This study investigated our Enzymelinks, COX-2-10aa-mPGES-1 and COX-2-10aa-PGIS, as cellular cross-screening targets for quick identification of lead compounds to inhibit inflammatory PGE biosynthesis while maintaining prostacyclin synthesis. We integrated virtual and wet cross-screening using Enzymelinks to rapidly identify lead compounds from a large compound library. From 380,000 compounds virtually cross-screened with the Enzymelinks, 1576 compounds were identified and used for wet cross-screening using HEK293 cells that overexpressed individual Enzymelinks as targets. The top 15 lead compounds that inhibited mPGES-1 activity were identified. The top compound that specifically inhibited inflammatory PGE biosynthesis alone without affecting COX-2 coupled to PGI synthase (PGIS) for PGI biosynthesis was obtained. Enzymelink technology could advance cyclooxygenase pathway-targeted drug discovery to a significant degree.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8204920 | PMC |
| http://dx.doi.org/10.4155/fmc-2021-0056 | DOI Listing |
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