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基于异吲哚酮衍生物的抗癌化合物:提高选择性和效率的策略。

Anticancer Compounds Based on Isatin-Derivatives: Strategies to Ameliorate Selectivity and Efficiency.

作者信息

Ferraz de Paiva Raphael Enoque, Vieira Eduardo Guimarães, Rodrigues da Silva Daniel, Wegermann Camila Anchau, Costa Ferreira Ana Maria

机构信息

Departamento de Química Fundamental, Instituto de Química, Universidade de São Paulo, São Paulo, Brazil.

出版信息

Front Mol Biosci. 2021 Feb 4;7:627272. doi: 10.3389/fmolb.2020.627272. eCollection 2020.

Abstract

In this review we compare and discuss results of compounds already reported as anticancer agents based on isatin-derivatives, metalated as well as non-metallated. Isatin compounds can be obtained from plants, marine animals, and is also found in human fluids as a metabolite of amino acids. Its derivatives include imines, hydrazones, thiosemicarbazones, among others, already focused on numerous anticancer studies. Some of them have entered in pre-clinical and clinical tests as antiangiogenic compounds or inhibitors of crucial proteins. As free ligands or coordinated to metal ions, such isatin derivatives showed promising antiproliferative properties against different cancer cells, targeting different biomolecules or organelles. Binding to metal ions usually improves its biological properties, indicating a modulation by the metal and by the ligand in a synergistic process. They also reveal diverse mechanisms of action, being able of binding DNA, generating reactive species that cause oxidative damage, and inhibiting selected proteins. Strategies used to improve the efficiency and selectivity of these compounds comprise structural modification of the ligands, metalation with different ions, syntheses of mononuclear and dinuclear species, and use of inserted or anchored compounds in selected drug delivery systems.

摘要

在本综述中,我们比较并讨论了已报道的基于异吲哚酮衍生物(包括金属化和非金属化的)的抗癌剂的研究结果。异吲哚酮化合物可从植物、海洋动物中获得,并且在人体体液中作为氨基酸的代谢产物也有发现。其衍生物包括亚胺、腙、硫代氨基脲等,这些已被众多抗癌研究关注。其中一些已作为抗血管生成化合物或关键蛋白抑制剂进入临床前和临床试验阶段。作为游离配体或与金属离子配位时,此类异吲哚酮衍生物对不同癌细胞表现出有前景的抗增殖特性,靶向不同生物分子或细胞器。与金属离子结合通常会改善其生物学特性,表明在协同过程中金属和配体起到了调节作用。它们还揭示了多种作用机制,能够结合DNA、产生活性物质导致氧化损伤以及抑制特定蛋白质。用于提高这些化合物效率和选择性的策略包括配体的结构修饰、用不同离子进行金属化、单核和双核物种的合成以及在选定药物递送系统中使用插入或锚定化合物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3d39/7889591/e2c6acb0305c/fmolb-07-627272-g001.jpg

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