Literature DB >> 31566060

High-Throughput Cellular Thermal Shift Assays in Research and Drug Discovery.

Mark J Henderson1, Marc A Holbert2, Anton Simeonov1, Lorena A Kallal3.   

Abstract

Thermal shift assays (TSAs) can reveal changes in protein structure, due to a resultant change in protein thermal stability. Since proteins are often stabilized upon binding of ligand molecules, these assays can provide a readout for protein target engagement. TSA has traditionally been applied using purified proteins and more recently has been extended to study target engagement in cellular environments with the emergence of cellular thermal shift assays (CETSAs). The utility of CETSA in confirming molecular interaction with targets in a more native context, and the desire to apply this technique more broadly, has fueled the emergence of higher-throughput techniques for CETSA (HT-CETSA). Recent studies have demonstrated that HT-CETSA can be performed in standard 96-, 384-, and 1536-well microtiter plate formats using methods such as beta-galactosidase and NanoLuciferase reporters and AlphaLISA assays. HT-CETSA methods can be used to select and characterize compounds from high-throughput screens and to prioritize compounds in lead optimization by facilitating dose-response experiments. In conjunction with cellular and biochemical activity assays for targets, HT-CETSA can be a valuable addition to the suite of assays available to characterize molecules of interest. Despite the successes in implementing HT-CETSA for a diverse set of targets, caveats and challenges must also be recognized to avoid overinterpretation of results. Here, we review the current landscape of HT-CETSA and discuss the methodologies, practical considerations, challenges, and applications of this approach in research and drug discovery. Additionally, a perspective on potential future directions for the technology is presented.

Entities:  

Keywords:  CETSA; cell-based assays; drug–target interaction; target engagement; thermal shift

Mesh:

Substances:

Year:  2019        PMID: 31566060     DOI: 10.1177/2472555219877183

Source DB:  PubMed          Journal:  SLAS Discov        ISSN: 2472-5552            Impact factor:   3.341


  8 in total

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Review 2.  An Overview of Cell-Based Assay Platforms for the Solute Carrier Family of Transporters.

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Journal:  Front Pharmacol       Date:  2021-08-10       Impact factor: 5.988

3.  Discovery and Structure-Activity Relationship Study of (Z)-5-Methylenethiazolidin-4-one Derivatives as Potent and Selective Pan-phosphatidylinositol 5-Phosphate 4-Kinase Inhibitors.

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Journal:  J Med Chem       Date:  2020-04-27       Impact factor: 7.446

Review 4.  Selective Modulation of Dynamic Protein Complexes.

Authors:  Julie M Garlick; Anna K Mapp
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7.  Real-Time Cellular Thermal Shift Assay to Monitor Target Engagement.

Authors:  Tino W Sanchez; Michael H Ronzetti; Ashley E Owens; Maria Antony; Ty Voss; Eric Wallgren; Daniel Talley; Krishna Balakrishnan; Sebastian E Leyes Porello; Ganesha Rai; Juan J Marugan; Samuel G Michael; Bolormaa Baljinnyam; Noel Southall; Anton Simeonov; Mark J Henderson
Journal:  ACS Chem Biol       Date:  2022-09-01       Impact factor: 4.634

Review 8.  Schistosomiasis Drug Discovery in the Era of Automation and Artificial Intelligence.

Authors:  José T Moreira-Filho; Arthur C Silva; Rafael F Dantas; Barbara F Gomes; Lauro R Souza Neto; Jose Brandao-Neto; Raymond J Owens; Nicholas Furnham; Bruno J Neves; Floriano P Silva-Junior; Carolina H Andrade
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  8 in total

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