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Probing Small-Molecule Microarrays with Tagged Proteins in Cell Lysates

Author(s)
Pop, Marius S.; Wassaf, Dina; Koehler, Angela Nicole
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Abstract
The technique of small-molecule microarray (SMM) screening is based on the ability of small molecules to bind to various soluble proteins. This type of interaction is easily detected by the presence of a fluorescence signal produced by labeled antibodies that specifically recognize a unique sequence (tag) present on the target protein. The fluorescent signal intensity values are determined based on signal-to-noise ratios (SNRs). SMM screening is a high-throughput, unbiased method that can rapidly identify novel direct ligands for various protein targets. This binding-based assay format is generally applicable to most proteins, but it is especially useful for protein targets that do not possess an enzymatic activity. SMMs enable screening a protein in a purified form or in the context of a cellular lysate, likely providing a more physiologically relevant screening environment.
Date issued
2014-12
URI
http://hdl.handle.net/1721.1/101761
Department
Massachusetts Institute of Technology. Department of Biological Engineering; Koch Institute for Integrative Cancer Research at MIT
Journal
Current Protocols in Chemical Biology
Publisher
Wiley Blackwell
Citation
Pop, Marius S., Dina Wassaf, and Angela N. Koehler. “Probing Small-Molecule Microarrays with Tagged Proteins in Cell Lysates.” Current Protocols in Chemical Biology (October 15, 2009): 209–220.
Version: Author's final manuscript
ISSN
2160-4762

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