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首页> 外文期刊>Microbial Biotechnology >Ustilago maydis produces itaconic acid via the unusual intermediate trans‐aconitate
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Ustilago maydis produces itaconic acid via the unusual intermediate trans‐aconitate

机译:乌斯地亚哥可能通过异常的中间反式衣康酸酯产生衣康酸

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SummaryItaconic acid is an important biomass-derived chemical building block but has also recently been identified as a metabolite produced in mammals, which has antimicrobial activity. The biosynthetic pathway of itaconic acid has been elucidated in the ascomycetous fungus Aspergillus terreus and in human macrophages. In both organisms itaconic acid is generated by decarboxylation of the tricarboxylic acid (TCA) cycle intermediate cis-aconitate. Here, we show that the basidiomycetous fungus Ustilago maydis uses an alternative pathway and produces itaconic acid via trans-aconitate, the thermodynamically favoured isomer of cis-aconitate. We have identified a gene cluster that contains all genes involved in itaconic acid formation. Trans-aconitate is generated from cis-aconitate by a cytosolic aconitate-Δ-isomerase (Adi1) that belongs to the PrpF family of proteins involved in bacterial propionate degradation. Decarboxylation of trans-aconitate is catalyzed by a novel enzyme, trans-aconitate decarboxylase (Tad1). Tad1 displays significant sequence similarity with bacterial 3-carboxy-cis,cis-muconate lactonizing enzymes (CMLE). This suggests that U. maydis has evolved an alternative biosynthetic pathway for itaconate production using the toxic intermediate trans-aconitate. Overexpression of a pathway-specific transcription factor (Ria1) or a mitochondrial tricarboxylic acid transporter (Mtt1) resulted in a twofold increase in itaconate yield. Therefore, our findings offer new strategies for biotechnological production of this valuable biomass-derived chemical.
机译:总结衣康酸是生物质衍生的重要化学组成部分,但最近也被确定为哺乳动物体内产生的代谢产物,具有抗菌活性。衣康酸真菌曲霉曲霉和人巨噬细胞已阐明了衣康酸的生物合成途径。在这两种生物中,衣康酸都是通过三羧酸(TCA)循环中间体顺式-阿魏酸酯的脱羧作用生成的。在这里,我们显示了担子菌真菌Ustilago maydis使用了一种替代途径,并通过反式-衣康酸酯(热力学上支持顺式-衣康酸酯的异构体)生产衣康酸。我们已经确定了一个基因簇,其中包含与衣康酸形成有关的所有基因。反式-aconitate是通过胞质乌头酸-Δ-异构酶(Adi1)从顺式-花生酸酯生成的,该酶属于参与细菌丙酸酯降解的PrpF蛋白家族。反式-烟酸酯的脱羧作用是由一种新型的酶,反式-烟酸酯脱羧酶(Tad1)催化的。 Tad1与细菌3-羧基-顺,粘液酸内酯化酶(CMLE)显示出显着的序列相似性。这表明梅氏酵母已经开发出使用毒性中间反式衣康酸酯的衣康酸酯生产的另一种生物合成途径。通路特异性转录因子(Ria1)或线粒体三羧酸转运蛋白(Mtt1)的过表达导致衣康酸酯收率提高两倍。因此,我们的发现为这种有价值的生物质衍生的化学品的生物技术生产提供了新的策略。

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