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首页> 外文期刊>Catalysis science & technology >Efficient asymmetric synthesis of chiral alcohols using high 2-propanol tolerance alcohol dehydrogenase SmADH2 via an environmentally friendly TBCR system
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Efficient asymmetric synthesis of chiral alcohols using high 2-propanol tolerance alcohol dehydrogenase SmADH2 via an environmentally friendly TBCR system

机译:有效的不对称合成手性醇使用高丙胺耐受酒精脱氢酶SmADH2通过一个环境友好的TBCR系统

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摘要

Alcohol dehydrogenases (ADHs) together with the economical substrate-coupled cofactor regeneration system play a pivotal role in the asymmetric synthesis of chiral alcohols; however, severe challenges concerning the poor tolerance of enzymes to 2-propanol and the adverse effects of the by-product, acetone, limit its applications, causing this strategy to lapse. Herein, a novel ADH gene smadh2 was identified from Stenotrophomonas maltophilia by traditional genome mining technology. The gene was cloned into Escherichia coli cells and then expressed to yield SmADH2. SmADH2 has a broad substrate spectrum and exhibits excellent tolerance and superb activity to 2-propanol even at 10.5 M (80%, v/v) concentration. Moreover, a new thermostatic bubble column reactor (TBCR) system is successfully designed to alleviate the inhibition of the by-product acetone by gas flow and continuously supplement 2-propanol. The organic waste can be simultaneously recovered for the purpose of green synthesis. In the sustainable system, structurally diverse chiral alcohols are synthesised at a high substrate loading (>150 g L-1) without adding external coenzymes. Among these, about 780 g L-1 (6 M) ethyl acetoacetate is completely converted into ethyl (R)-3-hydroxybutyrate in only 2.5 h with 99.9% ee and 7488 g L-1 d(-1) space-time yield. Molecular dynamics simulation results shed light on the high catalytic activity toward the substrate. Therefore, the high 2-propanol tolerance SmADH2 with the TBCR system proves to be a potent biocatalytic strategy for the synthesis of chiral alcohols on an industrial scale.
机译:乙醇脱氢酶(adh)一起经济substrate-coupled代数余子式再生系统中发挥关键作用不对称合成的手性醇;严峻的挑战有关贫穷的宽容的酶,丙胺和不利影响副产品,丙酮,限制其应用程序,使这一战略失误。在此,一种新的抗利尿激素基因smadh2被确认从Stenotrophomonas maltophilia传统基因组挖掘技术。成大肠杆菌细胞然后表示收益率SmADH2。优秀的宽容和频谱和展品丙胺的活动甚至在10.5米(80%, v / v)的浓度。鼓泡塔反应器恒温(TBCR)系统成功是为了缓解抑制副产物丙酮的气体流丙胺,不断补充。可以同时回收有机废物绿色合成的目的。可持续发展系统,结构不同的手性醇是合成在一个较高的衬底加载(> 150 g l - 1)在不增加外部辅酶。乙酰乙酸乙酯完全转化成乙(R) 3-hydroxybutyrate只有2.5 h99.9% ee和7488 g l - 1 d(1)时空产量。分子动力学模拟结果揭示高催化活性向衬底。宽容与TBCR系统SmADH2证明是一个强有力的biocatalytic战略合成手性醇工业规模。

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