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首页> 外文期刊>Nature Communications >Retro-biosynthetic screening of a modular pathway design achieves selective route for microbial synthesis of 4-methyl-pentanol
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Retro-biosynthetic screening of a modular pathway design achieves selective route for microbial synthesis of 4-methyl-pentanol

机译:逆向生物合成筛选的模块化途径设计实现了微生物合成4-甲基戊醇的选择性途径

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Increasingly complex metabolic pathways have been engineered by modifying natural pathways and establishing de novo pathways with enzymes from a variety of organisms. Here we apply retro-biosynthetic screening to a modular pathway design to identify a redox neutral, theoretically high yielding route to a branched C6 alcohol. Enzymes capable of converting natural E. coli metabolites into 4-methyl-pentanol ( 4MP ) via coenzyme A ( CoA )-dependent chemistry were taken from nine different organisms to form a ten-step de novo pathway. Selectivity for 4MP is enhanced through the use of key enzymes acting on acyl-CoA intermediates, a carboxylic acid reductase from Nocardia iowensis and an alcohol dehydrogenase from Leifsonia sp. strain S749. One implementation of the full pathway from glucose demonstrates selective carbon chain extension and acid reduction with 4MP constituting 81% (90±7?mg?l?1) of the observed alcohol products. The highest observed 4MP titre is 192±23?mg?l?1. These results demonstrate the ability of modular pathway screening to facilitate de novo pathway engineering.
机译:通过修饰天然途径并利用来自多种生物体的酶建立从头途径,已设计出越来越复杂的代谢途径。在这里,我们将逆向生物合成筛选应用于模块化途径设计,以鉴定氧化还原中性的,理论上高产的分支C6醇途径。从九种不同的生物体中提取能够通过辅酶A(CoA)依赖性化学将天然大肠杆菌代谢物转化为4-甲基戊醇(4MP)的酶,形成一条十步的从头途径。通过使用作用于酰基辅酶A中间体的关键酶,得自爱奥华氏诺卡氏菌的羧酸还原酶和得自Leifsonia sp。的醇脱氢酶,可以提高4MP的选择性。菌株S749。葡萄糖全路径的一种实现方法是选择性碳链延伸和酸还原,其中4MP占所观察到的醇产物的81%(90±7?mg?l ?1 )。观察到的最高4MP滴度为192±23?mg?l ?1 。这些结果证明了模块化途径筛选促进从头途径工程化的能力。

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