AI Article Synopsis
- The study focuses on developing aldosterone synthase inhibitors by enhancing a naphthalene scaffold with additional aromatic groups for better binding.
- Compounds 11 and 12 were designed, with compound 12 showing promising inhibitory activity (IC50 = 154 nM) due to its ability to target a new binding site.
- A total of 25 new compounds were synthesized, including highly potent inhibitors like compound 17 (IC50 = 2.7 nM), demonstrating selectivity for key steroidogenic enzymes.
Article Abstract
Pharmacophore modeling of a series of aldosterone synthase (CYP11B2) inhibitors triggered the design of compounds 11 and 12 by extending a previously established naphthalene molecular scaffold (e.g., present in molecules 1 and 2) via introduction of a phenyl or benzyl residue in 3-position. These additional aromatic moieties have been hypothesized to fit into the newly identified hydrophobic pharmacophore feature HY3. Subsequent docking studies in our refined CYP11B2 protein model have been performed prior to synthesis to estimate the inhibitory properties of the proposed molecules. While phenyl-substituted compound 11 (IC50 > 500 nM) did not dock under the given pharmacophore constraint (i.e., the Fe(heme)-N(ligand) interaction), benzyl-substituted compound 12 (IC50 = 154 nM) was found to exploit a previously unexplored subpocket of the inhibitor binding site. By structural optimization based on the pharmacophore hypothesis, 25 novel compounds were synthesized, among them highly potent CYP11B2 inhibitors (e.g., 17, IC50 = 2.7 nM) with pronounced selectivity toward the most important steroidogenic and hepatic CYP enzymes.
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| http://dx.doi.org/10.1021/jm800683c | DOI Listing |
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