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首页> 外文期刊>Angewandte Chemie >ZnCl2-Promoted Asymmetric Hydrogenation of beta-Secondary-Amino Ketones Catalyzed by a P-Chiral Rh-Bisphosphine Complex
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ZnCl2-Promoted Asymmetric Hydrogenation of beta-Secondary-Amino Ketones Catalyzed by a P-Chiral Rh-Bisphosphine Complex

机译:ZnCl 2促进的P-手性Rh-双膦配合物催化β-仲氨基酮的不对称加氢

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摘要

A new catalytic system has been developed for the asymmetric hydrogenation of beta-secondary-amino ketones using a highly efficient P-chiral bisphosphine-rhodium complex in combination with ZnCl2 as the activator of the catalyst. The chiral g-secondary-amino alcohols were obtained in 90-94% yields, 90-99% enantioselectivities, and with high turnover numbers (up to 2000 S/C; S/C-substrate/catalyst ratio). A mechanism for the promoting effect of ZnCl2 on the catalytic system has been proposed on the basis of NMR spectroscopy and HRMS studies. This method was successfully applied to the asymmetric syntheses of three important drugs, (S)-duloxetine, (R)-fluoxetine, and (R)-atomoxetine, in high yields and with excellent enantioselectivities.
机译:已经开发了一种新的催化系统,该系统使用高效的P-手性双膦-铑配合物与ZnCl2作为催化剂的活化剂,用于β-仲氨基酮的不对称加氢。以90-94%的收率,90-99%的对映选择性和高周转数(高达2000 S / C; S / C-底物/催化剂比)获得手性g-仲氨基醇。在NMR光谱学和HRMS研究的基础上,提出了ZnCl2对催化体系的促进作用的机理。该方法以高收率和优异的对映选择性成功地用于三种重要药物(S)-度洛西汀,(R)-氟西汀和(R)-atomoxetine的不对称合成。

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