Proteomic tools to study drug function

Celine Mulder; Niels Leijten; Simone Lemeer

doi:10.1016/j.coisb.2018.05.002

Proteomic tools to study drug function

Celine Mulder, Niels Leijten, Simone Lemeer^*

^*Corresponding author for this work

Research output: Contribution to journal › Review article › peer-review

Abstract

With the ever growing repertoire of drugs being developed, new unbiased methods are urgently needed that allow fast screening of protein targets and off-targets. Ideally, these methods are capable of studying target engagement in a cellular context and provide a link between drug and cellular phenotype. Mass spectrometry based strategies provide an excellent way to study drug-target interactions as well as drug effects in a cellular context with excellent sensitivity and depth. In order to perform unbiased drug target screening several methods have been developed over the last years. In this review, we discuss affinity pull-down approaches to study direct drug-target interaction, methods which use alterations in protein stability as a measure for drug binding and the biological relevance of PTM enrichments to study the effect of inhibitors on cellular signalling.

Original language	English
Pages (from-to)	9-18
Number of pages	10
Journal	Current Opinion in Systems Biology
Volume	10
DOIs	https://doi.org/10.1016/j.coisb.2018.05.002
Publication status	Published - 1 Aug 2018

Funding

SL acknowledges support from the Netherlands Organization for Scientific Research (NWO) through a VIDI grant (project 723.013.008 ).

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10.1016/j.coisb.2018.05.002

ProteomicFinal published version, 1.47 MBLicence: Taverne

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title = "Proteomic tools to study drug function",

abstract = "With the ever growing repertoire of drugs being developed, new unbiased methods are urgently needed that allow fast screening of protein targets and off-targets. Ideally, these methods are capable of studying target engagement in a cellular context and provide a link between drug and cellular phenotype. Mass spectrometry based strategies provide an excellent way to study drug-target interactions as well as drug effects in a cellular context with excellent sensitivity and depth. In order to perform unbiased drug target screening several methods have been developed over the last years. In this review, we discuss affinity pull-down approaches to study direct drug-target interaction, methods which use alterations in protein stability as a measure for drug binding and the biological relevance of PTM enrichments to study the effect of inhibitors on cellular signalling.",

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AB - With the ever growing repertoire of drugs being developed, new unbiased methods are urgently needed that allow fast screening of protein targets and off-targets. Ideally, these methods are capable of studying target engagement in a cellular context and provide a link between drug and cellular phenotype. Mass spectrometry based strategies provide an excellent way to study drug-target interactions as well as drug effects in a cellular context with excellent sensitivity and depth. In order to perform unbiased drug target screening several methods have been developed over the last years. In this review, we discuss affinity pull-down approaches to study direct drug-target interaction, methods which use alterations in protein stability as a measure for drug binding and the biological relevance of PTM enrichments to study the effect of inhibitors on cellular signalling.

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JO - Current Opinion in Systems Biology

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Proteomic tools to study drug function

Abstract

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