Recent Advances in the Design of RAR α and RAR β Agonists As Orally Bioavailable Drugs. A Review

Overview

Journal Bioorg Med Chem

Specialties Biochemistry
Chemistry

Date 2020 Oct 17

PMID 33069074

Citations 8

Authors

Alan D Borthwick

Maria B Goncalves

Jonathan P T Corcoran

Affiliations

Soon will be listed here.

Abstract

Retinoic acid receptors (RARs) α, β, and γ are members of the nuclear receptor superfamily. Compounds which bind to and activate the RARs are termed retinoids which regulate a wide variety of biological processes such as vertebrate embryonic morphogenesis and organogenesis, cell growth arrest, differentiation, and apoptosis, as well as their disorders. Although many synthetic selective RARα, RARβ, and RARγ agonists have been designed and prepared, these have generally been lipophilic acids without good drug-like properties and with low oral bioavailability. Recently this has been changing and drug design approaches to highly potent and selective RARα and RARβ agonists with low lipophilicity that are orally bioavailable and less toxic have been developed, that have a range of potential therapeutic uses. This review covers these new advances.

Citing Articles

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Corcoran J, Mey J Front Mol Neurosci. 2024; 17:1491745.

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C286, an orally available retinoic acid receptor β agonist drug, regulates multiple pathways to achieve spinal cord injury repair.

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Discovery of novel RARα agonists using pharmacophore-based virtual screening, molecular docking, and molecular dynamics simulation studies.

Ghorayshian A, Danesh M, Mostashari-Rad T, Fassihi A PLoS One. 2023; 18(8):e0289046.

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Revisiting APP secretases: an overview on the holistic effects of retinoic acid receptor stimulation in APP processing.

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