Knaus Tanja, Corrado Maria L, Mutti Francesco G
Van't Hoff Institute for Molecular Sciences, HIMS-Biocat, University of Amsterdam, Science Park 904, 1098 XH Amsterdam, The Netherlands.
ACS Catal. 2022 Dec 2;12(23):14459-14475. doi: 10.1021/acscatal.2c03052. Epub 2022 Nov 10.
The efficient asymmetric catalytic synthesis of amines containing more than one stereogenic center is a current challenge. Here, we present a biocatalytic cascade that combines ene-reductases (EReds) with imine reductases/reductive aminases (IReds/RedAms) to enable the conversion of α,β-unsaturated ketones into primary, secondary, and tertiary amines containing two stereogenic centers in very high chemical purity (up to >99%), a diastereomeric ratio, and an enantiomeric ratio (up to >99.8:<0.2). Compared with previously reported strategies, our strategy could synthesize two, three, or even all four of the possible stereoisomers of the amine products while precluding the formation of side-products. Furthermore, ammonium or alkylammonium formate buffer could be used as the only additional reagent since it acted both as an amine donor and as a source of reducing equivalents. This was achieved through the implementation of an NADP-dependent formate dehydrogenase (FDH) for the in situ recycling of the NADPH coenzyme, thus leading to increased atom economy for this biocatalytic transformation. Finally, this dual-enzyme ERed/IRed cascade also exhibits a complementarity with the recently reported EneIRED enzymes for the synthesis of cyclic six-membered ring amines. The ERed/IRed method yielded trans-1,2 and cis-1,3 substituted cyclohexylamines in high optical purities, whereas the EneIRED method was reported to yield one cis-1,2 and one trans-1,3 enantiomer. As a proof of concept, when 3-methylcyclohex-2-en-1-one was converted into secondary and tertiary chiral amines with different amine donors, we could obtain all the four possible stereoisomer products. This result exemplifies the versatility of this method and its potential for future wider utilization in asymmetric synthesis by expanding the toolbox of currently available dehydrogenases via enzyme engineering and discovery.
高效不对称催化合成含有多个立体中心的胺类是当前面临的一项挑战。在此,我们展示了一种生物催化级联反应,该反应将烯还原酶(EReds)与亚胺还原酶/还原胺化酶(IReds/RedAms)相结合,能够将α,β-不饱和酮转化为化学纯度极高(高达>99%)、具有非对映体比例和对映体比例(高达>99.8:<0.2)的含有两个立体中心的伯胺、仲胺和叔胺。与先前报道的策略相比,我们的策略能够合成胺产物的两种、三种甚至所有四种可能的立体异构体,同时避免副产物的形成。此外,甲酸铵或烷基甲酸铵缓冲液可作为唯一的额外试剂,因为它既作为胺供体又作为还原当量的来源。这是通过实施一种依赖NADP的甲酸脱氢酶(FDH)实现NADPH辅酶的原位循环来达成的,从而提高了这种生物催化转化的原子经济性。最后,这种双酶ERed/IRed级联反应在合成环状六元环胺方面也与最近报道的EneIRED酶表现出互补性。ERed/IRed方法能以高光学纯度生成反式-1,2和顺式-1,3取代的环己胺,而据报道EneIRED方法能生成一种顺式-1,2和一种反式-1,3对映体。作为概念验证,当用不同的胺供体将3-甲基环己-2-烯-1-酮转化为仲胺和叔胺手性胺时,我们能够获得所有四种可能的立体异构体产物。这一结果例证了该方法的多功能性及其通过酶工程和发现扩展现有脱氢酶工具箱,从而在未来不对称合成中更广泛应用的潜力。
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