Abstract

BackgroundEnantiopure (S)-1-(4-methoxyphenyl) ethanol {(S)-MOPE} can be employed as an important synthon for the synthesis of cycloalkyl [b] indoles with the treatment function for general allergic response. To date, the biocatalytic resolution of racemic MOPE through asymmetric oxidation in the biphasic system has remained largely unexplored. Additionally, deep eutectic solvents (DESs), as a new class of promising green solvents, have recently gained increasing attention in biocatalysis for their excellent properties and many successful examples in biocatalytic processes. In this study, the biocatalytic asymmetric oxidation of MOPE to get (S)-MOPE using Acetobacter sp. CCTCC M209061 cells was investigated in different two-phase systems, and adding DES in a biphasic system was also explored to further improve the reaction efficiency of the biocatalytic oxidation.ResultsOf all the examined water-immiscible organic solvents and ionic liquids (ILs), 1-butyl-3-methylimidazolium hexafluorophoshpate ([C4MIM][PF6]) afforded the best results, and consequently was selected as the second phase of a two-phase system for the asymmetric oxidation of MOPE with immobilized Acetobacter sp. CCTCC M209061 cells. For the reaction performed in the [C4MIM][PF6]/buffer biphasic system, under the optimized conditions, the initial reaction rate, the maximum conversion and the residual substrate e.e. recorded 97.8 μmol/min, 50.5 and >99.9 % after 10 h reaction. Furthermore, adding the DES [ChCl][Gly] (10 %, v/v) to the aqueous phase, the efficiency of the biocatalytic oxidation was rose markedly. The optimal substrate concentration and the initial reaction rate were significantly increased to 80 mmol/L and 124.0 μmol/min, respectively, and the reaction time was shortened to 7 h with 51.3 % conversion. The immobilized cell still retained over 72 % of its initial activity after 9 batches of successive reuse in the [C4MIM][PF6]/[ChCl][Gly]-containing buffer system. Additionally, the efficient biocatalytic process was feasible up to a 500-mL preparative scale.ConclusionThe biocatalytic asymmetric oxidation of MOPE with Acetobacter sp. CCTCC M209061 cells was successfully conducted in the [C4MIM][PF6]-containing biphasic system with high conversion and enantioselectivity, and the reaction efficiency was further enhanced by adding [ChCl][Gly] to the reaction system. The efficient biocatalytic process was promising for the preparation of enantiopure (S)-MOPE.

Highlights

  • Enantiopure (S)-1-(4-methoxyphenyl) ethanol {(S)-MOPE} can be employed as an important synthon for the synthesis of cycloalkyl [b] indoles with the treatment function for general allergic response

  • A biphasic system consisted of organic solvent or hydrophobic ionic liquids (ILs) and buffer was conducted to improve the efficiency of the biocatalytic process

  • Many investigations have shown that the effects of different hydrophobic organic solvents and ILs on a biocatalytic reaction varied widely, and in many cases [26, 30, 31], the conversion/yield and the residual substrate or product e.e. would be enhanced significantly in the presence of the organic solvents or ILs compared to those in a aqueous monophasic phase

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Summary

Introduction

Enantiopure (S)-1-(4-methoxyphenyl) ethanol {(S)-MOPE} can be employed as an important synthon for the synthesis of cycloalkyl [b] indoles with the treatment function for general allergic response. The biocatalytic resolution of racemic MOPE through asymmetric oxidation in the biphasic system has remained largely unexplored. CCTCC M209061 cells was investigated in different two-phase systems, and adding DES in a biphasic system was explored to further improve the reaction efficiency of the biocatalytic oxidation. Enantiopure 1-(4-methoxyphenyl) ethanol (MOPE) is a key chiral building block. (S)-1-(4methoxyphenyl) ethanol {(S)-MOPE} can be employed for the synthesis of cycloalkyl [b] indoles which have the treatment function for general allergic response [3, 4]. Enantiopure chiral alcohols could be prepared mainly through chemical or biological approaches. Utilization of immobilized microbial cells can facilitate separation of product, and make biocatalysts recyclable, greatly simplifying the biocatalytic process and reducing the cost

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