Identifying promising chemical starting points for small molecule inhibitors of active, GTP-loaded KRAS "on" remains of great importance to clinical oncology and represents a significant challenge in medicinal chemistry. Here, we describe broadly applicable learnings from a KRAS hit finding campaign: While we initially identified KRAS inhibitors in a biochemical high-throughput screen, we later discovered that compound potencies were all but assay artifacts linked to metal salts interfering with KRAS AlphaScreen assay technology. The source of the apparent biochemical KRAS inhibition was ultimately traced to unavoidable palladium impurities from chemical synthesis. This discovery led to the development of a Metal Ion Interference Set (MIIS) for up-front assay development and testing. Profiling of the MIIS across 74 assays revealed a reduced interference liability of label-free biophysical assays and, as a result, provided general estimates for luminescence- and fluorescence-based assay susceptibility to metal salt interference.
Chasing Red Herrings: Palladium Metal Salt Impurities Feigning KRAS Activity in Biochemical Assays.
追逐虚假信号:钯金属盐杂质在生化测定中伪装成 KRAS 活性
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作者:Gerstberger Thomas, Berger Helmut, Büttner Frank H, Gmachl Michael, Kessler Dirk, Koegl Manfred, Lucas Simon, Martin Laetitia J, Mayer Moriz, McConnell Darryl B, Mitzner Sophie, Scholz Guido, Treu Matthias, Wolkerstorfer Bernhard, Zahn Stephan, Zak Krzysztof M, Jaeger Philipp A, Ettmayer Peter
| 期刊: | Journal of Medicinal Chemistry | 影响因子: | 6.800 |
| 时间: | 2024 | 起止号: | 2024 Jul 25; 67(14):11701-11711 |
| doi: | 10.1021/acs.jmedchem.3c02381 | 研究方向: | 信号转导 |
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