的博来霉素的研究可提供重要的机理见解,并且通过固相合成实际精心制备修饰的博来霉素构成了此类工作的合理延伸。

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