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通过选择性 4-甲基咪唑 N-布赫瓦尔德芳基化合成吡啶并吡嗪-1,6-二酮 γ-分泌酶调节剂。

Synthesis of Pyridopyrazine-1,6-dione γ-Secretase Modulators via Selective 4-Methylimidazole N-Buchwald Arylation.

机构信息

Pfizer Worldwide Research and Development , Eastern Point Road , Groton , Connecticut 06340 , United States.

Pfizer Worldwide Research and Development , 1 Portland Street , Cambridge , Massachusetts 02139 , United States.

出版信息

J Org Chem. 2019 Apr 19;84(8):4921-4925. doi: 10.1021/acs.joc.8b02953. Epub 2019 Jan 23.

Abstract

An efficient synthesis of pyridopyrazine-1,6-dione γ-secretase modulators (GSMs) is described. Our route features the construction of a crystalline lactone intermediate via a selective palladium-catalyzed 4-methylimidazole N-arylation using the Buchwald Xantphos Pd G4 precatalyst, which does not require a preactivation step. The weak inorganic base KHCO was employed to minimize saponification of a particularly sensitive lactone substrate. Additional key transformations include DABAL-Me-mediated lactone aminolysis and a mild TBD/ethyl trifluoroacetate mediated lactam ring closure to afford a representative GSM in high yield.

摘要

描述了一种高效合成吡啶并吡嗪-1,6-二酮γ-分泌酶调节剂(GSMs)的方法。我们的路线通过使用 Buchwald Xantphos Pd G4 前催化剂选择性钯催化 4-甲基咪唑 N-芳基化反应构建结晶内酯中间体,该反应不需要预激活步骤。使用弱无机碱 KHCO 来最小化特别敏感的内酯底物的皂化。其他关键转化包括 DABAL-Me 介导的内酯氨解和温和的 TBD/乙基三氟乙酸酯介导的内酰胺环闭合,以高产率得到代表性的 GSM。

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