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从单次 Knoevenagel 缩合反应中能否获得所需构型的产物?异构化与立体定向合成。

Is It Possible to Obtain a Product of the Desired Configuration from a Single Knoevenagel Condensation? Isomerization vs. Stereodefined Synthesis.

机构信息

Laboratory of Molecular Pharmacology, St. Petersburg State Institute of Technology (Technical University), St. Petersburg 190013, Russia.

Crystallography Department, Institute of Earth Sciences, St. Petersburg State University, St. Petersburg 199034, Russia.

出版信息

Int J Mol Sci. 2023 Jul 12;24(14):11339. doi: 10.3390/ijms241411339.

Abstract

The biological activity of compounds directly depends on the three-dimensional arrangement of affinity fragments since a high degree of pharmacophore compliance with the binding site is required. 3-Benzylidene oxindoles are privileged structures due to their wide spectrum of biological activity, synthetic availability, and ease of modification. In particular, both kinase inhibitors and kinase activators can be found among 3-benzylidene oxindoles. In this work, we studied model compounds obtained via oxindole condensation with aldehydes and alkylphenones. These condensation products can exist in the form of - and -isomers and also undergo isomerization in solutions. The factors causing isomeric transformation of these compounds were established. Comparative kinetic studies to obtain quantitative characteristics of UV-driven isomerization were first performed. The results obtained indicate dramatic differences in two subclasses, which should be considered when developing biologically active molecules.

摘要

化合物的生物活性直接取决于亲和片段的三维排列,因为需要高度符合结合位点的药效团。3-亚苄基氧吲哚因其广泛的生物活性、合成可用性和易于修饰而成为优势结构。特别是,3-亚苄基氧吲哚中既有激酶抑制剂又有激酶激活剂。在这项工作中,我们研究了通过吲哚与醛和烷基苯酮缩合得到的模型化合物。这些缩合产物可以以 - 和 - 异构体的形式存在,并且也可以在溶液中发生异构化。确定了引起这些化合物异构转化的因素。首先进行了比较动力学研究,以获得 UV 驱动异构化的定量特征。所得结果表明在两个子类中存在显著差异,在开发具有生物活性的分子时应考虑这些差异。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b2e3/10379276/9b2f2193a2ea/ijms-24-11339-g001.jpg

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