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Advancements in screening technologies for small-molecule drug discovery including cellular assays, computational screening, and biophysics-based methods enhanced by structural biology breakthroughs have improved screeninghit rates and facilitated the identification of drug candidates for previously undruggable targets.
In terms of compound libraries, we have a high-throughput screening library of about 200,000 ligands. For fragmentscreening, which are much smaller compounds, we have a library of about 3000 fragments. We can screen with many different formats and modalities.
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