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通过无金属六步多米诺反应,由两种简单化合物在一步操作中生成复杂氮杂双环和碳双环。

Generation of Complex Azabicycles and Carbobicycles from Two Simple Compounds in a Single Operation through a Metal-Free Six-Step Domino Reaction.

作者信息

Bock Christina M, Parameshwarappa Gangajji, Bönisch Simon, Neiss Christian, Bauer Walter, Hampel Frank, Görling Andreas, Tsogoeva Svetlana B

机构信息

Institute of Organic Chemistry and Interdisciplinary Center for Molecular Materials (ICMM), Friedrich-Alexander-Universität Erlangen-Nürnberg, Henkestrasse 42, 91054, Erlangen, Germany.

Chair of Theoretical Chemistry and Interdisciplinary Center for Molecular Materials (ICMM), Friedrich-Alexander-Universität Erlangen-Nürnberg, Egerlandstrasse 3, 91058, Erlangen, Germany.

出版信息

Chemistry. 2016 Apr 4;22(15):5189-97. doi: 10.1002/chem.201504798. Epub 2016 Feb 26.

Abstract

Aza- and carbobicyclic compounds possess favorable pharmaceutical properties, but they are difficult to access. Herein, we demonstrate an unprecedented organocatalytic two component six-step chemodivergent domino reaction, which provides a straightforward, sustainable and atom economical route to difficult-to-access complex bicyclic architectures: azabicycles and carbobicycles, whose ratios can be controlled by the applied electrophiles and catalysts. Detailed NMR and X-ray studies on the structures and relative stereochemistry of selected compounds are presented. Mechanistic investigations of the chemoselective branching step have been carried out with DFT methods in conjunction with semiempirical van der Waals interactions. This new domino reaction opens up a new vista of generating, in a single operation, new bioactive compounds with strong antiviral properties (EC50 up to 0.071 μM for human cytomegalovirus (HCMV)) outperforming clinically used ganciclovir (EC50 2.6 μM).

摘要

氮杂和碳双环化合物具有良好的药物性质,但难以合成。在此,我们展示了一种前所未有的有机催化两组分六步化学发散多米诺反应,该反应为难以合成的复杂双环结构:氮杂双环和碳双环提供了一条直接、可持续且原子经济的路线,其比例可通过所使用的亲电试剂和催化剂来控制。文中给出了对所选化合物的结构和相对立体化学的详细核磁共振和X射线研究。利用密度泛函理论方法结合半经验范德华相互作用对化学选择性分支步骤进行了机理研究。这种新的多米诺反应开辟了一个新的前景,即在一次操作中生成具有强抗病毒特性的新型生物活性化合物(对人巨细胞病毒(HCMV)的半数有效浓度(EC50)高达0.071 μM),其性能优于临床使用的更昔洛韦(EC50为2.6 μM)。

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