Scientific Publications

Identifying cellular targets of small-molecule probes and drugs with biochemical enrichment and SILAC.

Publication TypeJournal Article
AuthorsOng, SE, Li X., Schenone M., Schreiber SL, and Carr SA
AbstractSequencing of the human genome in the last decade has not yet led to a concomitant increase in the numbers of novel drug targets. While the pharmaceutical industry has invested heavily in improving drugs for existing protein targets, it has not tended toward a similar investment in experimental approaches to identify cellular targets of drugs. It is striking that the targets of numerous widely used FDA-approved drugs remain unknown. The development of robust, unbiased methods for target identification would greatly enhance our understanding the mechanisms-of-action of small molecules. Cell-based phenotypic screens followed by unbiased target identification have the potential to identify novel combinations of small molecules and their protein targets, shed light on drug polypharmacology, and enable unbiased screening approaches to drug discovery. Classical biochemical enrichment with immobilized small molecules has been used for over four decades but has been limited by issues concerning specificity and sensitivity. The application of mass spectrometry-based quantitative proteomics in combination with these affinity reagents has proven to be especially useful in addressing these common issues in affinity purification experiments. We describe the use of SILAC in identifying proteins that bind small-molecule probes and drugs in a cellular context.
Year of Publication2012
JournalMethods in molecular biology (Clifton, N.J.)
Volume803
Pages129-40
Date Published (YYYY/MM/DD)2012/01/09
ISSN Number1064-3745
DOI10.1007/978-1-61779-364-6_9
PubMedhttp://www.ncbi.nlm.nih.gov/pubmed/22065222?dopt=Abstract