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Quantum Drug hit identification tool
Drug Hit Identification Tool calculates the IC50 (Kd, Ki, pKd) value of any protein-ligand complex, docks a small-molecule in the active site of a protein and performs screening a library of compounds against a target-protein or DNA/RNA. Hit Identification Tool consists of three modules: The IC50 module, 2) Ligand Docking and 3) Library Screening modules. Drug Hit Identification Tool can run both in Windows and Linux environments.
Hit Identification overview brochure
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Title: CRYSTAL STRUCTURE OF FREE ASPARTYL-TRNA SYNTHETASE FROM ESCHERICHIA COLI |
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Functional Class: Ligase Primary citation: Rees, B.,Webster, G.,Delarue, M.,Boeglin, M.,Moras, D. Aspartyl tRNA-synthetase from Escherichia coli: flexibility and adaptability to the substrates. J.Mol.Biol. v299 pp.1157-1164, 2000 |
Abstract Title: Aspartyl tRNA-synthetase from Escherichia coli: flexibility and adaptability to the substrates.
Keywords: Aspartyl-trna, Adenosine, Gyrase, Research, 1eqra2, 1eqra3, Coli, Bira, Molecular, (1eqr:a,, Dimerization, Sandwich, Acetyltransferase,, Catalytic, Synthetase, Base, Bira, 1eqrc1, Aminoacylation, Anticodon-binding, D1eqrc3, D1eqrc2, Non-u.s., Barrel, Insert, Proteins, Escherichia, Nucleic, Activity, Protein, Domain, Protein;, Synthetase, Anticodon, 1eqra1, Triphosphate, D1eqrb2, D1eqrb3, 1eqrc2, 1eqrc3, Acid, Aspartyl-trna, Aars, (aars)-, Binding, Rotation, Class, Study, Prokaryotic, Biosynthesis, 1eqrb3, 1eqrb2, 1eqrb1, Aspartate-trna, Domain, Crystallography, Trna, Tertiary, Gov't, X-ray, Amino, Pliability, Support, Pairing, E2p), Monophosphate, Models, (a+b), Dcoh-like, Beta, Transfer, Data, 2-layer, Like,, Magnesium, Acid-binding, (asprs), Translation, Nucleic, Fold, Mainly, Ligase, Aspartyl-trna, Comparative, Aminoacyl-trna, Secondary, (dihydrolipoamide, Aspartic, Cytoplasm, Binding, Sites, Protein, Acyl, Asprs,, Ob-fold, Ligase, Alpha, Structure, Bifunctional, Aspartate-trna, Synthetases, Beta, Ligase, D1eqrb1, Sequence, D1eqra3, D1eqra2, D1eqra1, D1eqrc1, Acid, Bacteria, Biotin, Machinery, Predictive powers, Simulation, Accuracy, Dissociation constant ligand docking, Optimize ligand alignments in torsional space, Performance, Kd, Relative selectivity associated, Confirmed, Yielded, Nanomolar, Correlation, Known, Cadd, Experimental, Comparison, Binding constant, Protein-ligand complexes, Proof of concept, Average, Absolute, Error, Kj/mol; relative error, Rmsd, Applications, Technology developers. platform, Range, Outstanding, Pkd, Molar, Dissolution, Dissociation constant, Pk receptor, Ab-initio first principals chemoinformatics, Sar, Pharmacological studies, Multigrid methods, Local optimization, Identification of low energy, Temperature, Nmol, Entropy contribution, Deactivate, Linear scaling, Quantum mechanics, Quantitative structure/activity relationship, Receptor are scored, Hierarchical filter, Genetic algorithm for protein-ligand docking,
