1mlz

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1mlz, resolution 2.15Å

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Crystal Structure of 7,8-Diaminopelargonic Acid Synthase in complex with the trans-isomer of amiclenomycin.

Overview

The antibiotic amiclenomycin blocks the biosynthesis of biotin by, inhibiting the pyridoxal-phosphate-dependent enzyme diaminopelargonic acid, synthase. Inactivation of the enzyme is stereoselective, i.e. the cis, isomer of amiclenomycin is a potent inhibitor, whereas the trans isomer is, much less reactive. The crystal structure of the complex of the holoenzyme, and amiclenomycin at 1.8 A resolution reveals that the internal aldimine, linkage between the cofactor and the side chain of the catalytic residue, Lys-274 is broken. Instead, a covalent bond is formed between the 4-amino, nitrogen of amiclenomycin and the C4' carbon atom of pyridoxal-phosphate., The electron density for the bound inhibitor suggests that aromatization, of the cyclohexadiene ring has occurred upon formation of the covalent, adduct. This process could be initiated by proton abstraction at the C4, carbon atom of the cyclohexadiene ring, possibly by the proximal side, chain of Lys-274, leading to the tautomer Schiff base followed by the, removal of the second allylic hydrogen. The carboxyl tail of the, amiclenomycin moiety forms a salt link to the conserved residue Arg-391 in, the substrate-binding site. Modeling suggests steric hindrance at the, active site as the determinant of the weak inhibiting potency of the trans, isomer.

About this Structure

1MLZ is a Single protein structure of sequence from Escherichia coli with TZA, NA and PLP as ligands. Active as Adenosylmethionine--8-amino-7-oxononanoate transaminase, with EC number 2.6.1.62 Full crystallographic information is available from OCA.

Reference

Structural basis for the inhibition of the biosynthesis of biotin by the antibiotic amiclenomycin., Sandmark J, Mann S, Marquet A, Schneider G, J Biol Chem. 2002 Nov 8;277(45):43352-8. Epub 2002 Sep 5. PMID:12218056

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