Pd-catalyzed asymmetric allylic alkylation of N-hydroxyphthalimide esters with allyl acetates†

Organic chemistry frontiers : an international journal of organic chemistry Pub Date : 2025-01-08 DOI:10.1039/d4qo02257b

Yixuan Zheng , Xinhao Deng , Fei Zhao , Yuanyuan Peng , Qiongjiao Yan , Wei Wang , Fener Chen , Hui Zhou

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Abstract

The palladium-catalyzed asymmetric allylic alkylation of carbon-based pronucleophiles is a highly efficient strategy for the synthesis of pharmaceutically relevant molecules. While significant progress has been made in the allylation of azlactones to access valuable α-amino acids, there remains a notable gap in catalytic asymmetric transformations regarding 2-alkyl-4-aryl-, 2,4-diaryl-, and 2,4-dialkyl-substituted azlactones. To address this challenge, we developed a palladium-catalyzed asymmetric allyl substitution of N-acyl phenylglycine N-hydroxyphthalimide esters with allyl acetates, featuring good yields, remarkable stereoselectivity, and a broad substrate scope. Furthermore, the allylated products can be readily derivatized into diverse polyfunctional compounds that have great potential for the exploitation of pharmaceuticals and biologically active molecules.

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pd催化n -羟基邻苯二胺酯与醋酸烯丙酯的不对称烯丙基烷基化反应

钯催化的碳基亲核试剂的不对称烯丙基烷基化是合成药物相关分子的高效和对映选择性策略。虽然氮唑内酯烯丙基化获得有价值的α-氨基酸方面取得了重大进展，但在催化不对称转化中涉及2-烷基-4-芳基-、2,4-二芳基-和2,4-二烷基取代氮唑内酯方面仍存在显著差距。为了解决这一挑战，我们开发了钯催化的n -酰基苯甘氨酸n -羟基邻苯亚胺酯与醋酸烯丙酯的不对称烯丙基取代，具有良好的产率，显著的立体选择性和广泛的底物范围。此外，该产品可以很容易地衍生成各种多功能化合物，这些化合物具有开发药物和生物活性分子的巨大潜力。

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来源期刊

Organic chemistry frontiers : an international journal of organic chemistry

CiteScore

7.80

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0.00%

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