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SummaryStructural detailsExperimental detailsFunctional detailsSequence NeighborHistoryDownloads

5OEY

Crystal structure of Leishmania major fructose-1,6-bisphosphatase in holo form.

Summary for 5OEY
Entry DOI10.2210/pdb5oey/pdb
DescriptorFBP protein, PHOSPHATE ION, MANGANESE (II) ION, ... (6 entities in total)
Functional Keywordsallostery, gluconeogenesis, hydrolase
Biological sourceLeishmania major
Total number of polymer chains4
Total formula weight156849.56
Authors
Yuan, M.,Vasquez-Valdivieso, M.G.,McNae, I.W.,Michels, P.A.M.,Fothergill-Gilmore, L.A.,Walkinshaw, M.D. (deposition date: 2017-07-10, release date: 2017-09-20, Last modification date: 2024-01-17)
Primary citationYuan, M.,Vasquez-Valdivieso, M.G.,McNae, I.W.,Michels, P.A.M.,Fothergill-Gilmore, L.A.,Walkinshaw, M.D.
Structures of Leishmania Fructose-1,6-Bisphosphatase Reveal Species-Specific Differences in the Mechanism of Allosteric Inhibition.
J. Mol. Biol., 429:3075-3089, 2017
Cited by
PubMed Abstract: The gluconeogenic enzyme fructose-1,6-bisphosphatase has been proposed as a potential drug target against Leishmania parasites that cause up to 20,000-30,000 deaths annually. A comparison of three crystal structures of Leishmania major fructose-1,6-bisphosphatase (LmFBPase) along with enzyme kinetic data show how AMP acts as an allosteric inhibitor and provides insight into its metal-dependent reaction mechanism. The crystal structure of the apoenzyme form of LmFBPase is a homotetramer in which the dimer of dimers adopts a planar conformation with disordered "dynamic loops". The structure of LmFBPase, complexed with manganese and its catalytic product phosphate, shows the dynamic loops locked into the active sites. A third crystal structure of LmFBPase complexed with its allosteric inhibitor AMP shows an inactive form of the tetramer, in which the dimer pairs are rotated by 18° relative to each other. The three structures suggest an allosteric mechanism in which AMP binding triggers a rearrangement of hydrogen bonds across the large and small interfaces. Retraction of the "effector loop" required for AMP binding releases the side chain of His23 from the dimer-dimer interface. This is coupled with a flip of the side chain of Arg48 which ties down the key catalytic dynamic loop in a disengaged conformation and also locks the tetramer in an inactive rotated T-state. The structure of the effector site of LmFBPase shows different structural features compared with human FBPases, thereby offering a potential and species-specific drug target.
PubMed: 28882541
DOI: 10.1016/j.jmb.2017.08.010
PDB entries with the same primary citation
Experimental method
X-RAY DIFFRACTION (2.8 Å)
Structure validation

245663

數據於2025-12-03公開中

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