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一种用于DNA拓扑异构酶和位点特异性重组酶的新型自杀底物。

A novel suicide substrate for DNA topoisomerases and site-specific recombinases.

作者信息

Burgin A B, Huizenga B N, Nash H A

机构信息

Laboratory of Molecular Biology, National Institute of Mental Health, Bethesda, MD 20892, USA.

出版信息

Nucleic Acids Res. 1995 Aug 11;23(15):2973-9. doi: 10.1093/nar/23.15.2973.

Abstract

DNA topoisomerases and DNA site-specific recombinases are biologically important enzymes involved in a diverse set of cellular processes. We show that replacement of a phosphodiester linkage by a 5'-bridging phosphorothioate linkage creates an efficient suicide substrate for calf thymus topoisomerase I and lambda integrase protein (Int). Although the bridging phosphorothioate linkage is cleaved by these enzymes, the 5'-sulfhydryl which is generated is not competent for subsequent ligation reactions. We use the irreversibility of Int-promoted cleavage to explore conditions and factors that contribute to various steps of lambda integrative recombination. The phosphorothioate substrates offer advantages over conventional suicide substrates, may be potent tools for inhibition of the relevant cellular enzymes and represent a unique tool for the study of many other phosphoryl transfer reactions.

摘要

DNA拓扑异构酶和DNA位点特异性重组酶是参与多种细胞过程的重要生物酶。我们发现,用5'-桥连硫代磷酸酯键取代磷酸二酯键可产生一种有效的小牛胸腺拓扑异构酶I和λ整合酶蛋白(Int)的自杀底物。尽管这些酶可切割桥连硫代磷酸酯键,但产生的5'-巯基不能进行后续的连接反应。我们利用Int促进的切割的不可逆性来探索有助于λ整合重组各个步骤的条件和因素。硫代磷酸酯底物比传统的自杀底物具有优势,可能是抑制相关细胞酶的有力工具,并且是研究许多其他磷酸转移反应的独特工具。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e087/307138/5d85e37d7ed4/nar00015-0183-a.jpg

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