Structural and functional dissection of aminocoumarin antibiotic biosynthesis: a review.

Journal of structural and functional genomics Pub Date : 2012-06-01 Epub Date: 2012-05-27 DOI:10.1007/s10969-012-9138-2

David M Lawson, Clare E M Stevenson

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引用次数: 6

Abstract

Aminocoumarin antibiotics are natural products of soil-dwelling bacteria called Streptomycetes. They are potent inhibitors of DNA gyrase, an essential bacterial enzyme and validated drug target, and thus have attracted considerable interest as potential templates for drug development. To date, aminocoumarins have not seen widespread clinical application on account of their poor pharmacological properties. Through studying the structures and mechanisms of enzymes from their biosynthetic pathways we will be better informed to redesign these compounds through rational pathway engineering. Novobiocin, the simplest compound, requires at least seventeen gene products to convert primary metabolites into the mature antibiotic. We have solved the crystal structures of four diverse biosynthetic enzymes from the novobiocin pathway, and used these as three-dimensional frameworks for the interpretation of functional and mechanistic data, and to speculate about how they might have evolved. The structure determinations have ranged from the routine to the challenging, necessitating a variety of different approaches.

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氨基香豆素抗生素生物合成的结构与功能解剖研究进展。

氨基香豆素抗生素是一种叫做链霉菌的土壤细菌的天然产物。它们是DNA回转酶的有效抑制剂，DNA回转酶是一种重要的细菌酶和经过验证的药物靶点，因此作为药物开发的潜在模板引起了相当大的兴趣。迄今为止，氨基香豆素还没有看到广泛的临床应用，由于其较差的药理性质。通过研究酶的生物合成途径的结构和机制，我们将更好地通过合理的途径工程来重新设计这些化合物。新生物素是最简单的化合物，它需要至少17种基因产物才能将初级代谢物转化为成熟的抗生素。我们已经从新生物素途径中解决了四种不同的生物合成酶的晶体结构，并将这些作为解释功能和机制数据的三维框架，并推测它们是如何进化的。结构的确定范围从常规到具有挑战性，需要各种不同的方法。

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Journal of structural and functional genomics

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