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| Item Type: | Preprint |
|---|---|
| Title: | LiP-Quant, an automated chemoproteomic approach to identify drug targets in complex proteomes |
| Creators Name: | Piazza, I., Beaton, N., Bruderer, R., Knobloch, T., Barbisan, C., Siepe, I., Rinner, O., de Souza, N., Picotti, P. and Reiter, L. |
| Abstract: | Chemoproteomics is a key technology to characterize the mode of action of drugs, as it directly identifies the protein targets of bioactive compounds and aids in developing optimized small-molecule compounds. Current unbiased approaches cannot directly pinpoint the interaction surfaces between ligands and protein targets. To address his limitation we have developed a new drug target deconvolution approach based on limited proteolysis coupled with mass spectrometry that works across species including human cells (LiP-Quant). LiP-Quant features an automated data analysis pipeline and peptide-level resolution for the identification of any small-molecule binding sites, Here we demonstrate drug target identification by LiP-Quant across compound classes, including compounds targeting kinases and phosphatases. We demonstrate that LiP-Quant estimates the half maximal effective concentration (EC50) of compound binding sites in whole cell lysates. LiP-Quant identifies targets of both selective and promiscuous drugs and correctly discriminates drug binding to homologous proteins. We finally show that the LiP-Quant technology identifies targets of a novel research compound of biotechnological interest. |
| Source: | bioRxiv |
| Title of Book: | LiP-Quant, an automated chemoproteomic approach to identify drug targets in complex proteomes |
| Publisher: | Cold Spring Harbor Laboratory Press |
| Article Number: | 860072 |
| Date: | 1 December 2019 |
| Official Publication: | https://doi.org/10.1101/860072 |
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