Enantioselective synthesis of α-(3-pyrrolyl)methanamines with an aza-tetrasubstituted center under metal-free conditions.

IF 2.9 3区化学 Q1 CHEMISTRY, ORGANIC

Organic & Biomolecular Chemistry Pub Date : 2024-11-13 DOI:10.1039/d4ob01729c

Atul Jankiram Dolas, Jyothi Yadav, Yadav Kacharu Nagare, Krishnan Rangan, Eldhose Iype, Indresh Kumar

引用次数: 0

Abstract

Construction of a chiral methanamine unit at the C3 position of pyrrole is highly desirable; nevertheless, it remains challenging due to its intrinsic electronic properties. Herein, we present an operationally straightforward and direct asymmetric approach for accessing α-(3-pyrrolyl)methanamines under benign organocatalytic conditions for the first time. The one-pot transformation proceeds smoothly through an amine-catalyzed direct Mannich reaction of succinaldehyde with various endo-cyclic imines, followed by a Paal-Knorr cyclization with a primary amine. Several N-H/alkyl/Ar α-(3-pyrrolyl)methanamines with an aza-tetrasubstituted center have been synthesized with good yields and excellent enantioselectivity.

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在无金属条件下对带有氮杂四取代中心的 α-(3-吡咯基)甲胺进行对映选择性合成。

在吡咯的 C3 位置构建手性甲胺单元是非常理想的，然而，由于其固有的电子特性，这种方法仍然具有挑战性。在此，我们首次提出了一种在良性有机催化条件下获得α-(3-吡咯基)甲胺的操作简单、直接的不对称方法。琥珀醛与各种内环亚胺在胺催化下直接发生曼尼希反应，然后与伯胺发生帕尔-克诺尔环化反应，从而顺利进行一锅转化。我们合成了几种具有氮杂四取代中心的 N-H/烷基/Ar α-(3-吡咯基)甲胺，产量高，对映选择性好。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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