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EC Number Subunits Commentary Reference
Show all pathways known for 2.3.1.191Display the word mapDisplay the reaction diagram Show all sequences 2.3.1.191homotrimer 3 * 35880, electrospray-ionization/time-of-flight mass spectrometry 696264
Show all pathways known for 2.3.1.191Display the word mapDisplay the reaction diagram Show all sequences 2.3.1.191homotrimer 3 * 35881, calculated from sequence 696264
Show all pathways known for 2.3.1.191Display the word mapDisplay the reaction diagram Show all sequences 2.3.1.191homotrimer each subunit of which is constructed from a novel combination of an N-terminal uridine binding domain, a core lipid-binding domain, and a C-terminal helical extension. Highly conserved residues dominate nucleotide binding. Phe43 and Tyr49 form pi-stacking interactions with uracil, and Asn46 and His284 form hydrogen bonds with the phosphate groups 700935
Show all pathways known for 2.3.1.191Display the word mapDisplay the reaction diagram Show all sequences 2.3.1.191More the LpxD domain architecture is consisting of an N-terminal domain, amino acids 2-95, a left-handed beta-helix central domain containing many short parallel beta-sheet segments wrappingthrough consecutive triangular sections, amino acids 101-305, and a C-terminal helix, amino acids 312-340 718513
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