Le Quement Sebastian T, Nielsen Thomas E, Meldal Morten
Carlsberg Laboratory, SPOCC Centre, Gamle Carlsberg Vej 10, DK-2500, Valby, Denmark.
J Comb Chem. 2007 Nov-Dec;9(6):1060-72. doi: 10.1021/cc700097k. Epub 2007 Nov 12.
The solid-phase synthesis of pharmacologically interesting heterocycles is presented. The formation of a series of (5,5)-, (5,6)-, (6,5)-, and (6,6)-fused bicyclic ring systems was systematically studied by implementation of a common strategy involving N-acyliminium intermediates. These are highly reactive and transformed further in intramolecular cascade reactions with strong as well as weak C, N, S, and O-nucleophiles. The methodology was successfully applied to the conversion of peptidomimetics into constrained small molecule core structures, such as the hexahydropyrrolo[2,1- b][1,3]oxazines, generally with full control of diastereoselectivity (>20:1) and in purities above 90%.
本文介绍了具有药理活性的杂环化合物的固相合成方法。通过实施一种涉及N-酰基亚胺离子中间体的通用策略,系统地研究了一系列(5,5)-、(5,6)-、(6,5)-和(6,6)-稠合双环体系的形成。这些中间体具有高反应活性,并在与强、弱碳、氮、硫和氧亲核试剂的分子内级联反应中进一步转化。该方法已成功应用于将拟肽转化为受限的小分子核心结构,如六氢吡咯并[2,1-b][1,3]恶嗪,通常能完全控制非对映选择性(>20:1),纯度高于90%。
