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EC Number Crystallization (Commentary) Reference
Show all pathways known for 5.3.3.2Display the word mapDisplay the reaction diagram Show all sequences 5.3.3.2enzyme shows a flexible N-terminal alpha-helix covering the active pocket and blocking the entrance. Substrate binding induces conformational change in the active site. A water molecule is the direct proton donor for the substrate 681412
Show all pathways known for 5.3.3.2Display the word mapDisplay the reaction diagram Show all sequences 5.3.3.2native enzyme at 1.7 A and in complex with substrate at 1.9 A resolution. comparison with Escherichia coli enzyme structure 681413
Show all pathways known for 5.3.3.2Display the word mapDisplay the reaction diagram Show all sequences 5.3.3.2comparison of orthorhombic, monoclinic and trigonal crystal forms, up to 2.2 A resolution. Crystallization of free enzyme and in complex wih transition-state analogue N,N-dimethyl-2-amino-1-ethyl diphosphate 690288
Show all pathways known for 5.3.3.2Display the word mapDisplay the reaction diagram Show all sequences 5.3.3.2in complex with diphosphate. The diphosphate moiety is located near the conserved residues H10, R97, H152, Q157, E158, and W219, and the flavin cofactor. The putative active site may stabilize a carbocationic intermediate 690998
Show all pathways known for 5.3.3.2Display the word mapDisplay the reaction diagram Show all sequences 5.3.3.2molecular modeling of structure and comparison with structures of Streptococcus pneumoniae and Thermus thermophilus enzymes 695056
Show all pathways known for 5.3.3.2Display the word mapDisplay the reaction diagram Show all sequences 5.3.3.2the crystal structures of the substrate-free enzyme and of the substrate-enzyme complexes, in the oxidized and reduced states, are solved to resolutions between 1.99 and 3.1 A, six distinct types of type 2 IDI crystals are obtained 704638
Show all pathways known for 5.3.3.2Display the word mapDisplay the reaction diagram Show all sequences 5.3.3.2sitting drop vapor diffusion method, using 0.6 M calcium acetate and 50 mM HEPES pH 7.5 713655
Show all pathways known for 5.3.3.2Display the word mapDisplay the reaction diagram Show all sequences 5.3.3.2crystallized at 20°C using the hanging-drop vapor diffusion method with a reservoir solution containing 0.1 M Tris-HCl (pH 8.0), 0.2 M sodium citrate, and 30% (vol/vol) polyethylene glycol 400 (PEG 400) 719740
Show all pathways known for 5.3.3.2Display the word mapDisplay the reaction diagram Show all sequences 5.3.3.2the covalent adduct formed between irreversible mechanism based inhibitors, 3-methylene-4-penten-1-yl diphosphate or 3-oxiranyl-3-buten-1-yl diphosphate, and the flavin cofactor are investigated by X-ray crystallography and UV-visible spectroscopy. Both the crystal structures of enzyme binding the flavin-inhibitor adduct and the UV-visible spectra of the adducts indicate that the covalent bond is formed at C4a of flavin rather than at N5. The high-resolution crystal structures of enzyme-substrate complexes and the kinetic studies of new mutants confirm that only the flavin cofactor can catalyze protonation of the substrates and suggest that N5 of flavin is most likely to be involved in proton transfer 728667
Show all pathways known for 5.3.3.2Display the word mapDisplay the reaction diagram Show all sequences 5.3.3.2sitting drop vapor diffusion method, using HEPES buffer (100 mM, pH 7.5 with 2 M (NH4)2SO4) 747530
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