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首页> 外文期刊>Frontiers in Chemistry >A Brief Overview of Two Major Strategies in Diversity-Oriented Synthesis: Build/Couple/Pair and Ring-distortion
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A Brief Overview of Two Major Strategies in Diversity-Oriented Synthesis: Build/Couple/Pair and Ring-distortion

机译:面向多样性的综合中的两种主要策略的简要概述:构建/耦合/对和环失真

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摘要

In the interdisciplinary research field of chemical biology and drug discovery, diversity-oriented synthesis (DOS) has become indispensable in the construction of novel small-molecule libraries rich in skeletal and stereochemical diversity. DOS aims to populate the unexplored chemical space with new potential bioactive molecules via forward synthetic analysis. Since the introduction of this concept by Schreiber, DOS has evolved along with many significant breakthroughs. It is therefore important to understand the key DOS strategies to build molecular diversity with maximized biological relevancy. Due to the length limitations of this mini review, we briefly discuss the recent DOS plans using build/couple/pair (B/C/P) and ring-distortion strategies for the synthesis of major biologically relevant target molecules like natural products and their related compounds, macrocycles, and privileged structures.
机译:在化学生物学和药物发现的跨学科研究领域中,面向多样性的合成(DOS)在构建具有丰富骨架和立体化学多样性的新型小分子文库中已变得不可缺少。 DOS旨在通过正向合成分析,用新的潜在生物活性分子填充未开发的化学空间。自Schreiber引入此概念以来,DOS便取得了许多重大突破,并且不断发展。因此,重要的是要了解建立最大生物学相关性的分子多样性的关键DOS策略。由于这篇小型综述的篇幅所限,我们简要讨论了最近的DOS计划,该计划使用构建/耦合/对(B / C / P)和环畸变策略来合成主要的生物学相关靶标分子,例如天然产物及其相关化合物,大环化合物和特权结构。

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