Issue 9, 2024

Antineoplastic indole-containing compounds with potential VEGFR inhibitory properties

Abstract

Cancer is one of the most significant health challenges worldwide. Various techniques, tools and therapeutics/materials have been developed in the last few decades for the treatment of cancer, together with great interest, funding and efforts from the scientific society. However, all the reported studies and efforts seem insufficient to combat the various types of cancer, especially the advanced ones. The overexpression of tyrosine kinases is associated with cancer proliferation and/or metastasis. VEGF, an important category of tyrosine kinases, and its receptors (VEGFR) are hyper-activated in different cancers. Accordingly, they are known as important factors in the angiogenesis of different tumors and are considered in the development of effective therapeutic approaches for controlling many types of cancer. In this case, targeted therapeutic approaches are preferable to the traditional non-selective approaches to minimize the side effects and drawbacks associated with treatment. Several indole-containing compounds have been identified as effective agents against VEGFR. Herein, we present a summary of the recent indolyl analogs reported within the last decade (2012–2023) with potential antineoplastic and VEGFR inhibitory properties. The most important drugs, natural products, synthesized potent compounds and promising hits/leads are highlighted. Indoles functionalized and conjugated with various heterocycles beside spiroindoles are also considered.

Graphical abstract: Antineoplastic indole-containing compounds with potential VEGFR inhibitory properties

Supplementary files

Article information

Article type
Review Article
Submitted
31 Dec 2023
Accepted
29 Jan 2024
First published
14 Feb 2024
This article is Open Access
Creative Commons BY license

RSC Adv., 2024,14, 5690-5728

Antineoplastic indole-containing compounds with potential VEGFR inhibitory properties

D. R. Aboshouk, M. A. Youssef, M. S. Bekheit, A. R. Hamed and A. S. Girgis, RSC Adv., 2024, 14, 5690 DOI: 10.1039/D3RA08962B

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