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工程化改造细菌苯丙氨酸4-羟化酶用于微生物合成人类神经递质前体5-羟色氨酸。

Engineering bacterial phenylalanine 4-hydroxylase for microbial synthesis of human neurotransmitter precursor 5-hydroxytryptophan.

作者信息

Lin Yuheng, Sun Xinxiao, Yuan Qipeng, Yan Yajun

机构信息

College of Engineering, University of Georgia , Athens, Georgia 30602, United States.

出版信息

ACS Synth Biol. 2014 Jul 18;3(7):497-505. doi: 10.1021/sb5002505. Epub 2014 Jun 30.

Abstract

5-Hydroxytryptophan (5-HTP) is a drug that is clinically effective against depression, insomnia, obesity, chronic headaches, etc. It is only commercially produced by the extraction from the seeds of Griffonia simplicifolia because of a lack of synthetic methods. Here, we report the efficient microbial production of 5-HTP via combinatorial protein and metabolic engineering approaches. First, we reconstituted and screened prokaryotic phenylalanine 4-hydroxylase activity in Escherichia coli. Then, sequence- and structure-based protein engineering dramatically shifted its substrate preference, allowing for efficient conversion of tryptophan to 5-HTP. Importantly, E. coli endogenous tetrahydromonapterin (MH4) could be utilized as the coenzyme, when a foreign MH4 recycling mechanism was introduced. Whole-cell bioconversion allowed the high-level production of 5-HTP (1.1-1.2 g/L) from tryptophan in shake flasks. On this basis, metabolic engineering efforts were further made to achieve the de novo 5-HTP biosynthesis from glucose. This work not only holds great scale-up potential but also demonstrates a strategy for expanding the native metabolism of microorganisms.

摘要

5-羟色氨酸(5-HTP)是一种临床上对抑郁症、失眠、肥胖、慢性头痛等有效的药物。由于缺乏合成方法,它仅通过从西非凤凰木种子中提取进行商业生产。在此,我们报告了通过组合蛋白质和代谢工程方法高效微生物生产5-HTP的情况。首先,我们在大肠杆菌中重构并筛选了原核苯丙氨酸4-羟化酶活性。然后,基于序列和结构的蛋白质工程极大地改变了其底物偏好,使得色氨酸能够高效转化为5-HTP。重要的是,当引入外源四氢生物蝶呤(MH4)循环机制时,大肠杆菌内源性四氢生物蝶呤(MH4)可作为辅酶使用。全细胞生物转化使得摇瓶中能够从色氨酸高产5-HTP(1.1 - 1.2 g/L)。在此基础上,进一步开展代谢工程工作以实现从葡萄糖从头合成5-HTP。这项工作不仅具有巨大的扩大规模潜力,还展示了一种扩展微生物天然代谢的策略。

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