Epigenetic assays for chemical biology and drug discovery

Epigenetic assays for chemical biology and drug discovery

Abstract The implication of epigenetic abnormalities in many diseases and the approval of a number of compounds that modulate specific epigenetic targets in a therapeutically relevant manner in cancer specifically confirms that some of these targets are druggable by small molecules. Furthermore, a n...

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Main Author: Sheraz Gul
Format: Article
Language:English
Published: BMC 2017-04-01
Series:Clinical Epigenetics
Subjects:
Assay development
Bromodomain
Chemical biology
Chemical probe
Drug discovery
High throughput screening
Online Access:http://link.springer.com/article/10.1186/s13148-017-0342-6
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spelling doaj-70347528ebde44b7a61411846a9abf792020-11-25T00:30:20ZengBMCClinical Epigenetics1868-70751868-70832017-04-019111910.1186/s13148-017-0342-6Epigenetic assays for chemical biology and drug discoverySheraz Gul0Fraunhofer Institute for Molecular Biology and Applied Ecology - ScreeningPortAbstract The implication of epigenetic abnormalities in many diseases and the approval of a number of compounds that modulate specific epigenetic targets in a therapeutically relevant manner in cancer specifically confirms that some of these targets are druggable by small molecules. Furthermore, a number of compounds are currently in clinical trials for other diseases including cardiovascular, neurological and metabolic disorders. Despite these advances, the approved treatments for cancer only extend progression-free survival for a relatively short time and being associated with significant side effects. The current clinical trials involving the next generation of epigenetic drugs may address the disadvantages of the currently approved epigenetic drugs. The identification of chemical starting points of many drugs often makes use of screening in vitro assays against libraries of synthetic or natural products. These assays can be biochemical (using purified protein) or cell-based (using for example, genetically modified, cancer cell lines or primary cells) and performed in microtiter plates, thus enabling a large number of samples to be tested. A considerable number of such assays are available to monitor epigenetic target activity, and this review provides an overview of drug discovery and chemical biology and describes assays that monitor activities of histone deacetylase, lysine-specific demethylase, histone methyltransferase, histone acetyltransferase and bromodomain. It is of critical importance that an appropriate assay is developed and comprehensively validated for a given drug target prior to screening in order to improve the probability of the compound progressing in the drug discovery value chain.http://link.springer.com/article/10.1186/s13148-017-0342-6Assay developmentBromodomainChemical biologyChemical probeDrug discoveryHigh throughput screening
collection DOAJ
language English
format Article
sources DOAJ
author Sheraz Gul
spellingShingle Sheraz Gul
Epigenetic assays for chemical biology and drug discovery
Clinical Epigenetics
Assay development
Bromodomain
Chemical biology
Chemical probe
Drug discovery
High throughput screening
author_facet Sheraz Gul
author_sort Sheraz Gul
title Epigenetic assays for chemical biology and drug discovery
title_short Epigenetic assays for chemical biology and drug discovery
title_full Epigenetic assays for chemical biology and drug discovery
title_fullStr Epigenetic assays for chemical biology and drug discovery
title_full_unstemmed Epigenetic assays for chemical biology and drug discovery
title_sort epigenetic assays for chemical biology and drug discovery
publisher BMC
series Clinical Epigenetics
issn 1868-7075
1868-7083
publishDate 2017-04-01
description Abstract The implication of epigenetic abnormalities in many diseases and the approval of a number of compounds that modulate specific epigenetic targets in a therapeutically relevant manner in cancer specifically confirms that some of these targets are druggable by small molecules. Furthermore, a number of compounds are currently in clinical trials for other diseases including cardiovascular, neurological and metabolic disorders. Despite these advances, the approved treatments for cancer only extend progression-free survival for a relatively short time and being associated with significant side effects. The current clinical trials involving the next generation of epigenetic drugs may address the disadvantages of the currently approved epigenetic drugs. The identification of chemical starting points of many drugs often makes use of screening in vitro assays against libraries of synthetic or natural products. These assays can be biochemical (using purified protein) or cell-based (using for example, genetically modified, cancer cell lines or primary cells) and performed in microtiter plates, thus enabling a large number of samples to be tested. A considerable number of such assays are available to monitor epigenetic target activity, and this review provides an overview of drug discovery and chemical biology and describes assays that monitor activities of histone deacetylase, lysine-specific demethylase, histone methyltransferase, histone acetyltransferase and bromodomain. It is of critical importance that an appropriate assay is developed and comprehensively validated for a given drug target prior to screening in order to improve the probability of the compound progressing in the drug discovery value chain.
topic Assay development
Bromodomain
Chemical biology
Chemical probe
Drug discovery
High throughput screening
url http://link.springer.com/article/10.1186/s13148-017-0342-6
work_keys_str_mv AT sherazgul epigeneticassaysforchemicalbiologyanddrugdiscovery
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