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6EO9

Crystal structure of thrombin in complex with a novel glucose-conjugated potent inhibitor

Replaces:  4NZE
Summary for 6EO9
Entry DOI10.2210/pdb6eo9/pdb
Related6EO8
DescriptorProthrombin, Hirudin variant-2, DIMETHYL SULFOXIDE, ... (6 entities in total)
Functional Keywordshydrolase-hydrolase inhibitor complex, blood clotting
Biological sourceHomo sapiens (Human)
More
Total number of polymer chains3
Total formula weight36744.46
Authors
Belviso, B.D.,Caliandro, R.,Aresta, B.M.,De Candia, M.,Altomare, C.D. (deposition date: 2017-10-09, release date: 2017-12-13, Last modification date: 2024-11-20)
Primary citationBelviso, B.D.,Caliandro, R.,de Candia, M.,Zaetta, G.,Lopopolo, G.,Incampo, F.,Colucci, M.,Altomare, C.D.
How a beta-D-glucoside side chain enhances binding affinity to thrombin of inhibitors bearing 2-chlorothiophene as P1 moiety: crystallography, fragment deconstruction study, and evaluation of antithrombotic properties.
J. Med. Chem., 57:8563-8575, 2014
Cited by
PubMed Abstract: The β-d-glucose-containing compound 3, bearing 2-chlorothiophene and 1-isopropylpiperidine moieties as binders of the S1 and S4 pockets, respectively, proved to be potent competitive inhibitor of factor Xa (fXa, Ki = 0.090 nM) and thrombin (fIIa, Ki = 100 nM). The potency of 3 increases, over the parent compound 1, against fIIa (110-fold), much more than against fXa (7-fold). Experimental deconstruction of 3 into smaller fragments revealed a binding cooperativity of the P3/P4 and propylene-linked β-d-glucose fragments, stronger in fIIa (15.5 kJ·mol(-1)) than in fXa (2.8 kJ·mol(-1)). The crystal structure of human fIIa in complex with 3 revealed a binding mode including a strong H-bond network between the glucose O1', O3', and O5' and two critical residues, namely R221a and K224, belonging to the Na(+)-binding site which may allosterically perturb the specificity sites. The potential of 3 as antithrombotic agent was supported by its ability to inhibit thrombin generation and to stimulate fibrinolysis at submicromolar concentration.
PubMed: 25268757
DOI: 10.1021/jm5010754
PDB entries with the same primary citation
Experimental method
X-RAY DIFFRACTION (1.84 Å)
Structure validation

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数据于2024-12-18公开中

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