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The Mandelate Pathway, an Alternative to the Phenylalanine Ammonia Lyase Pathway for the Synthesis of Benzenoids in Ascomycete Yeasts

机译:牙胶途径,是苯丙氨酸氨酶途径的替代方法,用于在Ascycete酵母中合成苯甲酸苯

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Benzenoid-derived metabolites act as precursors for a wide variety of products involved in essential metabolic roles in eukaryotic cells. They are synthesized in plants and some fungi through the phenylalanine ammonia lyase (PAL) and tyrosine ammonia lyase (TAL) pathways. Ascomycete yeasts and animals both lack the capacity for PAL/TAL pathways, and metabolic reactions leading to benzenoid synthesis in these organisms have remained incompletely known for decades. Here, we show genomic, transcriptomic, and metabolomic evidence that yeasts use a mandelate pathway to synthesize benzenoids, with some similarities to pathways used by bacteria. We conducted feeding experiments using a synthetic fermentation medium that contained either ~(13)C-phenylalanine or ~(13)C-tyrosine, and, using methylbenzoylphosphonate (MBP) to inhibit benzoylformate decarboxylase, we were able to accumulate intracellular intermediates in the yeast Hanseniaspora vineae . To further confirm this pathway, we tested in separate fermentation experiments three mutants with deletions in the key genes putatively proposed to form benzenoids ( Saccharomyces cerevisiae aro10 Δ, dld1 Δ, and dld 2Δ strains). Our results elucidate the mechanism of benzenoid synthesis in yeast through phenylpyruvate linked with the mandelate pathway to produce benzyl alcohol and 4-hydroxybenzaldehyde from the aromatic amino acids phenylalanine and tyrosine, as well as sugars. These results provide an explanation for the origin of the benzoquinone ring, 4-hydroxybenzoate, and suggest that Aro10p has benzoylformate and 4-hydroxybenzoylformate decarboxylase functions in yeast.IMPORTANCE We present here evidence of the existence of the mandelate pathway in yeast for the synthesis of benzenoids. The link between phenylpyruvate- and 4-hydroxyphenlypyruvate-derived compounds with the corresponding synthesis of benzaldehydes through benzoylformate decarboxylation is demonstrated. Hanseniaspora vineae was used in these studies because of its capacity to produce benzenoid derivatives at a level 2 orders of magnitude higher than that produced by Saccharomyces . Contrary to what was hypothesized, neither β-oxidation derivatives nor 4-coumaric acid is an intermediate in the synthesis of yeast benzenoids. Our results might offer an answer to the long-standing question of the origin of 4-hydroxybenzoate for the synthesis of Q10 in humans.
机译:苯突衍生的代谢物作为涉及真核细胞中基本代谢作用的各种产品的前体。它们通过苯丙氨酸氨裂解酶(PAL)和酪氨酸氨裂解酶(TAL)途径在植物和一些真菌中合成。 Ascomycete酵母和动物既缺乏适用于PAL / TAL途径的能力,并且在这些生物中导致苯骨合成的代谢反应仍然不完全众所周知。在这里,我们展示了酵母用牙出途径合成苯骨,与细菌使用的途径相似的基因组,转录组和代原证据。我们使用含有〜(13)C-苯丙氨酸或〜(13)C-酪氨酸的合成发酵培养基进行喂养实验,并使用甲基苯甲酰膦酸酯(MBP)来抑制苯甲酰胺酸脱羧酶,我们能够在酵母中积聚细胞内中间体Hanseniaspora Vineae。为了进一步证实该途径,我们在单独的发酵实验中测试了三个突变体,其缺失在旨在形成苯胞外(Saccharomyces CerevisiaeARO10δ,DLD1δ和DLD2δ菌株)中的关键基因中的缺失。我们的研究结果通过与施蛋白途径连接的苯吡啶替代物,阐明酵母合成的机制,从邦蛋白途径与芳族氨基酸苯丙氨酸和酪氨酸以及糖,以及糖。这些结果提供了苯醌环,4-羟基苯甲酸盐的起源的解释,并表明ARO10P在酵母中具有苯甲酰胺基和4-羟基苯甲酰胺脱羧酶功能.Importance我们在这里呈现酵母在酵母中存在的施手态途径的证据苯胞外。证实了通过苯甲酰胺脱羧与相应合成苯甲醛的苯吡啶磺酸盐和4-羟基苯丙烷衍生化合物的联系。在这些研究中使用Hanseniaspora Vineae,因为它的产能在2级的血栓衍生物的能力高于酿酒酵母产生的2级。与假设的相反,β-氧化衍生物和4-香豆酸是合成酵母苯甲酸的中间体。我们的结果可能会对4-羟基苯甲酸盐来源的长期问题提供答案,以便在人类中合成Q10。

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