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Asymmetric Cyanoethoxy Carbonylation Reaction of Aldehydes Catalyzed by a TiIV Macrocyclic Complex: An Efficient Synthetic Protocol for -Blocker and 1-Adrenergic Receptor Agonists

机译:通过TiIV宏环复合物催化的醛的不对称氰基乙氧基羰基化反应:用于-BlOcker和1-肾上腺素能受体激动剂的有效合成方案

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摘要

Chiral macrocyclic TiIV-salen complexes were used as efficient catalysts in the asymmetric cyanoethoxy carbonylation of aldehydes. The TiIV catalysts demonstrated excellent performance (product yields and ee values up to 99%) with ethyl cyanoformate as the cyanide source and a catalyst loading of 0.5mol%, which is the lowest known. The macrocyclic TiIV-salen complex retained its performance at multigram level and was conveniently recycled for a number of times. The product obtained was straightforwardly transformed to the pharmaceutically important chiral drugs (R)-proethalol (-blocker) and (R)-phenylephrine (1-adrenergic receptor agonist) in good yields. To understand the mechanism of the catalytic reaction, a kinetic investigation was conducted with various concentrations of the catalyst, ethyl cyanoformate and benzaldehyde as the representative substrate. The reaction of benzaldehyde was first order with respect to the concentration of the catalyst and the ethyl cyanoformate but did not depend on the initial concentration of the substrate. A possible mechanism of the cyano-ethoxy carbonylation reaction was proposed.
机译:在醛的不对称氰基乙氧基羰基化中使用手性宏环Tiiv-盐复合物作为高效催化剂。 TiIV催化剂具有优异的性能(产物产率和高达99%),用氰基甲酸乙酯作为氰化物源,催化剂负载量为0.5mol%,这是已知最低的。宏环Tiiv-Salen复合物在Multigram水平上保留了其性能,并且随时随地再循环了多次。将得到的产物直接转化为药学上重要的手性药物(R) - 丙醇(-L) - 苯甲肾上腺素(1-肾上腺素能受体激动剂),得到良好的产率。为了了解催化反应的机制,用各种浓度的催化剂,乙基乙烯类化合物和苯甲醛作为代表性基质进行动力学研究。苯甲醛的反应是相对于催化剂浓度和乙基乙酸乙基乙酸族浓度的第一阶,但不依赖于基材的初始浓度。提出了氰基乙氧基羰基化反应的可能机制。

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