Sammenlign metoder
Gjennomgå de valgte metodene side om side; rader som avviker, er uthevet.
| Farmakofor-modellering× | Homologimodellering× | Molekylær docking× | |
|---|---|---|---|
| Fagfelt | Bioinformatikk | Bioinformatikk | Bioinformatikk |
| Familie | Process / pipeline | Process / pipeline | Process / pipeline |
| Opprinnelsesår≠ | 1977 | 1993 | 1982 |
| Opphavsperson≠ | Peter Gund | Andrej Sali | Irwin Kuntz |
| Type≠ | Pattern-based virtual screening pipeline | Comparative structure prediction pipeline | Binding prediction pipeline |
| Opprinnelig kilde≠ | Wermuth, C. G., Ganellin, C. R., Lindberg, P., & Mitscher, L. A. (1998). Glossary of terms used in medicinal chemistry. Pure and Applied Chemistry, 70(5), 1129-1143. DOI ↗ | Sali, A. & Blundell, T. L. (1993). Comparative protein modelling by satisfaction of spatial restraints. Journal of Molecular Biology, 234(3), 779-815. DOI ↗ | Kuntz, I. D., Blaney, J. M., Oatley, S. J., Langridge, R., & Ferrin, T. E. (1982). A geometric approach to macromolecule-ligand interactions. Journal of Molecular Biology, 161(2), 269-288. DOI ↗ |
| Alias | pharmacophore pattern recognition, 3D pharmacophore | comparative modeling, template-based modeling | protein-ligand docking, binding prediction |
| Relaterte≠ | 3 | 4 | 4 |
| Sammendrag≠ | Pharmacophore modeling identifies the spatial arrangement of molecular features (hydrogen bond donors, acceptors, aromatic rings) that are essential for biological activity. Introduced by Gund in 1977, this ligand-based method creates a three-dimensional pattern that can screen chemical libraries and design new active compounds without requiring receptor structure. | Homology modeling, also called comparative modeling, predicts the three-dimensional structure of a protein using an experimentally-solved structure of a homologous protein as a template. Introduced by Sali and Blundell in 1993, this method exploits the principle that homologous proteins share similar spatial structures despite differing in amino acid sequence. | Molecular docking predicts the preferred binding orientation and affinity of a ligand (small molecule) within a protein binding pocket. Pioneered by Kuntz and colleagues in 1982, this computational method searches conformational space to find energetically favorable ligand-protein complexes, enabling rapid screening of chemical libraries for drug discovery. |
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