Rapid discovery of drug target engagement by isothermal shift assay-Reference-Cited by-同舟云学术

Rapid discovery of drug target engagement by isothermal shift assay

Published:2019-03-28 Issue: Volume: Page:
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Author:

Webb Kristofor J.,Ball Kerri A.,Coleman Stephen J.,Jacobsen Jeremy,Stowell Michael H.B.^ORCID,Old William M.^ORCID

Abstract

Identifying protein targets directly bound by drug molecules within living systems remains challenging. Here we present the isothermal shift assay, iTSA, for rapid identification of drug targets. Compared with thermal proteome profiling, a prevailing method for target engagement, iTSA offers a simplified workflow, 4-fold higher throughput, and multiplexed experimental designs with higher replication. We demonstrate application of iTSA to identify targets for several kinase inhibitors in lysates and living cells.

Publisher

Cold Spring Harbor Laboratory

Reference33 articles.

1. Network pharmacology: the next paradigm in drug discovery

2. Non-kinase targets of protein kinase inhibitors;Nat. Rev. Drug Discov.,2017

3. Protein promiscuity and its implications for biotechnology

4. Polypharmacology – Foe or Friend?

5. Klaeger, S. et al. The target landscape of clinical kinase drugs. Science 358, (2017).

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