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An L-threonine transaldolase is required for L-threo-β-hydroxy-α-amino acid assembly during obafluorin biosynthesis

机译:obafluorin生物合成过程中L-苏-β-羟基-α-氨基酸组装需要L-苏氨酸转醛酶

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摘要

β-Lactone natural products occur infrequently in nature but possess a variety of potent and valuable biological activities. They are commonly derived from β-hydroxy-α-amino acids, which are themselves valuable chiral building blocks for chemical synthesis and precursors to numerous important medicines. However, despite a number of excellent synthetic methods for their asymmetric synthesis, few effective enzymatic tools exist for their preparation. Here we report cloning of the biosynthetic gene cluster for the β-lactone antibiotic obafluorin and delineate its biosynthetic pathway. We identify a nonribosomal peptide synthetase with an unusual domain architecture and an L-threonine:4-nitrophenylacetaldehyde transaldolase responsible for (2S,3R)-2-amino-3-hydroxy-4-(4-nitrophenyl)butanoate biosynthesis. Phylogenetic analysis sheds light on the evolutionary origin of this rare enzyme family and identifies further gene clusters encoding L-threonine transaldolases. We also present preliminary data suggesting that L-threonine transaldolases might be useful for the preparation of L-threo-β-hydroxy-α-amino acids.
机译:β-内酯天然产物在自然界中很少出现,但具有多种有效而有价值的生物学活性。它们通常衍生自β-羟基-α-氨基酸,它们本身是用于化学合成的有价值的手性构建基块和许多重要药物的前体。然而,尽管有许多用于不对称合成的出色合成方法,但几乎没有有效的酶促工具可用于制备。在这里,我们报道了β-内酯类抗生素obafluorin的生物合成基因簇的克隆,并描述了其生物合成途径。我们确定非核糖体肽合成酶具有异常域结构和L-苏氨酸:4-硝基苯基乙醛反醛缩酶负责(2S,3R)-2-氨基-3-羟基-4-(4-硝基苯基)丁酸酯的生物合成。系统发生分析揭示了这种稀有酶家族的进化起源,并鉴定了编码L-苏氨酸反醛糖酶的其他基因簇。我们还提供了初步数据,表明L-苏氨酸反式糖核酸酶可能对制备L-苏氨酸-β-羟基-α-氨基酸有用。

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