1e7q

GDP-4-keto-6-deoxy-d-mannose epimerase/reductase is a bifunctional enzyme, responsible for the last step in the biosynthesis of GDP-l-fucose, the, substrate of fucosyl transferases. Several cell-surface antigens, including the leukocyte Lewis system and cell-surface antigens in, pathogenic bacteria, depend on the availability of GDP-l-fucose for their, expression. Therefore, the enzyme is a potential target for therapy in, pathological states depending on selectin-mediated cell-to-cell, interactions. Previous crystallographic investigations have shown that, GDP-4-keto-6-deoxy-d-mannose epimerase/reductase belongs to the, short-chain dehydrogenase/reductase protein homology family. The enzyme, active-site region is at the interface of an N-terminal NADPH-binding, domain and a C-terminal domain, held to bind the substrate. The design, expression and functional characterization of seven site-specific mutant, forms of GDP-4-keto-6-deoxy-d-mannose epimerase/reductase are reported, here. In parallel, the crystal structures of the native holoenzyme and of, three mutants (Ser107Ala, Tyr136Glu and Lys140Arg) have been investigated, and refined at 1. 45-1.60 A resolution, based on synchrotron data, (R-factors range between 12.6 % and 13.9 %). The refined protein models, show that besides the active-site residues Ser107, Tyr136 and Lys140, whose mutations impair the overall enzymatic activity and may affect the, coenzyme binding mode, side-chains capable of proton exchange, located, around the expected substrate (GDP-4-keto-6-deoxy-d-mannose) binding, pocket, are selectively required during the epimerization and reduction, steps. Among these, Cys109 and His179 may play a primary role in proton, exchange between the enzyme and the epimerization catalytic intermediates., Finally, the additional role of mutated active-site residues involved in, substrate recognition and in enzyme stability has been analyzed.

1E7Q is a Single protein structure of sequence from Escherichia coli with , , and as ligands. Known structural/functional Sites: and . Full crystallographic information is available from OCA.

Probing the catalytic mechanism of GDP-4-keto-6-deoxy-d-mannose Epimerase/Reductase by kinetic and crystallographic characterization of site-specific mutants., Rosano C, Bisso A, Izzo G, Tonetti M, Sturla L, De Flora A, Bolognesi M, J Mol Biol. 2000 Oct 13;303(1):77-91. PMID:11021971

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