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绘制具有生物学相关性的螺环化合物空间图。

Charting Biologically Relevant Spirocyclic Compound Space.

作者信息

Müller Gerhard, Berkenbosch Tim, Benningshof Jorg C J, Stumpfe Dagmar, Bajorath Jürgen

机构信息

Mercachem, Kerkenbos 1013, 6546 BB Nijmegen, P.O. Box 6747, 6503 GE, Nijmegen, The Netherlands.

Department of Life Science Informatics, B-IT, LIMES Program Unit Chemical Biology and Medicinal Chemistry, Rheinische Friedrich-Wilhelms-Universität, Dahlmannstr. 2, 53113, Bonn, Germany.

出版信息

Chemistry. 2017 Jan 12;23(3):703-710. doi: 10.1002/chem.201604714. Epub 2016 Dec 5.

Abstract

Spirocycles frequently occur in natural products and experience increasing interest in drug discovery, given their richness in sp centers and distinct three-dimensionality. We have systematically explored chemical space populated with currently available bioactive spirocycles. Compounds containing spiro systems were classified and their scaffolds and spirocyclic ring combinations analyzed. Nearly 47 000 compounds were identified that contained spirocycles in different structural contexts and were active against roughly 200 targets, among which several pharmaceutically relevant members of the G protein-coupled receptor (GPCR) family were identified. Spirocycles and corresponding compounds displayed notable scaffold diversity but contained only limited numbers of combinations of differently sized rings. These observations indicate that there should be significant potential to further expand spirocyclic chemical space for drug discovery, exploiting the privileged substructure concept. Inspired by those findings, we embarked on the design and chemical synthesis of three distinct novel spirocyclic scaffolds that qualify for downstream library synthesis, thus exploring principally new chemical space with high potential for pharmaceutical research.

摘要

螺环化合物在天然产物中频繁出现,并且鉴于其丰富的sp中心和独特的三维结构,在药物发现中受到越来越多的关注。我们系统地探索了当前可用的生物活性螺环化合物所占据的化学空间。对含有螺环系统的化合物进行了分类,并分析了它们的骨架和螺环环组合。鉴定出了近47000种化合物,这些化合物在不同的结构背景下含有螺环,并且对大约200种靶点具有活性,其中鉴定出了G蛋白偶联受体(GPCR)家族的几种与药物相关的成员。螺环化合物和相应的化合物显示出显著的骨架多样性,但不同大小环的组合数量有限。这些观察结果表明,利用特权子结构概念,进一步扩展用于药物发现的螺环化学空间具有巨大潜力。受这些发现的启发,我们着手设计和化学合成三种不同的新型螺环骨架,这些骨架有资格用于下游文库合成,从而主要探索具有高药物研究潜力的新化学空间。

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