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Structural and functional analysis of AsbF: Origin of the stealth 34-dihydroxybenzoic acid subunit for petrobactin biosynthesis

机译:AsbF的结构和功能分析:石蜡生物素合成的隐身34-二羟基苯甲酸亚基的起源

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摘要

Petrobactin, a virulence-associated siderophore produced by Bacillus anthracis, chelates ferric iron through the rare 3,4-isomer of dihydroxybenzoic acid (3,4-DHBA). Most catechol siderophores, including bacillibactin and enterobactin, use 2,3-DHBA as a biosynthetic subunit. Significantly, siderocalin, a factor involved in human innate immunity, sequesters ferric siderophores bearing the more typical 2,3-DHBA moiety, thereby impeding uptake of iron by the pathogenic bacterial cell. In contrast, the unusual 3,4-DHBA component of petrobactin renders the siderocalin system incapable of obstructing bacterial iron uptake. Although recent genetic and biochemical studies have revealed selected early steps in petrobactin biosynthesis, the origin of 3,4-DHBA as well as the function of the protein encoded by the final gene in the B. anthracis siderophore biosynthetic (asb) operon, asbF (BA1986), has remained unclear. In this study we demonstrate that 3,4-DHBA is produced through conversion of the common bacterial metabolite 3-dehydroshikimate (3-DHS) by AsbF—a 3-DHS dehydratase. Elucidation of the cocrystal structure of AsbF with 3,4-DHBA, in conjunction with a series of biochemical studies, supports a mechanism in which an enolate intermediate is formed through the action of this 3-DHS dehydratase metalloenzyme. Structural and functional parallels are evident between AsbF and other enzymes within the xylose isomerase TIM-barrel family. Overall, these data indicate that microbial species shown to possess homologs of AsbF may, like B. anthracis, also rely on production of the unique 3,4-DHBA metabolite to achieve full viability in the environment or virulence within the host.
机译:Petrobactin是一种由炭疽芽孢杆菌(Bacillus anthracis)产生的与毒力相关的铁载体,通过二羟基苯甲酸(3,4-DHBA)的稀有3,4-异构体螯合三价铁。大多数邻苯二酚铁载体,包括杆菌素和肠抑素,都使用2,3-DHBA作为生物合成亚基。值得注意的是,参与人类先天免疫的一个因素铁铁蛋白螯合带有更典型的2,3-DHBA部分的铁铁载体,从而阻碍病原细菌细胞摄取铁。相比之下,彼得罗布汀的3,4-DHBA异常成分使得铁铁蛋白系统无法阻碍细菌铁的吸收。尽管最近的遗传和生化研究已经揭示了石油链菌素生物合成中选择的早期步骤,但3,4-DHBA的起源以及炭疽芽孢杆菌铁载体生物合成(asb)操纵子asbF(由最终基因编码的蛋白质的功能)( BA1986),至今仍不清楚。在这项研究中,我们证明3,4-DHBA是由AsbF(一种3-DHS脱水酶)转化常见的细菌代谢物3-脱氢hydro草酸酯(3-DHS)产生的。与3,4-DHBA一起阐明AsbF的共晶体结构,结合一系列生化研究,支持了一种机制,其中通过该3-DHS脱水酶金属酶的作用形成了烯醇中间体。 AsbF和木糖异构酶TIM-桶家族中的其他酶之间存在结构和功能上的相似之处。总体而言,这些数据表明,显示出具有AsbF同系物的微生物可能像炭疽芽孢杆菌一样,也依赖于独特的3,4-DHBA代谢产物的产生来实现在环境中的完全生存力或宿主内的毒性。

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