Journal Article10.1016/S1093-3263(02)00164-X
LigandFit: a novel method for the shape-directed rapid docking of ligands to protein active sites
1K
TL;DR: A new shape-based method for accurately docking ligands into protein active sites, LigandFit, which appears quite promising, reproducing the X-ray structure ligand pose within an RMS of 2A in 14 out of the 19 complexes.
read more
Abstract: We present a new shape-based method, LigandFit, for accurately docking ligands into protein active sites. The method employs a cavity detection algorithm for detecting invaginations in the protein as candidate active site regions. A shape comparison filter is combined with a Monte Carlo conformational search for generating ligand poses consistent with the active site shape. Candidate poses are minimized in the context of the active site using a grid-based method for evaluating protein-ligand interaction energies. Errors arising from grid interpolation are dramatically reduced using a new non-linear interpolation scheme. Results are presented for 19 diverse protein-ligand complexes. The method appears quite promising, reproducing the X-ray structure ligand pose within an RMS of 2A in 14 out of the 19 complexes. A high-throughput screening study applied to the thymidine kinase receptor is also presented in which LigandFit, when combined with LigScore, an internally developed scoring function, yields very good hit rates for a ligand pool seeded with known actives.
read more
Chat with Paper
AI Agents for this Paper
Find similar papers on Google Scholar, PubMed and Arxiv
Write a critical review of this paper
Analyze citations of this paper to find unaddressed research gaps
Citations
Network pharmacology-based approach of novel traditional Chinese medicine formula for treatment of acute skin inflammation in silico.
Hsin-Chieh Tang,Hung-Jin Huang,Cheng-Chun Lee,Calvin Yu-Chian Chen,Calvin Yu-Chian Chen,Calvin Yu-Chian Chen +5 more
TL;DR: The herbs Hypericum patulum, Sedum acre, and Tripterygium wilfordii are suggested that containing Celallocinnine, Celacinnine and Lobelanidine might be a novel medicine formula to avoid the side effect of tetracycline and increase the efficacy of treatment.
27
KRC-408, a novel c-Met inhibitor, suppresses cell proliferation and angiogenesis of gastric cancer
Sang-Won Hong,K. H. Jung,Byung Hee Park,Hong-Mei Zheng,Hee-Seung Lee,Myung-Joo Choi,Jeong In Yun,Nam Sook Kang,Jongkook Lee,Soon-Sun Hong +9 more
TL;DR: Results of an in vivo mouse xenograft experiment showed that the administration of KRC-408 significantly delayed tumor growth in a dose-dependent manner, and suppressed Akt and Erk phosphorylation as well CD34 expression in tumor tissues, indicating that KCR-408 may exert anti-tumor effects by directly affecting tumor cell growth or survival via the c-Met receptor tyrosine kinase pathway.
27
Amino-pyrrolidine tricarboxylic acids give new insight into group III metabotropic glutamate receptor activation mechanism.
Mélanie Frauli,Nadia Hubert,Stephan Schann,Nicolas Triballeau,Hugues-Olivier Bertrand,Francine Acher,Pascal Neuville,Jean-Philippe Pin,Laurent Prézeau +8 more
TL;DR: This work elucidated why FP0429 behaves differently at these two highly homologous receptors by focusing on two residues within the binding site that differ between mGlu4 and mGLU8, and identified two residues that may allow a deeper positioning of this agonist in the cavity of lobe I, thereby ensuring optimal interactions with lobe II residues in the fully closed state of the VFT.
27
7-Ethynylcoumarins: Selective Inhibitors of Human Cytochrome P450s 1A1 and 1A2
Jiawang Liu,Thong T. Nguyen,Patrick S. Dupart,Jayalakshmi Sridhar,Xiaoyi Zhang,Naijue Zhu,Cheryl L. Klein Stevens,Maryam Foroozesh +7 more
TL;DR: To discover new selective mechanism-based P450 inhibitors, eight 7-ethynylcoumarin derivatives were prepared through a facile two-step synthetic route, and 7E3M4PC with its two-plane structure fits into the P450 1A2's active site cavity with an orientation leading to no reactive binding, causing it to act as a competitive inhibitor.
27
Effects of variable docking conditions and scoring functions on corresponding protein-aligned comparative molecular field analysis models constructed from diverse human protein tyrosine phosphatase 1B inhibitors.
Mutasem O. Taha,Murad A. AlDamen +1 more
TL;DR: To utilize the predictive potentials of the best CoMFA models collectively, it was decided to combine them in a single quantitative structure-activity relationship (QSAR) model, which illustrated excellent statistical properties.
27
References
Development and validation of a genetic algorithm for flexible docking.
TL;DR: GOLD (Genetic Optimisation for Ligand Docking) is an automated ligand docking program that uses a genetic algorithm to explore the full range of ligand conformational flexibility with partial flexibility of the protein, and satisfies the fundamental requirement that the ligand must displace loosely bound water on binding.
6.5K
DREIDING: A generic force field for molecular simulations
TL;DR: The DREIDING force field as discussed by the authors uses general force constants and geometry parameters based on simple hybridization considerations rather than individual force constants or geometric parameters that depend on the particular combination of atoms involved in the bond, angle, or torsion terms.
6.2K
A Fast Flexible Docking Method using an Incremental Construction Algorithm
TL;DR: This work presents an automatic method for docking organic ligands into protein binding sites that combines an appropriate model of the physico-chemical properties of the docked molecules with efficient methods for sampling the conformational space of the ligand.
2.8K
A geometric approach to macromolecule-ligand interactions
TL;DR: A method to explore geometrically feasible alignments of ligands and receptors of known structure and finds distinctly different geometries that provide good steric fits seems well-suited for generating starting conformations for energy refinement programs and interactive computer graphics routines.
2.4K
•Book
Fundamentals of interactive computer graphics
James D. Foley,Andries van Dam +1 more
- 01 Jan 1982
TL;DR: The foundations of interactive computer graphics are studied in detail in the second part of this monograph on computer graphics theory andUX.
2.2K