AI Article Synopsis
- - The internal strain from ligands when they bind to target sites plays a key role in their binding strength, influencing how scientists look for new drug-like molecules.
- - Using X-ray co-crystal structures, researchers have improved methods for estimating bound ligand strain, resulting in lower calculated strain energies.
- - The study finds that strain energy varies with molecular size in a non-linear way and follows a specific distribution pattern, which can improve techniques in both conformational search and molecular design.
Article Abstract
The internal conformational strain incurred by ligands upon binding a target site has a critical impact on binding affinity, and expectations about the magnitude of ligand strain guide conformational search protocols. Estimates for bound ligand strain begin with modeled ligand atomic coordinates from X-ray co-crystal structures. By deriving low-energy conformational ensembles to fit X-ray diffraction data, calculated strain energies are substantially reduced compared with prior approaches. We show that the distribution of expected global strain energy values is dependent on molecular size in a superlinear manner. The distribution of strain energy follows a rectified normal distribution whose mean and variance are related to conformational complexity. The modeled strain distribution closely matches calculated strain values from experimental data comprising over 3000 protein-ligand complexes. The distributional model has direct implications for conformational search protocols as well as for directions in molecular design.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9923749 | PMC |
| http://dx.doi.org/10.1021/acs.jmedchem.2c01744 | DOI Listing |
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