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Robust Strategy for Hit-to-Lead Discovery: NMR for SAR

J Med Chem. 2023-09; 
Sacha T Larda, Yann Ayotte, Maria M Denk, Paul Coote, Gregory Heffron, David Bendahan, Fatma Shahout, Nicolas Girard, Mustapha Iddir, Patricia Bouchard, Francois Bilodeau, Simon Woo, Luc J Farmer, Steven R LaPlante
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Plasmid DNA Preparation The codon-optimized sequences for HRasG12V (aa 1−166) and human SOS1 (SOScat, aa 564−1049) were prepared and cloned into the pET28a(+) plasmid at GenScript (https://www.genscript.com) Get A Quote

摘要

Establishing robust structure-activity relationships (SARs) is key to successful drug discovery campaigns, yet it often remains elusive due to screening and hit validation artifacts (false positives and false negatives), which frequently result in unproductive downstream expenditures of time and resources. To address this issue, we developed an integrative biophysics-driven strategy that expedites hit-to-lead discovery, mitigates false positives/negatives and common hit validation errors, and provides a robust approach to obtaining accurate binding and affinity measurements. The advantage of this method is that it vastly improves the clarity and reproducibility for affinity-driven SAR by monitoring and eliminat... More

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