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细菌生物合成基因簇编码抗癌哈特拉霉素类分子:广谱抗真菌和抗卵菌化合物 oocydin A 的生物发生。

Bacterial biosynthetic gene clusters encoding the anti-cancer haterumalide class of molecules: biogenesis of the broad spectrum antifungal and anti-oomycete compound, oocydin A.

机构信息

Department of Biochemistry, University of Cambridge, Tennis Court Road, Cambridge, CB2 1QW, United Kingdom.

出版信息

J Biol Chem. 2012 Nov 9;287(46):39125-38. doi: 10.1074/jbc.M112.401026. Epub 2012 Sep 24.

Abstract

Haterumalides are halogenated macrolides with strong antitumor properties, making them attractive targets for chemical synthesis. Unfortunately, current synthetic routes to these molecules are inefficient. The potent haterumalide, oocydin A, was previously identified from two plant-associated bacteria through its high bioactivity against plant pathogenic fungi and oomycetes. In this study, we describe oocydin A (ooc) biosynthetic gene clusters identified by genome sequencing, comparative genomics, and chemical analysis in four plant-associated enterobacteria of the Serratia and Dickeya genera. Disruption of the ooc gene cluster abolished oocydin A production and bioactivity against fungi and oomycetes. The ooc gene clusters span between 77 and 80 kb and encode five multimodular polyketide synthase (PKS) proteins, a hydroxymethylglutaryl-CoA synthase cassette and three flavin-dependent tailoring enzymes. The presence of two free-standing acyltransferase proteins classifies the oocydin A gene cluster within the growing family of trans-AT PKSs. The amino acid sequences and organization of the PKS domains are consistent with the chemical predictions and functional peculiarities associated with trans-acyltransferase PKS. Based on extensive in silico analysis of the gene cluster, we propose a biosynthetic model for the production of oocydin A and, by extension, for other members of the haterumalide family of halogenated macrolides exhibiting anti-cancer, anti-fungal, and other interesting biological properties.

摘要

海他拉霉素是具有强抗肿瘤活性的卤代大环内酯,这使它们成为化学合成的有吸引力的目标。不幸的是,目前这些分子的合成途径效率低下。强效海他拉霉素,即 oocydin A,先前从两种与植物相关的细菌中通过其对植物病原真菌和卵菌的高生物活性而被鉴定出来。在这项研究中,我们描述了通过基因组测序、比较基因组学和化学分析在四种与植物相关的肠杆菌属的沙雷氏菌属和迪基氏菌属中鉴定出的 oocydin A 生物合成基因簇。ooc 基因簇的破坏导致 oocydin A 的产生和对真菌和卵菌的生物活性丧失。ooc 基因簇跨越 77 到 80 kb,编码五个多模块聚酮合酶(PKS)蛋白、羟甲基戊二酰辅酶 A 合酶盒和三个黄素依赖性修饰酶。两个独立的酰基转移酶蛋白的存在将 oocydin A 基因簇归类为不断增长的跨酰基转移酶 PKS 家族内的基因簇。PKS 结构域的氨基酸序列和组织与与反式酰基转移酶 PKS 相关的化学预测和功能特殊性一致。基于对基因簇的广泛计算机分析,我们提出了 oocydin A 产生的生物合成模型,并且可以扩展到其他具有抗肿瘤、抗真菌和其他有趣生物特性的卤代大环内酯类海他拉霉素家族成员。

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