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A Francisella virulence factor catalyses an essential reaction of biotin synthesis

机译:弗氏杆菌毒力因子催化生物素合成的重要反应

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We recently identified a gene (FTN_0818) required for Francisella virulence that seemed likely involved in biotin metabolism. However, the molecular function of this virulence determinant was unclear. Here we show that this protein named BioJ is the enzyme of the biotin biosynthesis pathway that determines the chain length of the biotin valeryl side-chain. Expression of bioJ allows growth of an Escherichia colibioH strain on biotin-free medium, indicating functional equivalence of BioJ to the paradigm pimeloyl-ACP methyl ester carboxyl-esterase, BioH. BioJ was purified to homogeneity, shown to be monomeric and capable of hydrolysis of its physiological substrate methyl pimeloyl-ACP to pimeloyl-ACP, the precursor required to begin formation of the fused heterocyclic rings of biotin. Phylogenetic analyses confirmed that distinct from BioH, BioJ represents a novel subclade of the α/β-hydrolase family. Structure-guided mapping combined with site-directed mutagenesis revealed that the BioJ catalytic triad consists of Ser151, Asp248 and His278, all of which are essential for activity and virulence. The biotin synthesis pathway was reconstituted reaction in vitro and the physiological role of BioJ directly assayed. To the best of our knowledge, these data represent further evidence linking biotin synthesis to bacterial virulence.
机译:我们最近鉴定了弗朗西斯菌毒力所需的基因(FTN_0818),该基因似乎可能与生物素代谢有关。但是,这种毒力决定因素的分子功能尚不清楚。在这里,我们证明了这种名为BioJ的蛋白质是生物素生物合成途径的酶,它决定了生物素戊酰基侧链的链长。 bioJ的表达允许大肠杆菌bioH菌株在无生物素的培养基上生长,表明BioJ与范例庚二酰-ACP甲酯羧基酯酶BioH的功能相当。 BioJ被纯化至均质,显示为单体,并能够将其生理底物甲基庚二酰-ACP水解为庚二酰-ACP,这是开始形成生物素稠合杂环所需的前体。系统发育分析证实,不同于BioH,BioJ代表了α/β-水解酶家族的一个新分支。结构指导的定位结合定点诱变显示,BioJ催化三联体由Ser151,Asp248和His278组成,所有这些对于活性和毒力都是必不可少的。生物素合成途径在体外重建反应并直接测定BioJ的生理作用。据我们所知,这些数据代表了将生物素合成与细菌毒力联系起来的进一步证据。

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