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含吲哚/氮茚/色满骨架的小分子 ATP 竞争型激酶类药物的研发及结合模式分析。

Approved Small-Molecule ATP-Competitive Kinases Drugs Containing Indole/Azaindole/Oxindole Scaffolds: R&D and Binding Patterns Profiling.

机构信息

School of Pharmaceutical Sciences, Xiamen University, Xiamen 361102, China.

School of Medicine, Huaqiao University, Quanzhou 362021, China.

出版信息

Molecules. 2023 Jan 17;28(3):943. doi: 10.3390/molecules28030943.

Abstract

Kinases are among the most important families of biomolecules and play an essential role in the regulation of cell proliferation, apoptosis, metabolism, and other critical physiological processes. The dysregulation and gene mutation of kinases are linked to the occurrence and development of various human diseases, especially cancer. As a result, a growing number of small-molecule drugs based on kinase targets are being successfully developed and approved for the treatment of many diseases. The indole/azaindole/oxindole moieties are important key pharmacophores of many bioactive compounds and are generally used as excellent scaffolds for drug discovery in medicinal chemistry. To date, 30 ATP-competitive kinase inhibitors bearing the indole/azaindole/oxindole scaffold have been approved for the treatment of diseases. Herein, we summarize their research and development (R&D) process and describe their binding models to the ATP-binding sites of the target kinases. Moreover, we discuss the significant role of the indole/azaindole/oxindole skeletons in the interaction of their parent drug and target kinases, providing new medicinal chemistry inspiration and ideas for the subsequent development and optimization of kinase inhibitors.

摘要

激酶是最重要的生物分子家族之一,在调节细胞增殖、凋亡、代谢和其他关键生理过程中发挥着重要作用。激酶的失调和基因突变与各种人类疾病的发生和发展有关,特别是癌症。因此,越来越多的基于激酶靶点的小分子药物被成功开发并批准用于治疗许多疾病。吲哚/氮杂吲哚/氧化吲哚部分是许多生物活性化合物的重要药效团,通常被用作药物化学中药物发现的优秀支架。迄今为止,已有 30 种含有吲哚/氮杂吲哚/氧化吲哚支架的 ATP 竞争性激酶抑制剂被批准用于治疗疾病。本文总结了它们的研发(R&D)过程,并描述了它们与靶激酶的 ATP 结合位点的结合模式。此外,我们还讨论了吲哚/氮杂吲哚/氧化吲哚骨架在其母体药物与靶激酶相互作用中的重要作用,为后续激酶抑制剂的开发和优化提供了新的药物化学启示和思路。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/172f/9920796/b7e3480c46c7/molecules-28-00943-g001.jpg

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