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Synergetic activation of CO2 by the DBU-organocatalyst and amine substrates towards stable carbamate salts for synthesis of oxazolidinones

机译:协同作用的激活的二氧化碳DBU-organocatalyst和胺基板稳定的氨基甲酸盐的合成oxazolidinones

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摘要

The development of an efficient methodology to transform CO2 into valuable chemicals has attracted increasing attention concerning the challenging issues of CO2-utilization. Herein, an efficient approach for the preparation of oxazolidinones from CO2, primary (aliphatic/aromatic) amines and 1,2-dichloroethane (or its derivatives) catalyzed by DBU organo-superbase was achieved with yields of 47-97% under mild conditions (80-100 degrees C, 12 h, 1.0 MPa CO2). Control experiments demonstrated that the formation of an ion-pair carbamate salt intermediate IS-B derived from the reaction of CO2, DBU (catalyst) and an amine (substrate) was the key step for this three-component reaction. The available DBU-amine-CO2 adduct intermediate (like IS-B-2) with fair stability will evolve into the thermodynamically stable product oxazolidinones upon attack of 1,2-dichloroethane (or its derivatives), along with the regeneration of the DBU catalyst. Alternatively, the decomposition of the DBU-aryl amine-CO2 adduct (like IS-B-1) with relatively poor stability also could result in the competitive substitution reaction of 1,2-dichloroethane (or its derivatives) with the aryl amine. This work provides insights into synergetic CO2-activation by the DBU-catalyst and a nucleophilic amine-substrate via the formation of robust carbamate salt intermediates responsible for the final production of oxazolidinones.
机译:发展的一个有效方法将二氧化碳转换成有价值的化学物质吸引了越来越多的关注有关CO2-utilization的具有挑战性的问题。有效的制备方法从二氧化碳oxazolidinones,初选(脂肪族或芳香族)胺1、二氯乙烷(或其衍生物)催化由DBU organo-superbase取得收益在温和条件下47 - 97%(80 - 100度12 C, h, 1.0 MPa二氧化碳)。证明了一个离子对的形成氨基甲酸盐的中间是b反应的二氧化碳,DBU(催化剂)和一个胺(底物)是关键的一步三分量的反应。DBU-amine-CO2加合物中间(如IS-B-2)将演变成与公平稳定热力学稳定的产品oxazolidinones1攻击后,二氯乙烷(或其衍生品),随着再生DBU催化剂。的DBU-aryl amine-CO2加合物(如IS-B-1)相对贫穷的稳定也可能导致的竞争取代反应1、二氯乙烷(或其衍生物)芳基胺。协同作用的CO2-activation DBU-catalyst和通过形成一个亲核amine-substrate强劲的氨基甲酸盐中间体负责最终产品oxazolidinones。

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