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Directed Metabolic Pathway Evolution Enables Functional Pterin-Dependent Aromatic-Amino-Acid Hydroxylation in Escherichia coli

机译:指导的代谢途径进化使得在大肠杆菌中具有功能性Pterin依赖性芳族氨基酸羟基化

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摘要

Tetrahydrobiopterin-dependent hydroxylation of aromatic amino adds is the first step in the biosynthesis of many neuroactive compounds in humans. A fundamental challenge in building these pathways in Escherichia colt is the provision of the non-native hydroxylase cofactor, tetrahydrobiopterin. To solve this, we designed a genetic selection that relies on the tyrosine synthesis activity of phenylalanine hydroxylase. Using adaptive laboratory evolution, we demonstrate the use of this selection to discover: (1) a minimum set of heterologous enzymes and a host folE (T1981) mutation for achieving this type of hydroxylation chemistry in whole cells, (2) functional complementation of tetrahydrobiopterin by indigenous cofactors, and (3) a tryptophan hydroxylase mutation for improving protein abundance. Thus, the goal of having functional aromatic-amino-acid hydroxylation in E. coli was achieved through directed metabolic pathway evolution.
机译:芳族氨基依赖性羟基化的芳族氨基添加剂是人类中许多神经活性化合物生物合成的第一步。 在大肠杆菌中建立这些途径的基本挑战是提供非天然羟化酶辅因子四氢萘啶蛋白。 为了解决这一点,我们设计了依赖于苯丙氨酸羟化酶的酪氨酸合成活性的遗传选择。 使用自适应实验室演化,我们证明了使用该选择来发现:(1)最小一组异源酶和宿主福(T1981)突变,用于在整个细胞中实现这种类型的羟基化化学,(2)四氢螺旋蛋白的功能互补 通过本土辅助因子,(3)用于改善蛋白质丰度的色氨酸羟化酶突变。 因此,通过指导的代谢途径进化实现了大肠杆菌中具有功能性芳族氨基酸羟基化的目的。

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